CN1104432C - Pyrrole triazines and pyrimidines - Google Patents
Pyrrole triazines and pyrimidines Download PDFInfo
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- CN1104432C CN1104432C CN97196525A CN97196525A CN1104432C CN 1104432 C CN1104432 C CN 1104432C CN 97196525 A CN97196525 A CN 97196525A CN 97196525 A CN97196525 A CN 97196525A CN 1104432 C CN1104432 C CN 1104432C
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Abstract
Corticotropin releasing factor (CRF) antagonists of formula (I) or (II) and their use in treating anxiety, depression, and other psychiatric, neurological disorders as well as treatment of immunological, cardiovascular or heart-related diseases and colonic hypersensitivity associated with psychopathological disturbance and stress.
Description
The field of the invention
The present invention relates to by give some [1,5-a]-pyrazolo-1,3,5-triazines, [1,5-a]-1,2,3-triazolo-1,3,5-triazines, [1,5-a]-pyrazolo-pyrimidine class and [1,5-a]-1,2,3-triazolo-pyrimidines treatment mental disorder and nervous system disease comprise severe depression, with anxiety relative disease, wound after stress disease, nuclear go up and benumb and eating disorder, and treat immune, cardiovascular or with cardiac-related diseases, the adaptive colitis relevant with stress with mental disorder.
Background of the present invention
Corticotropin releasing factor(CRF) (after this claiming CRF), for having 41 amino acid whose peptides, it is main physiological regulation agent [J.Rivier etc., Proc.Nat.Acad.Sci. (USA) 80:4851 (1983) of the peptide deutero-proopiomelanocortin of prepituitary gland glandular secretion; W.Vale etc., Science 213:1394 (1981)].Except that its internal secretion effect to pituitary gland, the immunohistochemistry of CRF location shows that this hormone has widely in central nervous system and distributes outside the hypothalamus, and generation widely spontaneous, electric physiology and behavior effect [W.Vale etc., the Rec.Prog.Horm.Res.39:245 (1983) consistent in brain with neurotransmitter or neuroregulator effect; G.F.Koob, Persp.Behav.Med.2:39 (1985); E.B.De Souza etc., J.Neurosci.5:3189 (1985)].Evidence suggests that also CRF plays remarkable effect [J.E.Blalock, PhysiologicalReviews 69:1 (1989) in the integration that immunity system is replied physiology, psychology and immunological stress thing; J.E.Morley, Life Sci.41:527 (1987)].
Clinical data be CRF at mental disorder and nervous system disease, comprise dysthymia disorders, with anxiety relative disease and eating disorder in have effect evidence be provided.Suppose also that CRF benumbs on AlzheimerShi disease, ParkinsonShi disease, HuntingtonShi disease, carrying out property nuclear and the nosetiology of amyotrophic lateral sclerosis and physiopathology in work, because they with central nervous system in CRF neurone imbalance relevant [seeing E.B.De Souza, Hosp.Practice23:59 (1988)].
In thymopathy or severe depression, refuse to obey that the middle CRF concentration of individual cerebrospinal fluid (CSF) of medicine significantly increases [C.B.Nemeroff etc., Science 226:1342 (1984); C.M.Banki etc., Am. J.Psychiatry 144:873 (1987); R.D.France etc., Biol.Psychiatry 28:86 (1988); M.Arato etc., Biol Psychiatry 25:355 (1989)].And the CRF Rd significantly reduces in the preceding cortex of suicide patient, and CRF supersecretion [C.B.Nemeroff etc., Arch.Gen.Psychiatry 45:577 (1988)].In addition, the thyroliberin of observing in the patient of depression the CRF passivation (ACTH) reacts (behind the intravenously administrable) [P.W.Gold etc., Am.J.Psychiatry 141:619 (1984); F.Holsboer etc., Psychoneuroendocrinology 9:147 (1984); P.W.Gold etc., New Eng.J.Med.314:1129 (1986)].The preclinical study that carries out in rat and inhuman Primates may the hypothesis relevant with the symptom of observing in people's dysthymia disorders provide other support [R.M.Sapolsky, Arch.Gen.Psychiatry 46:1047 (1989)] for the too much secretion of CRF.Prima Facie Evidence shows that tricyclic antidepressants can change the number [Grigoriadis etc., Neuropsychopharmacology 2:53 (1989)] that therefore the CRF level also regulates CRF acceptor in the brain.
Also to CRF with the nosetiology of anxiety relative disease in effect supposition has been proposed.CRF produces anxiety (anxiogenic) effect in animal, and interaction [D.R.Britton etc., Life Sci.31:363 (1982) between benzodiazepine /non--benzodiazepine anxiolytic and CRF in multiple behavior anxiety model, have been proved; C.W.Berridge and A.J.DunnRegul.Peptides 16:83 (1986)].The preliminary study of carrying out in multiple behavior example with the CRF receptor antagonist a-spiral sheep CRF (9-41) that supposes shows that described antagonist produces and " anxiety sample " effect [C.W.Berridge and A.J.Dunn Horm.Behav.21:393 (1987), Brain Research Reviews 15:71 (1990)] of benzodiazepine similar performance.Neurochemistry, internal secretion and receptors bind research all show the interaction between CRF and benzodiazepine anxiolytic, for the relation of CRF and these diseases provides other evidence.Zeisin can weaken conflict test [K.T.Britton etc., the Psychophamacology 86:170 (1985) of CRF rat; K.T.Britton etc., Psychopharmacology 94:306 (1988)] and " anxiety " in the sense of hearing startles test [N.R.Swerdlow etc., Psychopharmacology 88:147 (1986)] effect.The CRF effect of benzodiazepine receptor antagonist (Ro15-1788) (no behavior activity in operability the is conflicted test separately) dosage that can reverse-dependence mode, and the opposite agonist (FG7142) of benzodiazepine can strengthen CRF effect [K.T.Britton etc., Psychopharmacology94:306 (1988)].
Mechanism and action site that standard anxiolytic and thymoleptic produce its therapeutic action are still waiting to illustrate.Yet we suppose that the too much excretory of they and observed CRF in these diseases suppresses relevant.The preliminary study that our interest is in multiple behavior model to measure the effect of CRF receptor antagonist (alpha-helix CRF 9-41) shows that the CRF antagonist produces " anxiety sample " effect of being similar to benzodiazepine in nature and [sees G.F.Koob and K.T.Britton: corticotropin releasing factor(CRF): the basis of neuropeptide and clinical study, E.B.De Souza and C.B.Nemeroff edit, CRF Press the 221st page (1990)].
Several publications have been described Corticotropin releasing factor antagonists compound and their purposes in treatment mental disorder and nervous system disease.The example of this type of publication comprises the WO 95/33727 of WO 95/34563, Pfizer of WO 95/33750, Pfizer of PCT application US94/11050, Pfizer of DuPont Merck and the EP0778277A1 of Pfizer.
It is reported up to the present, also not with [1,5-a]-pyrazolo-1,3,5-triazines, [1,5-a]-1,2,3-triazolo-1,3,5-triazines class, [1,5-a]-pyrazolo-pyrimidine class and [1,5-a]-1,2,3-triazoles also-pyrimidines is used for the treatment of the report of mental disorder and nervous system disease as the Corticotropin releasing factor antagonists compound.Yet part of compounds is used for other purposes to have report to incite somebody to action wherein.
For example, the method for preparation of pyrazolotriazine compounds of the open following formula of EP 0269859 (Ostuka, 1988):
R wherein
1Be OH or alkanoyl, R
2Be H, OH or SH, R
3Be the phenyl of undersaturated heterocyclic group, naphthyl or replacement, and think that these compounds have xanthine oxidase inhibitory activity and are used for the treatment of gout.
The method for preparation of pyrazolotriazine and the Pyrazolopyrimidine compound of the open following formula of EP 0594149 (Ostuka, 1994):
Wherein A is CH or N, R
0And R
3Be H or alkyl, R
1And R
2Be H, alkyl, alkoxyl group, alkylthio, nitro etc., and think that these compounds suppress male hormone, can be used for the treatment of benign prostatauxe and prostate cancer.
The method for preparation of pyrazolotriazine compounds of the open following formula of US 3910907 (ICI, 1975):
R wherein
1Be CH
3, C
2H
5Or C
6H
5, X is H, C
6H
5, m-CH
3C
6H
4, CN, COOEt, Cl, I or Br, Y is H, C
6H
5, o-CH
3C
6H
4Or p-CH
3C
6H
4, Z is OH, H, CH
3, C
2H
5, C
6H
5, n-C
3H
7, i-C
3H
7, SH, SCH
3, NHC
4H
9Or N (C
2H
5)
2, and think that these compounds are the c-AMP phosphodiesterase inhibitor, as bronchodilator.
The method for preparation of pyrazolotriazine compounds of US 3995039 open following formulas:
R wherein
1Be H or alkyl, R
2Be H or alkyl, R
3Be H, alkyl, alkanoyl, formamyl or elementary alkyl amido methanoyl, R is pyridyl, pyrimidyl or pyrazinyl, and thinks that these compounds can be used as bronchodilator.
The method for preparation of pyrazolotriazine compounds of US 5137887 open following formulas:
Wherein R is a lower alkoxy, and to propose these compounds be xanthine oxidase inhibitor, can be used for the treatment of gout.
The method for preparation of pyrazolotriazine compounds of US 4892576 open following formulas:
Wherein X is O or S, and Ar is phenyl, naphthyl, pyridyl or thienyl, R
6-R
8Be H, alkyl etc., R
9Be H, alkyl and phenyl etc.This patent points out that these compounds can be used as sterilant and plant-growth regulator.
US 5484760 and WO 92/10098 openly contain the insect-killing composition of the Pesticidal compound of following formula:
Wherein A can be N, and B can be CR
3, R
3Can be phenyl of phenyl or replacement etc., R is-N (R
4) SO
2R
5Or-SO
2N (R
6) R
7, R
1And R
2Can form together:
Or
Wherein X, Y and Z are H, alkyl, acyl group etc., and D is O or S.
US 3910907 and Senga etc. (J.Med.Chem., 1982,25,243-249) the triazolo triazine cAMP phosphodiesterase inhibitor of open following formula:
Wherein Z is H, OH, CH
3, C
2H
5, C
6H
5, n-C
3H
7, i-C
3H
7, SH, SCH
3, NH (n-C
4H
9) or N (C
2H
5)
2, R is H or CH
3, R
1Be CH
3Or C
2H
5This reference is listed the treatment field that 8 cAMP phosphodiesterase inhibitors have operability: asthma, diabetes, female contraception, male infertility, psoriasis, thrombosis, anxiety disorder and hypertension.
The open Pyrazolopyrimidine compound of WO 95/35298 (Otsuka, 1995), and think and can be used as analgesic agent.These compounds can be represented by following formula:
Wherein Q is carbonyl or alkylsulfonyl, and n is 0 or 1, and A is singly-bound, alkylidene group, alkylene group, R
1Be H, alkyl etc., R
2Be the phenyl or the phenoxy group of naphthyl, cycloalkyl, heteroaryl, replacement, R
3Be H, alkyl or phenyl, R
4Be H, alkyl, alkoxy carbonyl, phenylalkyl, phenyl or halogen that the optional benzene sulfenyl replaces, R
5And R
6Be H or alkyl.
The antiphlogistic use of the Pyrazolopyrimidine compound of the open following formula representative of EP 0591528 (Otsuka, 1991):
R wherein
1, R
2, R
3And R
4Be H, carboxyl, alkoxy carbonyl, optional alkyl, cycloalkyl or the phenyl that replaces, R
5Be SR
6Or NR
7R
8, R
6Be pyridyl or the optional phenyl that replaces, R
7And R
8Be H or the optional phenyl that replaces.
Springer etc. (J.Med.Chem., 1976, vol.19, no.2,291-296) with the U.S. patent 4021556 of Springer and the Pyrazolopyrimidine compound of 3920652 open following formulas:
Wherein R can be the phenyl or the pyridyl of phenyl, replacement, can be used for the treatment of gout so suppress XOD based on them.
Joshi etc. (J.Prakt.Chemie, 321,2,1979, the 341-344) compound of open following formula:
R wherein
1Be CF
3, C
2F
5Or C
6H
4F, R
2Be CH
3, C
2H
5, CF
3Or C
6H
4F.
Pyrazolo [1, the 5-a] pyrimidine compound of the open following formula of Mquestiau etc. (Bull.Soc.Belg., vol.101, no.2,1992, the 131-136 pages or leaves):
Open following formula pyrazolo [1, the 5-a] pyrimidine compound of Ibrahim etc. (Arch.Pharm. (weinheim) 320,487-491 (1987)):
Wherein R is NH
2Or OH, Ar is 4-phenyl-3-cyano group-2-aminopyridine-2-base.Other reference of open azolopyrimidines comprises:
EP 0 511 528 (Otsuka, 1992), US4,997,940 (Dow, 1991), EP 0 374 448 (Nissan, 1990), US4,621,556 (ICN, 1997), EP 0 531 901 (Fujisawa, 1993), US4,567,263 (BASF, 1986), EP 0 662 477 (Isagro, 1995), DE4 243 279 (Bayer, 1994), US 5,397,774 (Upjohn, 1995), EP0 521 622 (Upjohn, 1993), WO 94/109017 (Upjohn, 1994), J.Med.Chem., 24,610-613 (1981), with J. Het. Chem., 22,601 (1985).
General introduction of the present invention
According to an aspect of the present invention, the invention provides new compound, medicinal compositions and can be used for the treatment of affective disorder, anxiety disorder, dysthymia disorders, irritable bowel syndrome, stress disease after the wound, paralysis on the nuclear, immunosuppression, the AlzheimerShi disease, gastrointestinal dysfunction, anorexia nervosa or other eating disorder, medicine or alcohol withdrawal symptom, drug habit, diseases associated with inflammation, growing barrier, disorderly, the disease that can work or help to treat by antagonism CRF includes but not limited to the disease that CRF induces or helps, or following diseases associated with inflammation: for example rheumatoid arthritis and osteoarthritis, pain, asthma, psoriasis and transformation reactions; General anxiety disease; Fear, fear, obsessional idea and behavior disorder; Stress disease after the wound; The somnopathy of bringing out by stress; The pain perception is fibromyalgia for example; Affective disorder is dysthymia disorders for example, comprises dysthymia disorders and post-natal depression that severe depression, disposable outbreak dysthymia disorders, recurrent major depression, children's drug abuse are brought out; Dispiritment (dysthemia); Two-way affective disorder; Cyclothymia; Fatigue syndrome; The headache that stress brings out; Cancer, human immunodeficiency virus (HIV) infects; Neurodegenerative disease is AlzheimerShi disease, ParkinsonShi disease and HuntingtonShi disease for example; Gastrointestinal dysfunction for example ulcer, irritable bowel syndrome, CrohnShi disease, spastic colon, diarrhoea, postoperative ilius with spiritual pathology disorder or the relevant adaptive colitis of stress; Eating disorder is anorexia and bulimia nervosa for example; Hemorrhage stress reaction; Stress reaction inductive psychic fit; Thyropathy syndrome; Inappropriate antidiarrheal (antidiarrhetic) hormone (ADH) syndrome; Obesity; Infertility; Wound; Spinal cord injuries receptor; Ischemic neuron infringement (as cerebral ischemia cerebral hippocampus ischemic for example); The infringement of exitotoxicity (excitotoxic) neurone; Epilepsy; Cardiovascular disorder and the disease relevant with heart comprise hypertension, tachycardia and congestive heart failure; Apoplexy; Immune disorder comprise pressure inducement immune disorder (the inductive imbalance of laying eggs of the fever of bringing out as pressure, pig pressure syndrome, ox shipment fever (bovine shipping), horse paroxysmal fibrillation and chicken, in pure pressure in the sheep or the dog with people-animal relevant pressure that interacts); Muscle spasm; The urinary incontinence; The senile dementia of Alzheimer type; Multi-infarct dementia; Amyotrophic lateral sclerosis; Chemical relies on and habituation (as alcohol, Cocaine, heroine, benzodiazepine or other medicines habituation); Medicine and alcohol withdrawal syndrome; Osteoporosis, the psychological nanism of Mammals and hypoglycemia.
The invention provides new combining, and therefore change the compound of CRF excretory anxiety effect with the corticotropin-releasing factor receptor body.Compound of the present invention can be used for the treatment of paralysis and eating disorder on stress disease after Mammals mental disorder and nervous system disease, the disease relevant with anxiety, the wound, the nuclear, and the treatment mammalian immune, cardiovascular or with cardiac-related diseases and with the adaptive colitis of spiritual pathology imbalance and pressure correlation.
According on the other hand, the invention provides new formula (1) and (2) (as following) compound, they can be as the antagonist of corticotropin releasing factor(CRF).As if compound of the present invention shows active as Corticotropin releasing factor antagonists, and suppress the CRF excessive secretion.The present invention also comprises the medicinal compositions that contains this formula (1) and (2) compound, and the method that suppresses CRF excessive secretion and/or treatment anxiety disorder with this compounds.
According to a further aspect in the invention, the invention provides also can be as the standard of the ability of measuring potential medicine and CRF receptors bind and the compound (The compounds of this invention that particularly marks) of reagent.
Detailed description of the present invention
[1] the present invention includes treatment Mammals affective disorder, anxiety disorder, dysthymia disorders, headache, irritable bowel syndrome, pressure disease after the wound, paralysis on the nuclear, immunosuppression, the AlzheimerShi disease, gastrointestinal dysfunction, anorexia nervosa or other eating disorder, drug habit, medicine or alcohol withdrawal symptom, diseases associated with inflammation, cardiovascular or and cardiac-related diseases, growing barrier, people's HIVvirus blood serum immunity infects, the hemorrhagic stress reaction, obesity, infertility, head and spinal cord injuries receptor, epilepsy, apoplexy, ulcer, amyotrophic lateral sclerosis, the disease that hypoglycemia maybe can work or help to treat by antagonism CRF, include but not limited to be induced or promoted disease by CRF, this method comprises formula (1) or (2) compound and its isomer that gives Mammals treatment significant quantity, the mixture of steric isomer or steric isomer with and pharmacy acceptable salt or prodrug:
Wherein:
A is N or CR;
Z is N or CR
2
Ar is selected from phenyl, naphthyl, pyridyl, pyrimidyl, triazinyl, furyl, thienyl, benzothienyl, benzofuryl, 2,3-dihydro benzo furyl, 2,3-dihydrobenzo thienyl, 2,3-indanyl, 1,2-benzopyranyl, 3,4-dihydro-1,2-benzopyranyl, 1,2,3, the 4-tetrahydro naphthyl, each Ar is optional by 1-5 R
4Group replaces, and each Ar can link to each other with undersaturated carbon atom;
R independently is selected from H, C
1-C
4Alkyl, C
2-C
4Alkenyl, C
2-C
4Alkynyl, C
3-C
6Cycloalkyl, C
4-C
7Cycloalkylalkyl, halogen, CN, C
1-C
4Haloalkyl;
R
1Independently be selected from H, C
1-C
4Alkyl, C
2-C
4Alkenyl, C
2-C
4Alkynyl, halogen, CN, C
1-C
4Haloalkyl, C
1-C
12Hydroxyalkyl, C
2-C
12Alkoxyalkyl, C
2-C
10Cyano group alkyl, C
3-C
6Cycloalkyl, C
4-C
10Cycloalkylalkyl, NR
9R
10, C
1-C
4Alkyl-NR
9R
10, NR
9COR
10, OR
11, SH or S (O)
nR
12
R
2Be selected from H, C
1-C
4Alkyl, C
2-C
4Alkenyl, C
2-C
4Alkynyl, C
3-C
6Cycloalkyl, C
4-C
10Cycloalkylalkyl, C
1-C
4Hydroxyalkyl, halogen, CN ,-NR
6R
7, NR
9COR
10,-NR
6S (O)
nR
7, S (O)
nNR
6R
7, C
1-C
4Haloalkyl, OR
7, SH or S (O)
nR
12
R
3Be selected from
-H, OR
7, SH, S (O)
nR
13, COR
7, CO
2R
7, OC (O) R
13, NR
8COR
7, N (COR
7)
2, NR
8CONR
6R
7, NR
8CO
2R
13, NR
6R
7, NR
6aR
7a, N (OR
7) R
6, CONR
6R
7, aryl, heteroaryl and heterocyclic radical, or
-C
1-C
10Alkyl, C
2-C
10Alkenyl, C
2-C
10Alkynyl, C
3-C
8Cycloalkyl, C
5-C
8Cycloalkenyl group, C
4-C
12Cycloalkylalkyl or C
6-C
10Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl and heterocyclic radical;
R
4Independently be selected from: C
1-C
10Alkyl, C
2-C
10Alkenyl, C
2-C
10Alkynyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, NO
2, halogen, CN, C
1-C
4Haloalkyl, NR
6R
7, NR
8COR
7, NR
8CO
2R
7, COR
7, OR
7, CONR
6R
7, CO (NOR
9) R
7, CO
2R
7Or S (O)
nR
7, each C wherein
1-C
10Alkyl, C
2-C
10Alkenyl, C
2-C
10Alkynyl, C
3-C
6Cycloalkyl and C
4-C
12Cycloalkylalkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
4Alkyl, NO
2, halogen, CN, NR
6R
7, NR
8COR
7, NR
8CO
2R
7, COR
7, OR
7, CONR
6R
7, CO
2R
7, CO (NOR
9) R
7Or S (O)
nR
7
R
6And R
7, R
6aAnd R
7aIndependently be selected from:
-H,
-C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl), heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
Perhaps, NR
6R
7And NR
6aR
7aIndependent is piperidines, tetramethyleneimine, piperazine, N methyl piperazine, morpholine or thiomorpholine, and each is optional by 1-3 C
1-C
4Alkyl replaces;
R
8Independently be selected from H or C
1-C
4Alkyl;
R
9And R
10Independently be selected from H, C
1-C
4Alkyl or C
3-C
6Cycloalkyl;
R
11Be selected from H, C
1-C
4Alkyl, C
1-C
4Haloalkyl or C
3-C
6Cycloalkyl;
R
12Be C
1-C
4Alkyl or C
1-C
4Haloalkyl;
R
13Be selected from C
1-C
4Alkyl, C
1-C
4Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, aryl, aryl (C
1-C
4Alkyl)-, heteroaryl or heteroaryl (C
1-C
4Alkyl)-;
R
14Be selected from C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, C
3-C
8Cycloalkyl or C
4-C
12Cycloalkylalkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
15, COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
15, NR
16R
15, CONR
16R
15And C
1-C
6Alkylthio, C
1-C
6Alkyl sulphinyl and C
1-C
6Alkyl sulphonyl;
R
15And R
16Independently be selected from H, C
1-C
6Alkyl, C
3-C
10Cycloalkyl, C
4-C
16Cycloalkylalkyl, but when being S (O)
nR
15The time, R
15Can not be H;
Aryl is a phenyl or naphthyl, and each is chosen wantonly by 1-5 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
15, COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
15, NR
16R
15And CONR
16R
15
Heteroaryl is pyridyl, pyrimidyl, triazinyl, furyl, pyranyl, quinolyl, isoquinolyl, thienyl, imidazolyl, thiazolyl, indyl, pyrryl, oxazolyl, benzofuryl, benzothienyl, benzothiazolyl, isoxazolyl, pyrazolyl, 2,3-dihydrobenzo thienyl or 2, the 3-dihydro benzo furyl, each is chosen wantonly by 1-5 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
15, COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
15, NR
16R
15And CONR
16R
15
Heterocyclic radical is the heteroaryl of saturated or fractional saturation, chooses wantonly by 1-5 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
15, COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
15, NR
16R
15And CONR
16R
15
N independently is 0,1 or 2.
[2] preferable methods of the present invention is such method, and wherein in formula (1) or (2) compound, Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, and each is optional by 1-4 R
4Substituting group replaces.
[3] the also preferred such method of the present invention, wherein in formula (1) or (2) compound, A is N, Z is CR
2, Ar is a 2,4 dichloro benzene base, 2,4-3,5-dimethylphenyl or 2,4,6-trimethylphenyl, R
1And R
2Be CH
3, R
3Be NR
6aR
7a
[4] mixture that the present invention includes the compound of formula (1) or (2) and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form:
Wherein:
A is N or CR;
Z is N or CR
2
Ar is selected from phenyl, naphthyl, pyridyl, pyrimidyl, triazinyl, furyl, thienyl, benzothienyl, benzofuryl, 2,3-dihydro benzo furyl, 2,3-dihydrobenzo thienyl, 2,3-indanyl, 1,2-benzopyranyl, 3,4-dihydro-1,2-benzopyranyl, 1,2,3, the 4-tetrahydro naphthyl, each Ar is optional by 1-5 R
4Group replaces, and each Ar can link to each other with undersaturated carbon atom;
R independently is selected from H, C
1-C
4Alkyl, C
2-C
4Alkenyl, C
2-C
4Alkynyl, C
3-C
6Cycloalkyl, C
4-C
7Cycloalkylalkyl, halogen, CN, C
1-C
4Haloalkyl;
R
1Independently be selected from H, C
1-C
4Alkyl, C
2-C
4Alkenyl, C
2-C
4Alkynyl, halogen, CN, C
1-C
4Haloalkyl, C
1-C
12Hydroxyalkyl, C
2-C
12Alkoxyalkyl, C
2-C
10Cyano group alkyl, C
3-C
6Cycloalkyl, C
4-C
10Cycloalkylalkyl, NR
9R
10, C
1-C
4Alkyl-NR
9R
10, NR
9COR
10, OR
11, SH or S (O)
nR
12
R
2Be selected from H, C
1-C
4Alkyl, C
2-C
4Alkenyl, C
2-C
4Alkynyl, C
3-C
6Cycloalkyl, C
4-C
10Cycloalkylalkyl, C
1-C
4Hydroxyalkyl, halogen, CN ,-NR
6R
7, NR
9COR
10,-NR
6S (O)
nR
7, S (O)
nNR
6R
7, C
1-C
4Haloalkyl ,-OR
7, SH or S (O)
nR
12
R
3Be selected from
-H, OR
7, SH, S (O)
nR
13, COR
7, CO
2R
7, OC (O) R
13, NR
8COR
7, N (COR
7)
2, NR
8CONR
6R
7, NR
8CO
2R
13, NR
6R
7, NR
6aR
7a, N (OR
7) R
6, CONR
6R
7, aryl, heteroaryl and heterocyclic radical, or
-C
1-C
10Alkyl, C
2-C
10Alkenyl, C
2-C
10Alkynyl, C
3-C
8Cycloalkyl, C
5-C
8Cycloalkenyl group, C
4-C
12Cycloalkylalkyl or C
6-C
10Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl and heterocyclic radical;
R
4Independently be selected from: C
1-C
10Alkyl, C
2-C
10Alkenyl, C
2-C
10Alkynyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, NO
2, halogen, CN, C
1-C
4Haloalkyl, NR
6R
7, NR
8COR
7, NR
8CO
2R
7, COR
7, OR
7, CONR
6R
7, CO (NOR
9) R
7, CO
2R
7Or S (O)
nR
7, each C wherein
1-C
10Alkyl, C
2-C
10Alkenyl, C
2-C
10Alkynyl, C
3-C
6Cycloalkyl and C
4-C
12Cycloalkylalkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
4Alkyl, NO
2, halogen, CN, NR
6R
7, NR
8COR
7, NR
8CO
2R
7, OR
7, CONR
6R
7, CO
2R
7, CO (NOR
9) R
7Or S (O)
nR
7
R
6And R
7, R
6aAnd R
7aIndependently be selected from:
-H,
-C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl), heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
Perhaps, NR
6R
7And NR
6aR
7aIndependent is piperidines, tetramethyleneimine, piperazine, N methyl piperazine, morpholine or thiomorpholine, and each is optional by 1-3 C
1-C
4Alkyl replaces;
R
8Independently be selected from H or C
1-C
4Alkyl;
R
9And R
10Independently be selected from H, C
1-C
4Alkyl or C
3-C
6Cycloalkyl;
R
11Be selected from H, C
1-C
4Alkyl, C
1-C
4Haloalkyl or C
3-C
6Cycloalkyl;
R
12Be C
1-C
4Alkyl or C
1-C
4Haloalkyl;
R
13Be selected from C
1-C
4Alkyl, C
1-C
4Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, aryl, aryl (C
1-C
4Alkyl)-, heteroaryl or heteroaryl (C
1-C
4Alkyl)-;
R
14Be selected from C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, C
3-C
8Cycloalkyl or C
4-C
12Cycloalkylalkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
15, COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
15, NR
16R
15, CONR
16R
15And C
1-C
6Alkylthio, C
1-C
6Alkyl sulphinyl and C
1-C
6Alkyl sulphonyl;
R
15And R
16Independently be selected from H, C
1-C
6Alkyl, C
3-C
10Cycloalkyl, C
4-C
16Cycloalkylalkyl, but when being S (O)
nR
15The time, R
15Can not be H;
Aryl is a phenyl or naphthyl, and each is chosen wantonly by 1-5 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
15, COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
15, NR
16R
15And CONR
16R
15
Heteroaryl is pyridyl, pyrimidyl, triazinyl, furyl, pyranyl, quinolyl, isoquinolyl, thienyl, imidazolyl, thiazolyl, indyl, pyrryl, oxazolyl, benzofuryl, benzothienyl, benzothiazolyl, isoxazolyl, pyrazolyl, 2,3-dihydrobenzo thienyl or 2, the 3-dihydro benzo furyl, each is chosen wantonly by 1-5 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
15,-COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
15, NR
16R
15And CONR
16R
15
Heterocyclic radical is the heteroaryl of saturated or fractional saturation, chooses wantonly by 1-5 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
15, COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
15, NR
15R
16And CONR
16R
15
N independently is 0,1 or 2,
Prerequisite is:
(1) when A be N, Z is CR
2, R
2Be H, R
3For-OR
7Or-OCOR
13And R
7During for H, R so
1Can not be H, OH or SH;
(2) when A be N, Z is CR
2, R
1Be CH
3Or C
2H
5, R
2Be H, R
3Be OH, H, CH
3, C
2H
5, C
6H
5, n-C
3H
7, i-C
3H
7, SH, SCH
3, NHC
4H
9Or N (C
2H
5)
2The time, so Ar can not for phenyl or-CH
3-phenyl;
(3) when A be N, Z is CR
2, R
2Be H, Ar is pyridyl, pyrimidyl or pyrazinyl, R
3Be NR
6aR
7aThe time, R so
6aAnd R
7aCan not be H or alkyl;
(4) when A be N, Z is CR
2, R
2Be SO
2NR
6R
7The time, R so
3Can not be OH or SH;
(5) when A be CR, Z is CR
2, R so
2Can not be-NR
6SO
2R
7Or SO
2NR
6R
7
(6) when A be N, Z is CR
2, R
2Be NR
6SO
2R
7Or-SO
2NR
6R
7The time, R so
3Can not be OH or SH;
(7) when A be N, Z is CR
2, R
1Be methyl or ethyl, R
2Be H, R
3Be H, OH, CH
3, C
2H
5, C
6H
5, n-C
3H
7, i-C
3H
7, SH, SCH
3, NH (n-C
4H
9) or N (C
2H
5)
2The time, so Ar can not for unsubstituted phenyl or-aminomethyl phenyl;
(8) when A be CR, Z is CR
2, R
2Be H, phenyl or alkyl, R
3Be NR
8COR
7, when Ar is phenyl or the phenyl that replaced by thiophenyl, R so
7Can not be aryl, aryl (C
1-C
4Alkyl), heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
(9) when A be CR, Z is CR
2, R
2Be H or alkyl, Ar is a phenyl, R
3Be SR
13Or NR
6aR
7aThe time, R so
13Can not be aryl or heteroaryl, R
6aAnd R
7aCan not be H or aryl; Or
(10) when A be CH, Z is CR
2, R
1Be OR
11, R
2Be H, R
3Be OR
7, R
7And R
11When all being H, Ar can not be phenyl, p-Br-phenyl, p-Cl-phenyl, p-NHCOCH so
3-phenyl, p-CH
3-phenyl, pyridyl or naphthyl;
(11) when A be CH, Z is CR
2, R
2Be H, Ar is unsubstituted phenyl, R
3Be CH
3, C
2H
5, CF
3Or C
6H
4During F, R so
1Can not be CF
3Or C
2F
5
(12) when A be CR, R is H, Z is CR
2, R
2Be OH, R
1And R
3All be H, Ar can not be phenyl so;
(13) when A be CR, R is H, Z is CR
2, R
2Be OH or NH
2, R
1And R
3All be CH
3, Ar can not be 4-phenyl-3-cyano group-2-aminopyridine-2-base so.
[5] the preferred compound of the present invention be formula (1) and (2) compound and its isomer, steric isomer or steric isomer mixture with and pharmacy acceptable salt or prodrug, prerequisite is: (1) when A be N, R
1Be H, C
1-C
4Alkyl, halogen, CN, C
1-C
12Hydroxyalkyl, C
1-C
4Alkoxyalkyl or SO
2(C
1-C
4Alkyl), R
3Be NR
6aR
7a, R
6aBe unsubstituted C
1-C
4During alkyl, R so
7aCan not be phenyl, naphthyl, thienyl, benzothienyl, pyridyl, quinolyl, pyrazinyl, furyl, benzofuryl, benzothiazolyl, indyl or C
3-C
6Cycloalkyl; (2) A is N, R
1Be H, C
1-C
4Alkyl, halogen, CN, C
1-C
12Hydroxyalkyl, C
1-C
4Alkoxyalkyl or SO
2(C
1-C
4Alkyl), R
3Be NR
6aR
7a, R
7aBe unsubstituted C
1-C
4During alkyl, R so
6aCan not be phenyl, naphthyl, thienyl, benzothienyl, pyridyl, quinolyl, pyrazinyl, furyl, benzofuryl, benzothiazolyl, indyl or C
3-C
6Cycloalkyl.
[6] the preferred compound of the present invention also comprises the mixture of formula (1) and (2) compound and its isomer, steric isomer or steric isomer, with and pharmacy acceptable salt or prodrug, wherein Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, and each is optional by 1-4 R
4Substituting group replaces.
[7] the preferred compound of the present invention also comprises the mixture of formula (1) and (2) compound and its isomer, steric isomer or steric isomer, with and pharmacy acceptable salt or prodrug form, wherein A is N, Z is CR
2, Ar is a 2,4 dichloro benzene base, 2,4-3,5-dimethylphenyl or 2,4,6-trimethylphenyl, R
1And R
2Be CH
3, R
3Be NR
6aR
7a
[11] the preferred compound of the present invention is the mixture of such compound and its isomer, steric isomer or steric isomer, with and pharmacy acceptable salt or prodrug form, wherein A is N.
[12] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form.
[13] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, each Ar is optional by 1-4 R
4Substituting group replaces.
[14] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
3Be NR
6aR
7aOr OR
7
[15] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, each Ar is optional by 1-4 R
4Substituting group replaces, R
3Be NR
6aR
7aOr OR
7
[16] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein Z is CR
2
[17] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug, wherein Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, each Ar is optional by 1-4 R
4Substituting group replaces.
[18] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
3Be NR
6aR
7aOr OR
7
[19] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aIndependently be selected from:
-H,
-C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl)-, heteroaryl, heteroaryl (C
1-C
4Alkyl)-, heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl)-; With
R
7aIndependently be selected from:
-H,
-C
5-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl), heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
Perhaps, NR
6R
7And NR
6aR
7aIndependent is piperidines, tetramethyleneimine, piperazine, N methyl piperazine, morpholine or thiomorpholine, and each is optional by 1-3 C
1-C
4Alkyl replaces.
[20] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aIdentical and be selected from:
-C
1-C
4Alkyl or C
3-C
6Cycloalkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical; With
-aryl or heteroaryl.
[21] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug, wherein R
6aBe selected from:
-H,
-C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl), heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
R
7aBe selected from:
-C
1-C
4Alkyl, each C
1-C
4Alkyl independently is selected from following substituting group by 1-3 and replaces: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[22] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aOne of be selected from:
-C
3-C
6Cycloalkyl, each C
3-C
6Cycloalkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl,
-heteroaryl or
-heterocyclic radical, and R
6aAnd R
7aIn another be unsubstituted C
1-C
4Alkyl.
[23] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aIndependent is H or C
1-C
10Alkyl, each C
1-C
10Alkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, R
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[24] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, each Ar is optional by 1-4 R
4Substituting group replaces, R
3Be NR
6aR
7aOr OR
7
[25] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aIndependently be selected from:
-H,
-C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl)-, heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
R
7aIndependently be selected from:
-H,
-C
5-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl), heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
Perhaps, NR
6R
7And NR
6aR
7aIndependent is piperidines, tetramethyleneimine, piperazine, N methyl piperazine, morpholine or thiomorpholine, and each is optional by 1-3 C
1-C
4Alkyl replaces.
[26] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aIdentical and be selected from:
-C
1-C
4Alkyl or C
3-C
6Cycloalkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13,-COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical; With
-aryl or heteroaryl.
[27] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aIdentical and be:
-C
1-C
4Alkyl, each C
1-C
4Alkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13,-COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[28] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug, wherein R
6aBe selected from:
-H,
-C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl), heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
R
7aFor:
-C
1-C
4Alkyl, each C
1-C
4Alkyl independently is selected from following substituting group by 1-3 and replaces: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[29] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aOne of be selected from:
-C
3-C
6Cycloalkyl, each C
3-C
6Cycloalkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl,
-heteroaryl or
-heterocyclic radical, and R
6aAnd R
7aIn another be unsubstituted C
1-C
4Alkyl.
[30] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aIndependent is H or C
1-C
10Alkyl, each C
1-C
10Alkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, R
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[31] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein
-Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, and each Ar is optional by 1-4 R
4Substituting group replaces;
-R
3Be NR
6aR
7aOr OR
7And
-R
1And R
2Independently be selected from H, C
1-C
4Alkyl, C
3-C
6Cycloalkyl, C
4-C
10Cycloalkylalkyl.
[32] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aIndependently be selected from:
-H,
-C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl)-, heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
R
7aIndependently be selected from:
-H,
-C
5-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
15, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl), heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
Perhaps, NR
6R
7And NR
6aR
7aIndependent is piperidines, tetramethyleneimine, piperazine, N methyl piperazine, morpholine or thiomorpholine, and each is optional by 1-3 C
1-C
4Alkyl replaces.
[33] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aIdentical and be selected from:
-C
1-C
4Alkyl or C
3-C
6Cycloalkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13,-COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical; With
-aryl or heteroaryl.
[34] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug, wherein R
6aAnd R
7aIdentical and be:
-C
1-C
4Alkyl, each C
1-C
4Alkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[35] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug, wherein R
6aBe selected from:
-H,
-C
1-C
10Alkyl, C
3-C
10Alkenyl, C
3-C
10Alkynyl, has the C of 1-10 halogen atom
1-C
10Haloalkyl, C
2-C
8Alkoxyalkyl, C
3-C
6Cycloalkyl, C
4-C
12Cycloalkylalkyl, C
5-C
10Cycloalkenyl group or C
6-C
14Cycloalkenyl alkyl, each is chosen wantonly by 1-3 and independently is selected from following substituting group replacement: C
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl, aryl (C
1-C
4Alkyl), heteroaryl, heteroaryl (C
1-C
4Alkyl), heterocyclic radical or heterocyclic radical (C
1-C
4Alkyl);
R
7aFor:
-C
1-C
4Alkyl, each C
1-C
4Alkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[36] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aOne of be selected from:
-C
3-C
6Cycloalkyl, each C
3-C
6Cycloalkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, NR
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical;
-aryl,
-heteroaryl or
-heterocyclic radical, and R
6aAnd R
7aIn another be unsubstituted C
1-C
4Alkyl.
[37] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aIndependent is H or C
1-C
10Alkyl, each C
1-C
10Alkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, R
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[38] the particularly preferred compound of the present invention be formula (50) compound and its isomer, steric isomer or steric isomer mixture with and pharmacy acceptable salt or prodrug form:
Formula (50)
They are selected from: R wherein3For-NHCH (n-Pr)2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et) (n-Bu), R4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-(n-Pr) (CH2cPr),R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NNCH (Et) (n-Bu), R4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et) (CH2OMe),R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OEt)
2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Me) (Ph), R4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (n-Pr)2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et) (n-Pr), R4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for Me; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et) (CH2OMe),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-OEt, R4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CN)
2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Me) (CH2OMe),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-OCH (Et) (CH2OMe),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (n-Pr) (CH2cPr),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Me) (CH2N(Me)
2),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (cPr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (n-Pr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (n-Bu) (CH2CN),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et) (CH2OMe),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for Me; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for Me; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for Me; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Br, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et) (CH2OMe),R
4aFor Br, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for Me; R wherein3For-NHCH (CH2OEt)
2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for Me; R wherein3For-NHCH (CH2CH
2OMe)(CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for Me; R wherein3For morpholino, R4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Br, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Br, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Br, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NH (c-Pr), R4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor CN, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (c-Pr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for Me; R wherein3For-NCH (CH2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Br, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)(CH
2CH
2OMe),R
4aFor Me, R4bFor H, R4cFor Br, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor Me, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor Me, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor Me, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor Me, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et) (CH2OMe),R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)(CH
2CH
2OMe),R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (c-Pr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor Me, R4eFormula (50) compound for H; R wherein3For-N (c-Pr) (CH2CH
2CN),R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For (S)-NHCH (CH2OMe)(CH
2CH
2OMe),R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)(CH
2CH
2OMe),R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor H, R4cFor Br, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Br, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NH (CH2OMe)(CH
2-iPr),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor H, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor NMe2,R
4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)(n-Pr),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OEt)(Et),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)(CH
2CH
2OMe),R
4aFor Me, R4bFor H, R4cFor NMe2,R
4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Me, R4bFor H, R4cFor Br, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor H, R4cFor NMe2,
R
4dFor H, R4eFormula (50) compound for H; R wherein3For (S)-NHCH (CH2OMe)(CH
2CH
2OMe),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)(CH
2CH
2OMe),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (50) compound for H; R wherein3For (S)-NHCH (CH2OMe)(CH
2CH
2OMe),R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4cFormula (50) compound for H; R wherein3For-NHCH (CH2OMe)(CH
2CH
2OMe),R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (c-Pr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NH (Et) (CH2CN),R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Me, R4bFor Me, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)(CH
2CH
2OH),R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor Me, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor Me, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2c-Pr)(n-Pr),R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (c-Pr) (CH2CH
2CN),R
4aFor Me, R4bFor Me, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Cl, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Cl, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Cl, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (Et) (CH2OMe),R
4aFor Cl, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (Et)2,R
4aFor Cl, R4bFor H, R4cFor CN, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (c-Pr) (CH2CH
2CN),R
4aFor Cl, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H; R wherein3For-NHCH (CH2OH)
2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (50) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (50) compound for H.
[39] more particularly preferred compound is 4-(two-(2-methoxy ethyl) amino)-2,7-dimethyl-8-(2-methyl-4-p-methoxy-phenyl)-[1,5-a]-pyrazolo-1,3, the mixture of 5-triazine and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form.
[40] more particularly preferred compound is 4-(two-(2-methoxy ethyl) amino)-2,7-dimethyl-8-(2,5-dimethyl-4-p-methoxy-phenyl)-[1,5-a]-pyrazolo-1,3, the mixture of 5-triazine and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug.
[41] the preferred compound of the present invention be such compound and its isomer, steric isomer or steric isomer mixture with and pharmacy acceptable salt or prodrug form, wherein A is CR.
[42] the preferred compound of the present invention mixture that also comprises all cpds and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form.
[43] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, each Ar is optional by 1-4 R
4Substituting group replaces.
[44] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
3Be NR
6aR
7aOr OR
7
[45] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, each Ar is optional by 1-4 R
4Substituting group replaces, and R
3Be NR
6aR
7aOr OR
7
[46] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein Z is CR
2
[47] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug, wherein Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, each Ar is optional by 1-4 R
4Substituting group replaces.
[48] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
3Be NR
6aR
7aOr OR
7
[49] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, each Ar is optional by 1-4 R
4Substituting group replaces, and R
3Be NR
6aR
7aOr OR
7
[50] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aIndependent is H or C
1-C
10Alkyl, each C
1-C
10Alkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, R
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[51] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug, wherein
-Ar is phenyl, pyridyl or 2, the 3-dihydro benzo furyl, and each Ar is optional by 1-4 R
4Substituting group replaces;
-R
3Be NR
6aR
7aOr OR
7And
-R
1And R
2Independently be selected from H, C
1-C
4Alkyl, C
3-C
6Cycloalkyl, C
4-C
10Cycloalkylalkyl.
[52] the preferred compound of the present invention mixture that also comprises such compound and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form, wherein R
6aAnd R
7aIndependent is H or C
1-C
10Alkyl, each C
1-C
10Alkyl is optional independently to be selected from following substituting group replacement: C by 1-3
1-C
6Alkyl, C
3-C
6Cycloalkyl, halogen, C
1-C
4Haloalkyl, cyano group, OR
15, SH, S (O)
nR
13, COR
15, CO
2R
15, OC (O) R
13, NR
8COR
15, N (COR
15)
2, R
8CONR
16R
15, NR
8CO
2R
13, NR
16R
15, CONR
16R
15, aryl, heteroaryl or heterocyclic radical.
[53] the particularly preferred compound of the present invention be formula (51) compound and its isomer, steric isomer or steric isomer mixture with and pharmacy acceptable salt or prodrug:
Formula (51)
They are selected from: R wherein3For-NHCH (n-Pr)2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (c-Pr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4cFormula (51) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4cFormula (51) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (Et)2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (n-Pr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (n-Bu) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (n-Pr) (CH2OMe),R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H; R wherein3For (S)-NH (CH2CH
2OMe)CH
2OMe,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NH (CH2CH
2OMe)CH
2OMe,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NH (Et), R4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (n-Pr)2,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For (S)-NH (CH2CH
2OMe)CH
2OMe,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NH (CH2CH
2OMe)CH
2OMe,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (n-Pr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (Et)2,R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H; R wherein3For (S)-NH (CH2CH
2OMe)CH
2OMe,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NH (CH2CH
2OMe)CH
2OMe,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (Et)2,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (c-Pr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (c-Pr) (CH2CH
2CN),R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (n-Pr) (CH2OMe),R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (n-Pr) (CH2OMe),R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Br, R4bFor H, R4cFor OMe, R4dFor OMe, R4eFormula (51) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Br, R4bFor H, R4cFor OMe, R4dFor H, R4cFormula (51) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Br, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Br, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (Et)2,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (Et)2,R
4aFor Cl, R4bFor H, R4cFor OMe, R4dFor OMe, R4eFormula (51) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Cl, R4bFor H, R4cFor OMe, R4dFor OMe, R4cFormula (51) compound for H; R wherein3For-N (CH2CH
2OMe)
2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (CH2OMe)
2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (Pr) (CH2CH
2CN),R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (Bu) (Et), R4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (Et) CH2OMe,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Cl, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Cl, R4bFor H, R4cFor Me, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NHCH (Et)2,R
4aFor Me, R4bFor H, R4cFor Cl, R4dFor H, R4eFormula (51) compound for H; R wherein3For-NEt2,R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H; R wherein3For-N (Pr) (CH2CH
2CN),R
4aFor Me, R4bFor H, R4cFor OMe, R4dFor H, R4eFormula (51) compound for H.
[54] more particularly preferred compound is 7-(3-penta amino)-2, the mixture of 5-dimethyl-3-(2-methyl-4-p-methoxy-phenyl)-[1,5-a]-pyrazolopyrimidine and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form.
[55] more particularly preferred compound is 7-(diethylin)-2, the mixture of 5-dimethyl-3-(2-methyl-4-p-methoxy-phenyl)-[1,5-a] pyrazolopyrimidine and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form.
[56] more particularly preferred compound is 7-(N-(3-cyano group propyl group)-N-third amino)-2,5-dimethyl-3-(2, the 4-3,5-dimethylphenyl)-[1,5-a] mixture of pyrazolopyrimidine and its isomer, steric isomer or steric isomer with and pharmacy acceptable salt or prodrug form.
The present invention also provides the medicinal compositions that contains formula (1) and (2) compound and pharmaceutically acceptable carrier.
Many compounds of the present invention have one or more asymmetric centers or plane.Except that specializing, the present invention includes all chiralitys (enantiomorph and diastereomer) and racemic form.Also can have the multiple geometrical isomer of alkene, the two keys of C=N etc. in the compound, all these type of desmotropes all comprise in the present invention.Can separate described compound with opticity or racemic form.The well known opticity form that how to prepare is for example synthesized by the fractionation of racemic form or by the opticity raw material.Except that specializing specific stereochemistry or isomeric forms, comprise all geometrical isomer forms of all chiralitys (enantiomorph and diastereomer) and racemic form and structure.
Term " alkyl " comprises having specific carbonatoms purpose side chain and straight chained alkyl.Common being abbreviated as of using: Me is methyl, and Et is an ethyl, and Pr is a propyl group, and Bu is a butyl.Prefix " n " expression straight chained alkyl.Prefix " c " representative ring alkyl.Prefix " (S) " expression S enantiomorph, prefix " (R) " expression R enantiomorph." alkenyl " comprises the hydrocarbon chain of straight or branched configuration, can have one or more unsaturated C-Cs, for example vinyl, propenyl etc. at any stable point on this chain." alkynyl " comprises the hydrocarbon chain of straight or branched configuration, can have one or more carbon-to-carbon triple bonds, for example ethynyl, proyl etc. at any stable point on this chain." haloalkyl " is intended to comprise side chain and the straight chained alkyl that has the particular carbon atom number, replaced by one or more halogen atoms; " alkoxyl group " representative is by the alkyl of the particular carbon atom number of oxo bridge connection; " cycloalkyl " be intended to comprise saturated cyclic group, comprises one, two or polycyclic system, for example cyclopropyl, cyclobutyl, cyclopentyl, cyclohexyl etc." halo " or " halogen atom " comprises fluorine, chlorine, bromine and iodine.
Replace for the group that the one or more hydrogen on the specified atom are selected from the designated groups in this used term " replacement " meaning, its prerequisite is the common rate that is no more than specified atom, and should replacement produce stable compound.When substituting group is that ketone (promptly=O) time, has two hydrogen to be substituted on described atom so.
As long as the combination results stable compound of substituting group and/or replacement, then this combination is allowed to.The meaning of " stable compound " or " rock steady structure " is separated into the purity of useful degree and makes effective medicine with experience for enough stable from reaction mixture.
Term " suitable amino acid blocking group " refers to the known any group that is used to protect amine or hydroxy-acid group in the organic synthesis field.This type of amine protecting group group comprises that Greene and Wuts are at " Protective Groups in Organic Synthesis " (John Wiley﹠amp; Sons, NewYork (1991)) and those groups described in " The Peptides:Analysis, Syntheis, Biology, Vol.3, Academic Press, New York (1981) ", it is for referencial use to be incorporated herein its disclosed content.Can use any amine protecting group known in the art group.The example of amine protecting group group includes, but is not limited to: 1) for example formyl radical, trifluoroacetyl group, phthaloyl and ptoluene-sulfonyl of acyl group type; 2) for example benzyloxycarbonyl (Cbz) and the benzyloxycarbonyl, 1-(right-xenyl)-1-methyl ethoxy carbonyl and the 9-fluorenyl methoxy carbonyl (Fmoc) that replace of fragrant carbamic acid ester type; 3) for example tert-butoxycarbonyl (Boc), ethoxy carbonyl, di-isopropyl methoxycarbonyl and allyloxy carbonyl of aliphatic carbamate type; 4) for example cyclopentyloxy carbonyl and adamantyl oxygen base carbonyl of cycloalkyl amino manthanoate type; 5) for example trityl and benzyl of alkyl type; 6) trialkyl silane trimethyl silane for example; And 7) contain hydroxyl sulfenyl type for example thiophenyl carbonyl and dithio succinyl.
Term " pharmacy acceptable salt " comprises the acid or the alkali salt of formula (1) and (2) compound.The example of pharmacy acceptable salt includes, but is not limited to the alkaline residue for example mineral acid or the organic acid salt of amine; Acidic residues is the basic metal of carboxylic acid or organic salt etc. for example.
Suitable alkali that can be by making these compound free acids or alkali form and stoichiometric quantity or acid water or in organic solvent or mixture at both the pharmacy acceptable salt of prepared in reaction The compounds of this invention, described solvent generally is preferably non-aqueous media as ether, ethyl acetate, ethanol, Virahol or acetonitrile.Suitable salt is seen Remington ' s PharmaceuticalSciences (17 th ed., Mack Publishing Company, Easton, PA, 1985, the 1418 pages), and it is for referencial use to be incorporated herein its disclosed content.
Think the carrier that " prodrug " links to each other for any covalency, when giving mammalian subject with it, this type of medicine in vivo can release type (I) or (II) active parent drug.Can by the method for routine or in vivo the cracking modification group mode that becomes parent compound modify functional group in the described compound, and the preparation formula (I) and (II) prodrug of compound.Prodrug comprises such compound, and wherein hydroxyl, amine or sulfydryl link to each other with any group that can cracking when giving the mammalian subject medicine forms free hydroxyl, amino or sulfydryl respectively.The example of prodrug includes, but is not limited to formula (I) and (II) acetic ester, manthanoate and the benzoate derivatives etc. of the alkohol and amine functional group of compound.
Term " the treatment significant quantity " compound of the present invention refers to the amount of effective antagonism CRF abnormal level or treatment host affective disorder, anxiety disorder or dysthymia disorders.
Synthetic
According to the method shown in the flow process 1, can prepare segment bounds (1) compound with formula (7) compound intermediate:
Flow process 1
(7)Y=O (8)
(1) A=N
In the presence of alkali or alkali-free; exist or do not exist under the inert solvent; between-80 ℃ to 250 ℃ temperature of reaction; handle formula (7) compound (wherein Y is O) with halogenating agent or sulfonyl agent, obtain formula (8) product (wherein X is halogen, alkane sulfonyloxy, aryl-sulfonyl oxygen or haloalkane-sulfonyloxy).Halogenating agent includes, but is not limited to SOCl
2, POCl
3, PCl
3, PCl
5, POBr
3, PBr
3Or PBr
5Sulfonyl agent includes, but is not limited to alkane sulfonic acid halide or acid anhydrides (for example methylsulfonyl chloride or methylsulfonic acid acid anhydride), aryl sulfonyl halide or acid anhydrides (for example right-tolylsulfonyl oxygen or acid anhydrides) or haloalkyl sulfonic acid halide or acid anhydrides (preferred trifluoromethanesulfanhydride anhydride).Alkali includes, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine or triethylamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, the haloalkane (preferred methylene dichloride) of N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Preferable reaction temperature is-20 ℃ to 100 ℃.
In the alkali existence or not,, between-80 ℃ to 250 ℃ temperature of reaction, can make formula (8) compound and formula R in the inert solvent existence or not
3H (R wherein
3Identical with above-mentioned definition, but R
3Be not SH, COR
7, CO
2R
7, aryl or heteroaryl) compound reacting generating (1) compound.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, alkali metal hydrocarbonate, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), the haloalkane (preferred methylene dichloride) of aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Preferable reaction temperature is 0 ℃ to 140 ℃.
Flow process 2 is described the method that formula (7) midbody compound (wherein Y is S) is converted into segment bounds (1) compound:
Flow process 2
In the alkali existence or not,, between-80 ℃ to 250 ℃ temperature of reaction, can use alkylating agent R in the inert solvent existence or not
13X (R wherein
13Identical with above-mentioned definition, but R
13Be not aryl or heteroaryl) processing formula (7) compound (wherein Y is S).Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, alkali metal hydroxide, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine or triethylamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), the haloalkane (preferred methylene dichloride) of aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Preferable reaction temperature is-80 ℃ to 100 ℃.
Use then that above-mentioned flow process 1 is described to be converted into the same terms and the reagent of formula (1) compound with formula (8) compound, make formula (12) compound (R wherein
3Be SR
13Formula (1) compound) with formula R
3The reaction of H compound obtains formula (1) compound.Perhaps, in the presence of inert solvent, between-80 ℃ to 250 ℃ temperature, by with oxidizer treatment with formula (12) compound (R wherein
3Be SR
13Formula (1) compound) be oxidized to formula (13) compound (R wherein
3Be S (O)
nR
13, n is 1,2 formula (1) compound).Oxygenant comprises (but being not limited to) hydrogen peroxide, alkyl or aryl peracid (preferred acetic hydroperoxide or m-chloro-peroxybenzoic acid), diepoxide for example, oxone or sodium periodate.Inert solvent includes, but is not limited to the haloalkane (preferred methylene dichloride) or their mixture of alkane ketone (3-10 carbon atom, preferred acetone), water, alkyl alcohol (1-6 carbon atom), aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Oxygenant and choice of Solvent are well known to those skilled in the art (referring to Uemura, S., Oxidation of Sulfur, Selenium and Tellurium, in Comprehensive Organic Synthesis, Trost, B.M.ed., (Elmsford, NY:Pergamon Press, 1991), 7,762-769).Preferable reaction temperature is-20 ℃ to 100 ℃.Use then shown in the above-mentioned flow process (1) formula (8) compound to be converted into the used the same terms of formula (1) compound, make formula (13) compound (R wherein
3Be S (O)
nR
13, n is 1,2 formula (1) compound) and formula R
3The reaction of H compound obtains formula (1) compound.
According to the method shown in the flow process 3, can be by formula (7) compound (wherein Y is NH) preparation formula (1) compound, wherein R
3Can be-NR
8COR
7,-N (COR
7)
2,-NR
8CONR
6R
7,-NR
8CO
2R
13,-NR
6R
7,-NR
8SO
2R
7:
Flow process 3
(7)Y=NH (1)
A=N;
R
3=NR
6R
7,NR
8COR
7,
N(COR
7)
2,NR
8CONR
6R
7,
NR
8CO
2R
13
Being in or be not in alkali exists down; in inert solvent, between-80 ℃ to 250 ℃ temperature of reaction, making Y wherein is formula (7) compound of NH and alkylating agent, sulfonyl agent or acylation reaction or order and their composite reaction; can obtain formula (1) compound, wherein R
3Can be-NR
8COR
7,-N (COR
7)
2,-NR
8CONR
6R
7,-NR
8CO
2R
13,-NR
6R
7,-NR
8SO
2R
7Alkylating agent can include, but is not limited to C
1-C
10Alkyl-halogenide ,-tosylate ,-methanesulfonates or-triflate; C
1-C
10Haloalkyl (1-10 halogen atom)-halogenide ,-tosylate ,-methanesulfonates or-triflate; C
2-C
8Alkoxyalkyl-halogenide ,-tosylate ,-methanesulfonates or-triflate; C
3-C
6Cycloalkyl-halogenide ,-tosylate ,-methanesulfonates or-triflate; C
4-C
12Cycloalkylalkyl-halogenide ,-tosylate ,-methanesulfonates or-triflate; Aryl (C
1-C
4Alkyl)-halogenide ,-tosylate ,-methanesulfonates or-triflate; Heteroaryl (C
1-C
4Alkyl)-halogenide ,-tosylate ,-methanesulfonates or-triflate; Or heterocyclic radical (C
1-C
4Alkyl)-halogenide ,-tosylate ,-methanesulfonates or-triflate.Acylating agent includes, but is not limited to C
1-C
10Alkane carboxylic acid halides or acid anhydrides, has the C of 1-10 halogen atom
1-C
10Halogenated alkane carboxylic acid halides or acid anhydrides, C
2-C
8Alkoxyl group alkane carboxylic acid halides or acid anhydrides, C
3-C
6Cycloalkyl alkane carboxylic acid halides or acid anhydrides, C
4-C
12Cycloalkyl alkane carboxylic acid halides or acid anhydrides, fragrant carboxylic acid halides or acid anhydrides, aryl (C
1-C
4) alkane carboxylic acid halides or acid anhydrides, assorted fragrant carboxylic acid halides or acid anhydrides, heteroaryl (C
1-C
4) alkane carboxylic acid halides or acid anhydrides, heterocycle carboxylic acid halides or acid anhydrides or heterocyclic radical (C
1-C
4) alkane carboxylic acid halides or acid anhydrides.Sulfonyl agent includes, but is not limited to C
1-C
10Heteroaryl-alkylsulfonyl halides or acid anhydrides, has the C of 1-10 halogen atom
1-C
10Haloalkyl sulfonic acid halide or acid anhydrides, C
2-C
8Alkoxyalkyl sulfonic acid halide or acid anhydrides, C
3-C
6Naphthene sulfamide halogen or acid anhydrides, C
4-C
12Cycloalkylalkyl sulfonic acid halide or acid anhydrides, aryl sulfonyl halide or acid anhydrides, aryl (C
1-C
4Alkyl)-, heteroaryl sulfonic acid halide or acid anhydrides, heteroaryl (C
1-C
4Alkyl) sulfonic acid halide or acid anhydrides, heterocyclic radical sulfonic acid halide or acid anhydrides or heterocyclic radical (C
1-C
4Alkyl) sulfonic acid halide or acid anhydrides.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl ethamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is 0 ℃ to 100 ℃.
Flow process 4 is described and can be used for preparation formula (7) midbody compound (wherein Y is O, S, and Z is CR
2) method:
Flow process 4
(7)Y=O,S;Z=CR
2
In the presence of alkali, in inert solvent, between-78 ℃ to 200 ℃ temperature of reaction, make formula ArCH
2CN compound and formula R
2COR
b(R wherein
2Identical with above-mentioned definition, R
bBeing halogen atom, cyano group, lower alkoxy (1-6 carbon atom) or lower alkane acyloxy (1-6 carbon atom)) compound reaction obtains formula (3) compound.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, alkali metal hydroxide, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), water, dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is 0 ℃ to 100 ℃.
In the presence of inert solvent,, in preferred 70 ℃ to the 150 ℃ temperature ranges, handle formula (3) compound production (4) compound with hydrazine-hydrate in 0 ℃ to 200 ℃.Inert solvent includes, but is not limited to water, alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Be in or be not in acid and exist down, in inert solvent, in 0 ℃ to 200 ℃ temperature range, can make formula (4) compound and formula (5) compound (R wherein
cBe alkyl (1-6 carbon atom)) reacting generating (6) compound.Acid can include, but is not limited to paraffinic acid (preferred acetate), halogenated-chain acid (2-10 carbon atom, a 1-10 halogen atom, for example trifluoroacetic acid), the aryl sulfonic acid (preferably right-toluenesulphonic acids or Phenylsulfonic acid) of 2-10 carbon atom, alkylsulphonic acid (preferably methylsulfonic acid), hydrochloric acid, sulfuric acid or the phosphoric acid of a 1-10 carbon atom.Can use this type of acid of stoichiometric quantity or catalytic amount.Inert solvent includes, but is not limited to water, alkyl nitrile (1-6 carbon atom, preferred acetonitrile), for example dioxane or tetrahydrofuran (THF) of the alkyl alcohol (preferred alcohol) of the halohydrocarbon of a 1-6 carbon atom and 1-6 halogen atom (preferably methylene dichloride or chloroform), a 1-10 carbon atom, dialkyl ether (4-12 carbon atom, preferably ether or Di Iso Propyl Ether) or cyclic ethers.Preferred temperature range is a room temperature to 100 ℃.
Be in or be not in alkali and exist down, in inert solvent, between-50 ℃ to 200 ℃ temperature of reaction, with Compound C=Y (R
d)
2(wherein Y is O or S, R
dBe halogen atom (preferred chlorine), alkoxyl group (1-4 carbon atom) or alkylthio (1-4 carbon atom)) handle, formula (6) compound can be converted into formula (7) midbody compound.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline carbonate, alkali metal hydroxide, trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine or triethylamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is 0 ℃ to 150 ℃.
According to method shown in the flow process 5, can synthesis type (7) midbody compound, wherein Z is N:
Flow process 5
(7)Y=O,S;Z=N
Be in or be not in alkali and exist down, in inert solvent, in 0 ℃ to 200 ℃ temperature range, make ArCH
2CN compound and formula R
qCH
2N
3Compound (R wherein
qBe the optional phenyl that is replaced by H, alkyl (1-6 carbon atom) or alkoxyl group (1-6 carbon atom)) reacting generating (9) compound.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium, sodium ethylate or potassium tert.-butoxide), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, alkali metal hydroxide, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine or triethylamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is a room temperature to 100 ℃.
In inert solvent, between-100 ℃ to 100 ℃ temperature, can handle formula (9) compound with reductive agent and obtain formula (10) product.Reductive agent includes, but is not limited to (a) hydrogen and noble metal catalyst, for example palladium charcoal, PtO
2, platinum charcoal, rhodium-aluminum oxide or Raney nickel combination, (b) basic metal (preferred sodium) and the combination of liquefied ammonia or (c) ceric ammonium nitrate.Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), water, dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is-50 ℃ to 60 ℃.Then, use formula (4) compound is converted into formula (7) compound (wherein Z is CR shown in the flow process 4
2) agents useful for same and reaction conditions, through formula (11) intermediate formula (9) compound is converted into formula (7) compound (wherein Z is N).
Shown in flow process 6, also can be by formula (7) compound (wherein Y is O, S, and Z is identical with above-mentioned definition) preparation formula (1) compound:
Flow process 6
(7)Y=O,S;Z=N,CR
2 (1)A=N
In the presence of dewatering agent, in inert solvent, in 0 ℃ to 250 ℃ range of reaction temperature, can make formula (7) compound and formula R
3The reaction of H compound.Dewatering agent includes, but is not limited to P
2O
5, molecular sieve or inorganic or organic acid.Acid can include, but is not limited to paraffinic acid (preferred acetate), the aryl sulfonic acid (preferably right-toluenesulphonic acids or Phenylsulfonic acid) of 2-10 carbon atom, alkylsulphonic acid (preferably methylsulfonic acid), hydrochloric acid, sulfuric acid or the phosphoric acid of a 1-10 carbon atom.Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred glyme or diglyme), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), the halohydrocarbon (preferably chloroform) of aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Preferred temperature of reaction is a room temperature to 150 ℃.
According to the method shown in the flow process 7, also can prepare segment bounds (1) compound (wherein A is N):
Flow process 7
Be in or be not in acid and exist down, in inert solvent, in 0 ℃ to 250 ℃ range of reaction temperature, can make formula (14) midbody compound (wherein Z is identical with above-mentioned definition) and formula R
3C (OR
e)
3(R wherein
eCan be alkyl (1-6 carbon atom)) the compound reaction.Acid can include, but is not limited to paraffinic acid (preferred acetate), the aryl sulfonic acid (preferably right-toluenesulphonic acids or Phenylsulfonic acid) of 2-10 carbon atom, alkylsulphonic acid (preferably methylsulfonic acid), hydrochloric acid, sulfuric acid or the phosphoric acid of a 1-10 carbon atom.Can use this type of acid of stoichiometric quantity or catalytic amount.Inert solvent includes, but is not limited to low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, the halohydrocarbon (preferably methylene dichloride) of N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Preferred temperature of reaction is 50 ℃ to 150 ℃.
According to the reaction shown in the flow process 8, also can synthesis type (7) midbody compound:
Flow process 8
Be in or be not in organo-metallic catalyst and exist down, alkali exist or not in the presence of, in inert solvent, in-100 ℃ to 200 ℃ temperature ranges, (wherein Y is OH, SH, NR can to make formula (15) compound
6R
7Z is identical with above-mentioned definition, and X is Br, Cl, I, O
3SCF
3Or B (OR " ")
2, and R " " be H or alkyl (1-6 carbon atom)) (wherein M is halogen atom, basic metal, ZnCl, ZnBr, ZnI, MgBr, MgCl, MgI, CeCl with formula ArM
2, CeBr
2Or copper halide) compound reaction.Those skilled in the art will recognize that reagent A rM can produce on the spot.Organo-metallic catalyst includes, but is not limited to palladium phosphine composition (Pd (PPh for example
3)
4), palladium halogenide or alkanoate (PdCl for example
2(PPh
3)
2Or Pd (OAc)
2) or nickel complex (NiCl for example
2(PPh
3)
2).Alkali can include, but is not limited to alkaline carbonate or trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine or triethylamine).Inert solvent includes, but is not limited to dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), aromatic hydrocarbon (preferred benzene or toluene) or water.Preferable reaction temperature is-80 ℃ to 100 ℃.The selection of M and X is known (referring to Imamoto, T., Organocerium Reagents in to those skilled in the art
Comprehensive Organic Synthesis, Trost, B.M.ed., (Elmsford, NY:Pergamon Press, 1991), 1,231-250; Knochel, P., Organozinc, Organocadmium and Organomercury Reagents in
Comprehensive Organic Synthesis, Trost, B.M.ed., (Elmsford, NY:Pergamon Press, 1991), 1,211-230; Knight, D.W., Coupling Reactionsbetween sp
2Carbon Centers, in
Comprehensive Organic Synthesis, Trost, B.M.ed., (Elmsford, NY:Pergamon Press, 1991), 3,481-520).According to the method shown in the flow process 9, also can preparation formula (1) compound:
(16)X=Br,Cl,I, (1)
B(OR″″)
2,O
3SCF
3
Be in or be not in organo-metallic catalyst and exist down, alkali exist or not in the presence of, in inert solvent, in-100 ℃ to 200 ℃ temperature ranges, can make formula (16) compound (wherein A, Z, R
1And R
3Identical with above-mentioned definition, X is Br, Cl, I, O
3SCF
3Or B (OR " ")
2, and R " " be H or alkyl (1-6 carbon atom)) (wherein M is halogen atom, basic metal, ZnCl, ZnBr, ZnI, MgBr, MgCl, MgI, CeCl with formula ArM
2, CeBr
2Or copper halide) compound reaction.Those skilled in the art will recognize that reagent A rM can produce on the spot (sees
Comprehensive Organic SynthesisIn above-mentioned reference).Organo-metallic catalyst includes, but is not limited to palladium phosphine composition (Pd (PPh for example
3)
4), palladium halogenide or alkanoate (PdCl for example
2(PPh
3)
2Or Pd (OAc)
2) or nickel complex (NiCl for example
2(PPh
3)
2).Alkali can include, but is not limited to alkaline carbonate or trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine or triethylamine).Inert solvent includes, but is not limited to dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), aromatic hydrocarbon (preferred benzene or toluene) or water.Preferable reaction temperature is-80 ℃ to 100 ℃.
Shown in flow process 10, can preparation formula (7) midbody compound (wherein Y is O, S, NH, and Z is CR
2, R
1, R
2Identical with Ar with above-mentioned definition):
Flow process 10
(7)Y=O,S,NH;Z=CR
2,
Be in or be not in alkali or acid and exist down, in inert solvent, in 0 ℃ to 250 ℃ temperature range, can make formula (3) compound and formula H
2NNH (C=Y) NH
2(wherein Y is O, S or NH) compound reacting generating (17) compound.Acid can include, but is not limited to paraffinic acid (preferred acetate), the aryl sulfonic acid (preferably right-toluenesulphonic acids or Phenylsulfonic acid) of 2-10 carbon atom, alkylsulphonic acid (preferably methylsulfonic acid), hydrochloric acid, sulfuric acid or the phosphoric acid of a 1-10 carbon atom.Can use this type of acid of stoichiometric quantity or catalytic amount.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine or triethylamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-6 carbon atom), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, the haloalkane (preferred methylene dichloride) of N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.
Preferable reaction temperature is 0 ℃ to 150 ℃.Be in or be not in acid then and exist down, in inert solvent, in 0 ℃ to 250 ℃ range of reaction temperature, can make formula (17) compound and formula R
3C (OR
e)
3(R wherein
eCan be alkyl (1-6 carbon atom)) the compound reaction.Acid can include, but is not limited to paraffinic acid (preferred acetate), the aryl sulfonic acid (preferably right-toluenesulphonic acids or Phenylsulfonic acid) of 2-10 carbon atom, alkylsulphonic acid (preferably methylsulfonic acid), hydrochloric acid, sulfuric acid or the phosphoric acid of a 1-10 carbon atom.Can use this type of acid of stoichiometric quantity or catalytic amount.Inert solvent includes, but is not limited to low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, the halohydrocarbon (preferably methylene dichloride) of N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Preferred temperature of reaction is 50 ℃ to 150 ℃.
Flow process 11 is depicted as: in inert solvent, and in-80 ℃ to 250 ℃ temperature ranges, can be by handling with class formula (a 1) compound (R wherein with reductive agent
3Be COR
7, CO
2R
7, NR
8COR
7And CONR
6R
7) be converted into another kind of formula (1) compound (R wherein
3Be CH (OH) R
7, CH
2OH, NR
8CH
2R
7And CH
2NR
6R
7) method:
Flow process 11
(1)R
3=COR
7,CO
2R
7, (1)R
3=C(OH)R
7,
CONR
6R
7 CH
2OH,
CH
2NR
6R
7
Reductive agent includes, but is not limited to basic metal or alkaline-earth metal borohydride (preferred lithium borohydride or sodium borohydride), borane, dialkyl group borane (for example two-isopentyl borane), composite alkali aluminum hydride (preferred lithium aluminum hydride), basic metal (tri-alkoxy) alanate or dialkyl aluminum hydride (for example Di-Isobutyl alanate).Inert solvent includes, but is not limited to alkyl alcohol (1-6 carbon atom), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1,4-dioxane), aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is-80 ℃ to 100 ℃.
In flow process 12, be depicted as in inert solvent, in-80 ℃ to 250 ℃ temperature ranges, by using formula R
7The M agent treated can be with class formula (a 1) compound (R wherein
3Be COR
7Or CO
2R
7) be converted into another kind of formula (1) compound (R wherein
3Be C (OH) (R
7)
2Method:
Flow process 12
(1)R
3=COR
7,CO
2R
7, (1)R
3=C(OH)(R
7)
2
M is halogen atom, basic metal, ZnCl, ZnBr, ZnI, MgBr, MgCl, MgI, CeCl
2, CeBr
2Or copper halide.Inert solvent includes, but is not limited to dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF)) or aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is-80 ℃ to 100 ℃.
As described in flow process 13, can synthesis type (1) compound, wherein R
3For-NR
8COR
7,-N (COR
7)
2,-NR
8CONR
6R
7,-NR
8CO
2R
13,-NR
6R
7,-NR
8SO
2R
7:
Flow process 13
(4)Z=CR
2
(10)Z=N
A=CR
R
3=NR
6R
7,NR
8COR
7,
N(COR
7)
2,
NR
8CONR
6R
7,
NR
8CO
2R
13
Be in or be not in alkali and exist down, in inert solvent, in-50 ℃ to 250 ℃ temperature ranges, make formula (18) compound (wherein R and R
1Identical with above-mentioned definition) and formula (4) or formula (10) compound reacting generating (19) compound.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred two-sec.-propyl ethamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Preferred range of reaction temperature is 0 ℃ to 100 ℃.
Be in or be not in alkali and exist down, in inert solvent, between-80 ℃ to 250 ℃ temperature of reaction, make formula (19) compound and alkylating agent, sulfonyl agent or acylation reaction or in proper order with their composite reaction, can obtain formula (1) compound, wherein R
3Can be-NR
8COR
7,-N (COR
7)
2,-NR
8CONR
6R
7,-NR
8CO
2R
13,-NR
6R
7,-NR
8SO
2R
7Alkylating agent can include, but is not limited to C
1-C
10Alkyl-halogenide ,-tosylate ,-methanesulfonates or-triflate; C
1-C
10Haloalkyl (1-10 halogen atom)-halogenide ,-tosylate ,-methanesulfonates or-triflate; C
2-C
8Alkoxyalkyl-halogenide ,-tosylate ,-methanesulfonates or-triflate; C
3-C
6Cycloalkyl-halogenide ,-tosylate ,-methanesulfonates or-triflate; C
4-C
12Cycloalkylalkyl-halogenide ,-tosylate ,-methanesulfonates or-triflate; Aryl (C
1-C
4Alkyl)-halogenide ,-tosylate ,-methanesulfonates or-triflate; Heteroaryl (C
1-C
4Alkyl)-halogenide ,-tosylate ,-methanesulfonates or-triflate; Or heterocyclic radical (C
1-C
4Alkyl)-halogenide ,-tosylate ,-methanesulfonates or-triflate.Acylating agent includes, but is not limited to C
1-C
10Alkane carboxylic acid halides or acid anhydrides, has the C of 1-10 halogen atom
1-C
10Halogenated alkane carboxylic acid halides or acid anhydrides, C
2-C
8Alkoxyl group alkane carboxylic acid halides or acid anhydrides, C
3-C
6Cycloalkyl alkane carboxylic acid halides or acid anhydrides, C
4-C
12Cycloalkyl alkane carboxylic acid halides or acid anhydrides, fragrant carboxylic acid halides or acid anhydrides, aryl (C
1-C
4) alkane carboxylic acid halides or acid anhydrides, assorted fragrant carboxylic acid halides or acid anhydrides, heteroaryl (C
1-C
4) alkane carboxylic acid halides or acid anhydrides, heterocycle carboxylic acid halides or acid anhydrides or heterocyclic radical (C
1-C
4) alkane carboxylic acid halides or acid anhydrides.Sulfonyl agent includes, but is not limited to C
1-C
10Heteroaryl-alkylsulfonyl halides or acid anhydrides, has the C of 1-10 halogen atom
1-C
10Haloalkyl sulfonic acid halide or acid anhydrides, C
2-C
8Alkoxyalkyl sulfonic acid halide or acid anhydrides, C
3-C
6Naphthene sulfamide halogen or acid anhydrides, C
4-C
12Cycloalkylalkyl sulfonic acid halide or acid anhydrides, aryl sulfonyl halide or acid anhydrides, aryl (C
1-C
4Alkyl)-, heteroaryl sulfonic acid halide or acid anhydrides, heteroaryl (C
1-C
4Alkyl) sulfonic acid halide or acid anhydrides, heterocyclic radical sulfonic acid halide or acid anhydrides or heterocyclic radical (C
1-C
4Alkyl) sulfonic acid halide or acid anhydrides.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred two-sec.-propyl ethamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is 0 ℃ to 100 ℃.
According to method shown in the flow process 14, can synthesis type (1) compound, wherein A is CR, R is identical with above-mentioned definition:
Flow process 14
Be in or be not in alkali and exist down, in inert solvent, in 0 ℃ to 250 ℃ temperature range, can use formula (20) compound (R wherein
1And R
3Identical with above-mentioned definition) processing formula (4) or formula (10) compound, obtain formula (1) compound (wherein A is CR, and R is identical with above-mentioned definition).Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred two-sec.-propyl ethamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is 0 ℃ to 100 ℃.Perhaps, can synthesis type (1) compound by intermediate (22) and (23), wherein A is CR, R is identical with above-mentioned definition.
Be in or be not in alkali and exist down, in inert solvent, in 0 ℃ to 250 ℃ temperature range, can use formula (21) compound (R wherein
1Identical with above-mentioned definition, R
eBe alkyl (1-6 carbon atom)) processing formula (4) or formula (10) compound, obtain formula (1) compound (wherein A is CR, and R is identical with above-mentioned definition).Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred two-sec.-propyl ethamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)) or aromatic hydrocarbon (preferred benzene or toluene).Preferable reaction temperature is 0 ℃ to 100 ℃.Being in or be not in alkali exists down; being in or be not in inert solvent exists down; in-80 ℃ to 250 ℃ temperature ranges; can handle formula (22) compound with halogenating agent or sulfonyl agent, obtain formula (23) product (wherein X is halogen atom, alkylsulfonyloxy, aryl-sulfonyl oxygen or haloalkyl sulfonyloxy).Halogenating agent includes, but is not limited to SOCl
2, POCl
3, PCl
3, PCl
5, POBr
3, PBr
3Or PBr
5Sulfonyl agent includes, but is not limited to heteroaryl-alkylsulfonyl halides or acid anhydrides (for example methylsulfonyl chloride or methylsulfonic acid acid anhydride), aryl sulfonyl halide or acid anhydrides (for example p-toluenesulfonyl chloride or acid anhydrides) or haloalkyl sulfonic acid halide or acid anhydrides (preferred trifluoromethanesulfanhydride anhydride).Alkali includes, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine or triethylamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, the haloalkane (preferred methylene dichloride) of N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Preferable reaction temperature is-20 ℃ to 100 ℃.
In the alkali existence or not,, between-80 ℃ to 250 ℃ temperature of reaction, can make formula (23) compound and formula R in the inert solvent existence or not
3H (R wherein
3Identical with above-mentioned definition, but R
3Be not SH, COR
7, CO
2R
7, aryl or heteroaryl) compound reacting generating (1) compound.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), alkaline carbonate, alkali metal hydrocarbonate, two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to alkyl alcohol (1-8 carbon atom, particular methanol or ethanol), low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), the haloalkane (preferred methylene dichloride) of aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Preferable reaction temperature is 0 ℃ to 140 ℃.
Use method shown in the flow process 15, also can prepare segment bounds (1) compound:
Flow process 15
(27)Y=O,S (1)Z=CR
2
Be in or be not in inert solvent and exist down, can make formula (24) compound (R wherein
cBe low alkyl group, Ar is identical with above-mentioned definition) and hydrazine reaction, formula (25) intermediate (wherein Ar is identical with above-mentioned definition) obtained.Conditional likelihood shown in employed reaction conditions and the flow process 4 by formula (3) compound formula (4) intermediate.Be in or be not in acid and exist down, in inert solvent, can make formula (25) compound (wherein A is N) and formula R
1C (=NH) OR
e(R wherein
1Identical with above-mentioned definition, R
eBe low alkyl group) reagent react, then be in or be not in alkali and exist down, in inert solvent, with formula YisC (R
d)
2(wherein Y is O or S, R
dBeing halogen atom (preferred chlorine), alkoxyl group (1-4 carbon atom) or alkylthio (1-4 carbon atom)) compound reacts and obtains formula (27) compound (wherein A is N, and Y is O, S).It is identical in the condition of these conversions and the flow process 4 formula (4) compound to be converted into the employed condition of formula (7) compound.
Perhaps, use to flow process 14 is employed formula (21) compound is converted into the similar condition of formula (22) compound, make formula (25) compound (wherein A is CR) and formula R
1(C=O) CHR (C=Y) OR
c(R wherein
1Identical with R with above-mentioned definition, R
cBe low alkyl group) the compound reaction, obtain formula (27) compound (wherein A is CR).Be in or be not in alkali and exist down, in inert solvent, can handle formula (27) intermediate (wherein Y is O), then be in or be not in alkali and exist down, in inert solvent, with R with halogenating agent or sulfonyl agent
3H or R
2The H reaction obtains formula (1) compound, and (wherein Z is CR
2).
Those skilled the in art will appreciate that in flow process 15 and can use various halogenating agents, sulfonyl agent, R with the different order of response procedures
3H or R
2The combination of H is to provide formula (I) compound.For example, in some cases, can need to make halogenating agent or the sulfonyl agent reaction and the R of compound and stoichiometric quantity
2H (or R
3H) react, and then react with halogenating agent or sulfonyl agent, and and R
3H (or R
2H) reaction obtains formula (1) compound.These transform, and the reaction conditions use and reagent and flow process 14 are employed to be converted into (23) with formula (22) midbody compound and to be converted into the employed conditional likelihood of (1) (wherein A is CR) again, perhaps with flow process 1 formula (7) midbody compound is converted into (8) and is converted into the employed conditional likelihood of (1) (wherein A is N) again.
Perhaps, can in flow process 15, formula (27) compound (wherein Y is S) be converted into formula (1) compound.In inert solvent, can use compound R
fX (R wherein
fBe low alkyl group, X is halogen atom, alkylsulfonyloxy or haloalkyl sulfonyloxy) make formula (27) midbody compound alkylation, (choose wantonly then and use the oxygenant oxidation in inert solvent) then is in or be not in alkali and exists down, in inert solvent with R
3The H reaction obtains formula (1) compound.In employed condition and reagent and the flow process 2 formula (7) midbody compound being converted into (12) (or being converted into 13), to be converted into formula (1) compound more employed similar.
With the other approach shown in the flow process 15, can be by formula (24) compound formula (1) compound.Exist down by being in or be not in acid, in inert solvent, make formula (24) compound warp and formula NH
2NH (C=NH) NH
2Compound reaction is then used in the flow process 10 formula (3) compound to be converted into (17) and to be converted into (7) employed condition again, with compound R
1C (OR
c)
3(R wherein
cBe low alkyl group, R
1Identical with above-mentioned definition) reaction, can be translated into formula (27) compound.
According to the method shown in the flow process 16, can prepare segment bounds (2) compound:
Flow process 16
(27b)Y=O,S (28)Y=O,S
Be in or be not in alkali and exist down, in inert solvent, can be with various alkylating agent R
14X (R wherein
14Identical with above-mentioned definition, X is halogen atom, alkylsulfonyloxy or haloalkyl sulfonyloxy) processing formula (27b) compound, obtain the structure of formula (28).Be in or be not in alkali then and exist down, in inert solvent,, can be translated into formula (2) compound, then be in or be not in alkali and exist down, in inert solvent, with R by handling formula (28) compound (wherein Y is O) with halogenating agent or sulfonyl agent
3The H reaction obtains formula (2) compound.These transform and in employed reaction conditions and the flow process 14 midbody compound (22) are converted into (23) and are converted into the employed conditional likelihood of (1) (wherein A is CR) again, perhaps with in the flow process 1 formula (7) midbody compound is converted into (8) is converted into the employed conditional likelihood of (1) (wherein A is N) again.Perhaps, in inert solvent, can use compound R
tX (R wherein
fBe low alkyl group, X is halogen atom, alkylsulfonyloxy or haloalkyl sulfonyloxy) make formula (28) (wherein Y is S) alkylation, (choose wantonly then and use the oxygenant oxidation in inert solvent) then is in or be not in alkali and exists down, in inert solvent with R
3The H reaction obtains formula (1) compound.In employed condition and reagent and the flow process 2 formula (7) midbody compound being converted into (12) (or being converted into 13), to be converted into formula (1) compound more employed similar.
With method shown in the flow process 16, formula (1) compound (wherein Z is COH) can be converted into formula (2) compound.Be in or be not in alkali and exist down, in inert solvent, with various alkylating agent R
14X (R wherein
14Identical with above-mentioned definition, X is halogen atom, alkylsulfonyloxy or haloalkyl sulfonyloxy) handle and to obtain structure (2).Those skilled in the art will recognize that (wherein Z is COR to method preparation formula (1) compound that also can use flow process 16
7).
In flow process 16, term " alkali " and " inert solvent " can have following meaning.Alkali can include, but is not limited to alkalimetal hydride (preferred sodium hydride), alkali metal alcoholate (1-6 carbon atom) (particular methanol sodium or sodium ethylate), alkaline earth metal hydride, basic metal dialkyl group ammonification thing (preferred di-isopropyl lithamide), two (trialkylsilanyl) amides of basic metal (preferred two (TMS) ammonification sodium), trialkylamine (preferred N, N-two-sec.-propyl-N-ethamine or triethylamine) or aromatic amine (preferred pyridine).Inert solvent includes, but is not limited to low alkyl group nitrile (1-6 carbon atom, preferred acetonitrile), dialkyl ether (preferred ether), cyclic ethers (preferred tetrahydrofuran (THF) or 1, the 4-dioxane), N, N-dialkylformamide (preferred dimethyl formamide), N, the haloalkane (preferred methylene dichloride) of N-dialkyl acetamides (preferred N,N-DIMETHYLACETAMIDE), cyclic amide (preferred N-methylpyrrolidin-2-ketone), dialkyl sulphoxide (preferred dimethyl sulfoxide (DMSO)), aromatic hydrocarbon (preferred benzene or toluene) or 1-10 carbon atom and 1-10 halogen atom.Preferable reaction temperature is-20 ℃ to 100 ℃.
Embodiment
Analytical data with following general method record following compounds.With IBM-Bruker FT-NMR (300MHz) record proton N MR spectrum; In tritiate chloroform or tritiate dimethyl sulfoxide (DMSO), the ppm (δ) that is offset with mark in tetramethylsilane writes down chemical shift according to following.(NH is used in chemistry-ionization (CI) with Finnegan MAT 8230 spectrographs
3Do carrier gas, or as following gas chromatography (GC)) or write down mass spectrum (MS) or high resolution mass spectrum (HRMS) with Hewlett Packard 5988A type spectrograph.Fusing point is record on Buchi Model 510 fusing point devices, and does not proofread and correct.Boiling point is not for proofreading and correct.All pH measure and all carry out with test paper in processing.
Reagent is buied by commerce, when needing before use, according to D.Perrin and W.L.F.Armarego at the general method purifying described in the Purification of Laboratory Chemicals (third edition, New York:Pergamon Press, 1988).Chromatography carries out on silica gel, uses the following solvents system.For mixed solvent system, provide the ratio of volume.Except that specializing, all umbers and per-cent are by weight.
Provide the following example to describe the present invention in more detail.These embodiment (having proposed to implement optimal mode of the present invention) are used to illustrate the present invention, and are not used in restriction the present invention.
Embodiment 1
2, the preparation of 7-dimethyl-8-(2, the 4-3,5-dimethylphenyl) [1,5-a]-pyrazolo-[1,3,5]-triazine-4 (3H)-ketone
(formula 7, wherein Y is O, R
1Be CH
3, Z is C-CH
3, Ar is 2, the 4-3,5-dimethylphenyl)
A.1-cyano group-1-(2, the 4-3,5-dimethylphenyl) third-2-ketone
Under room temperature, with the sodium particle (9.8g, 0.43mol) gradation adds to 2, (48g is in ethyl acetate 0.33mol) (150ml) solution for 4-3,5-dimethylphenyl acetonitrile.This reaction mixture is heated to reflux temperature, and stirred 16 hours.The suspension that produces is cooled to room temperature and filtration.With the precipitation of a large amount of ether washing collections, dry air then.Solid is soluble in water, add 1N HCl solution to pH=5-6.(3 * 200ml) extract this mixture, and the organic layer that merges through dried over mgso also filters with ethyl acetate.Vacuum is removed solvent and is obtained white solid (45.7g, 74% productive rate): NMR (CDCl
3, 300MHz); CI-MS:188 (M+H).
B.5-amino-4-(2, the 4-3,5-dimethylphenyl)-3-methylpyrazole
Under reflux temperature, with 1-cyano group-1-(2, the 4-3,5-dimethylphenyl) third-2-ketone (43.8g, 0.23mol), hydrazine-hydrate (22ml, 0.46mol), glacial acetic acid (45ml, 0.78mol) and the mixture of toluene (500ml) in being furnished with the dean stark trap device, stirred 18 hours.This reaction mixture is cooled to room temperature, and vacuum is removed solvent.Residue is dissolved among the 6N HCl, with ether with the solution extraction that produces three times.Add ammonium hydroxide solution,stronger to pH=11 to water layer.With ethyl acetate will produce not exclusively-solution extraction three times.Through the organic layer of dried over mgso merging, and filter.Vacuum is removed solvent and is obtained the sticking oily matter (34.6g, 75% productive rate) of light brown; NMR (CDCl
3, 300MHz); 7.10 (s, 1H), 7.05 (d, 2H, J=1), 2.37 (s, 3H), 2.10 (s, 3H); CI-MS:202 (M+H).
C.5-ethanamidine base-4-(2, the 4-3,5-dimethylphenyl)-3-methylpyrazole, acetate
With Ethyl acetamidate hydrochloride (60g, 0.48mol) add to fast salt of wormwood (69.5g, 0.50mol), methylene dichloride (120ml) and water (350ml) is rapidly in the stirred mixture.Separate each layer, with methylene dichloride (2 * 120ml) aqueous layer extracted.Organic layer through dried over mgso merges filters.Removing solvent through simple distillation, is the not purified use of clarifying weak yellow liquid (35.0g) with residue.
With glacial acetic acid (9.7ml, 0.17mol) add to stirring 5-amino-4-(2, the 4-3,5-dimethylphenyl)-3-methylpyrazole (34g, 0.17mol), (22g is 0.25mol) and in acetonitrile (500ml) mixture for ethyl acetamidate.Under room temperature, the reaction mixture that produces was stirred 3 days, then with its vacuum concentration to 1/3rd of about original volume.Filter the suspension that produces, with the solid of a large amount of ether washing collections.Vacuum-drying white solid (31.4g, 61% productive rate); NMR (DMSO-d
6, 300MHz); 7.00 (s, 1H), 6.90 (dd, 2H, J=7,1), 2.28 (s, 3H), 2.08 (s, 3H), 2.00 (s, 3H), 1.90 (s, 3H), 1.81 (s, 3H); CI-MS:243 (M+H).
D.2,7-dimethyl-8-(2, the 4-3,5-dimethylphenyl) [1,5-a]-pyrazolo-[1,3,5]-triazine-4 (3H)-ketone
Under vigorous stirring, (23g, 1mol) gradation adds in the ethanol (500ml) with the sodium particle.After the reaction of all sodium, add 5-ethanamidine base-4-(2, the 4-3,5-dimethylphenyl)-3-methylpyrazole acetate (31.2g, 0.1mol) and diethyl carbonate (97ml, 0.8mol).The reaction mixture that produces is heated to reflux temperature, stirred 18 hours.With this mixture cool to room temperature, vacuum is removed solvent.Residue is soluble in water, slowly add 1N HCl solution to pH=5-6.With water layer extraction three times, the organic layer that merges through dried over mgso also filters with ethyl acetate.Vacuum is removed solvent and is obtained filbert solid (26g, 98% productive rate); NMR (CDCl
3, 300MHz); 7.15 (s, 1H), 7.09 (s, 2H), 2.45 (s, 3H), 2.39 (s, 3H), 2.30 (s, 3H); CI-MS:269 (M+H).
Embodiment 2
The preparation of 5-methyl-3-(2,4, the 6-trimethylphenyl) [1,5-a]-[1,2,3]-triazolo-[1,3,5]-triazine-7 (6H)-ketone
(formula 7, wherein Y is O, R
1Be CH
3, Z is N, Ar is 2,4, the 6-trimethylphenyl)
A.1-phenyl methyl-4-(2,4, the 6-trimethylphenyl)-5-aminotriazole
Under room temperature, with 2,4,6-trimethyl benzyl cyanogen (1.0g, 6.3mmol), benzyl azide (0.92g, 6.9mmol) and potassium tert.-butoxide (0.78g, tetrahydrofuran (THF) 6.9mmol) (10ml) mixture stirred 2.5 days.The suspension that dilute with water produces is used ethyl acetate extraction three times.Through the organic layer of dried over mgso merging, and filter.Vacuum is removed solvent, obtains brown oil.Grind and filter with ether, obtain yellow solid (1.12g, 61% productive rate); NMR (CDCl
3, 300MHz); 7.60-7.30 (m, 5H), 7.30-7.20 (m, 2H), 5.50 (s, 2H), 3.18 (br, s, 2H), 2.30 (s, 3H), 2.10 (s, 6H); CI-MS:293 (M+H).
B.4-(2,4, the 6-trimethylphenyl)-5-aminotriazole
Under agitation, (500mg 22mmol) adds to that liquefied ammonia (30ml) and 1-phenyl methyl-4-(2,4, the 6-trimethylphenyl)-(1.1g is in mixture 3.8mmol) for the 5-aminotriazole with sodium.Stirring this reaction mixture to deep green does not take off.Add ammonium chloride solution (ml), stir this mixture simultaneously with being heated to room temperature in 16 hours.With 1M HCl solution-treated residue and filtration.With the ammonium hydroxide solution,stronger water layer (pH=9) that alkalizes, use ethyl acetate extraction then three times.Organic layer through dried over mgso merges filters.Vacuum removes solvent and obtains yellow solid (520mg), proves homogeneous through thin-layer chromatography (ethyl acetate):
NMR(CDCl
3,300MHz);6.97(s,2H),3.68-3.50(br,s,2H),2.32(s,3H),2.10(s,6H);CI-MS:203(M+H)。
C.4-(2,4, the 6-trimethylphenyl)-5-ethanamidine base triazole acetate
Under room temperature, with 4-(2,4, the 6-trimethylphenyl)-5-aminotriazole (400mg, 1.98mmol), ethyl acetamidate (261mg, 3mmol) and glacial acetic acid (0.1ml, mixture in acetonitrile 1.98mmol) (6ml) stirred 4 hours.Filter the suspension that produces, with the solid of a large amount of ether washing collections.Vacuum-drying obtains white solid (490mg, 82% productive rate): NMR (DMSO-d
6, 300MHz); 7.90-7.70 (br s, 0.5H), 7.50-7.20 (br s, 0.5H), 6.90 (s, 2H), 6.90 (s, 2H), 3.50-3.10 (br, s, 3H), 2.30-2.20 (br s, 3H), 2.05 (d, 1H, J=7), 1.96 (s, 6H), 1.87 (s, 6H); CI-MS:244 (M+H).
D.5-methyl-3-(2,4, the 6-trimethylphenyl) [1,5-a]-[1,2,3]-triazolo-[1,3,5]-triazine-7 (4H)-ketone
In room temperature, stirring down, (368mg 16.2mmol) adds in the ethanol (10ml) with sodium.After the reaction of described sodium, add 4-(2,4, the 6-trimethylphenyl)-5-ethanamidine base triazole acetate (490mg, 1.6mmol) and diethyl carbonate (1.6ml, 13mmol).This reaction mixture was stirred 5 hours down in reflux temperature, be cooled to room temperature then.This reaction mixture of dilute with water adds 1N HCl solution to pH=5-6.With water layer extraction three times, the organic layer through dried over mgso merges filters with ethyl acetate.Vacuum is removed solvent and is obtained yellow residue.Obtain yellow solid (300mg, 69% productive rate) with ether grinding and filtration; NMR (CDCl
3, 300MHz); 6.98 (s, 2H), 2.55 (s, 3H), 2.35 (s, 3H), 2.10 (s, 6H); CI-MS:270 (M+H).
Embodiment 3
4-(two (carbonyl methoxyl group) methyl)-2, the preparation of 7-dimethyl-8-(2, the 4-3,5-dimethylphenyl) [1,5-a]-pyrazolo-1,3,5-triazines
(formula 1, wherein R
3Be CH (CHCO
2H
3)
2, R
1Be CH
3, Z is C-CH
3, Ar is 2, the 4-3,5-dimethylphenyl)
A.4-chloro-2,7-dimethyl-8-(2,4 dichloro benzene base) [1,5-a]-method for preparation of pyrazolotriazine
Under reflux temperature, with 2,7-dimethyl-8-(2, the 4-3,5-dimethylphenyl) [1,5-a]-(embodiment 1,1.38g for pyrazolo-1,3,5-triazines-4-ketone, 4.5mmol), N, accelerine (1ml, 8mmol) and the mixture of phosphoryl chloride (10ml) stirred 48 hours.Vacuum is removed excessive phosphoryl chloride.Residue is inclined to frozen water, and brief the stirring extracts three times fast with ethyl acetate.Organic layer with the frozen water washing merges also filters with dried over mgso then.Vacuum is removed solvent and is obtained brown oil.Rapid column chromatography (ethyl acetate: hexane=1: 4) obtain a component (R
f=0.5).Vacuum is removed solvent and is obtained yellow oil (1.0g, 68% productive rate); NMR (CDCl
3, 300MHz); 7.55 (d, 1H, J=1), 7.38 (dd, 1H, J=7,1), 7.30 (d, 1H, J=7), 2.68 (s, 3H), 2.45 (s, 3H); CI-MS:327 (M+H).
B.4-(two (carbonyl methoxyl group) methyl)-2,7-dimethyl-8-(2, the 4-3,5-dimethylphenyl) [1,5-a]-pyrazolo-1,3,5-triazines
With hexane with sodium hydride (2mmol) washed twice is washed hypsokinesis at every turn and is gone out hexane for 60% fluid, 80mg, be dissolved in anhydrous tetrahydro furan (THF, 1ml) in.(0.32g, THF 2mmol) (2ml) solution begin acutely to produce gas this moment to drip diethyl malonate with 5 minutes.Add 4-chloro-2, (0.5g, THF 1.75mmol) (2ml) solution stir this reaction mixture 48 hours down in nitrogen environment 7-dimethyl-8-(2,4 dichloro benzene base) [1,5-a]-method for preparation of pyrazolotriazine then.The suspension that produces is inclined to water, use ethyl acetate extraction three times.With salt solution the organic layer that merges is washed once, through dried over mgso and filtration.Vacuum is removed solvent, obtains brown oil.(ethyl acetate: hexane=1: 9), vacuum obtains faint yellow solid (R after removing solvent through column chromatography
f=0.2,250mg, 35% productive rate); Mp 50-52 ℃; NMR (CDCl
3, 300MHz): 12.35 (br.s, 1H), 7.15-7.00 (m, 3H), 4.40 (q, 2H, J=7), 4.30 (q, 2H, J=7), 2.4,2.35,2.3,2.2,2.1 (5s, 12H), 1.4 (t, 3H, J=7), 1.35-1.25 (m, 3H); CI-HRMS: calculated value: 411.2032, measured value: 411.2023.
Embodiment 6
4-(1,3-dimethoxy-2-third amino)-2, the preparation of 7-dimethyl-8-(2,4 dichloro benzene base) [1,5-a]-pyrazolo-1,3,5-triazines
(formula 1, wherein R
3Be NHCH (CH
2OCH
3)
2, R
1Be CH
3, Z is C-CH
3, Ar is the 2,4 dichloro benzene base)
A.4-chloro-2,7-dimethyl-8-(2,4 dichloro benzene base) [1,5-a]-method for preparation of pyrazolotriazine
Under reflux temperature, with 2,7-dimethyl-8-(2, the 4-3,5-dimethylphenyl) [1,5-a]-(embodiment 1,1.38g for pyrazolo-1,3,5-triazines-4-ketone, 4.5mmol), N, accelerine (1ml, 8mmol) and phosphoryl chloride (10ml) mixture stirred 48 hours.Vacuum is removed excessive phosphoryl chloride.Residue is inclined to frozen water, and brief the stirring extracts three times fast with ethyl acetate.Organic layer with the frozen water washing merges also filters with dried over mgso then.Vacuum is removed solvent and is obtained brown oil.Rapid column chromatography (ethyl acetate: hexane=1: 4) obtain a component (R
f=0.5).Vacuum is removed solvent and is obtained yellow oil (1.0g, 68% productive rate); NMR (CDCl
3, 300MHz); 7.55 (d, 1H, J=1), 7.38 (dd, 1H, J=7,1), 7.30 (d, 1H, J=7), 2.68 (s, 3H), 2.45 (s, 3H); CI-MS:327 (M+H).
B.4-(1,3-dimethoxy-2-third amino)-2,7-dimethyl-8-(2,4 dichloro benzene base) [1,5-a]-pyrazolo-1,3,5-triazines
Under room temperature, with 4-chloro-2,7-dimethyl-8-(2,4 dichloro benzene base) [1,5-a]-pyrazolo-1,3,5-triazines (part A, 570mg, 1.74mmol), 1,3-dimethoxy propyl group-2-aminopropane (25mg, 2.08mmol) and the mixture of ethanol (10ml) stirred 18 hours.This reaction mixture is inclined to water (25ml), use ethyl acetate extraction three times.The organic layer that merges through dried over mgso also filters.Vacuum is removed solvent.Through column chromatography (methylene dichloride: methyl alcohol=50: 1) obtain a component.Vacuum obtains solid (250mg, 35% productive rate) after removing solvent; Mp 118-120 ℃; NMR (CDCl
3, 300MHz); 7.50 (s, 1H), 7.28 (dd, 2H, J=8,1), 6.75 (d, 1H, J=8), 4.70-4.58 (m, 1H), 3.70-3.55 (m, 4H), 3.43 (s, 6H), 2.50 (s, 3H), 2.35 (s, 3H); CI-HRMS: calculated value: 409.1072, measured value 409.1085.C
18H
21Cl
2N
5O
2Analytical calculation value: C, 52.69; H, 5.17; N, 17.07, Cl, 17.28; Measured value: C, 52.82; H, 5.06; N, 16.77, Cl, 17.50.
With aforesaid method and the known modification of organic synthesis those skilled in the art, can prepare additional embodiments compound among the 1-4 that tabulates down.
According to embodiment 1,2,3 or 6 described methods, can prepare the described embodiment compound of table 1.Use following abbreviation: Ph to be phenyl, Pr is a propyl group, and Me is a methyl, and Et is an ethyl, and Bu is a butyl, and Ex is embodiment.
Table 1
Ex.
Z
R3
Ar
mp (℃)
6
a C-Me NHCH(CH
2OMe)
2 2,4-Cl
2-Ph 118-120
7
b C-Me NHCHPr
2 2,4-Cl
2-Ph 114-116
8
c C-Me NEtBu 2,4-Cl
2-Ph grease 9d C-Me NPr(CH
2-c-C
3H
5) 2,4-Cl
2-Ph grease 10e C-Me N(CH
2CH
2OMe)
2 2,4-Cl
2-Ph grease 11fC-Me NH-3-heptyl 2,4-Cl2-Ph 90-92
12
g C-Me NHCH(E)CH
2OMe 2,4-Cl
2-Ph 179-181
13
h C-Me NEt
2 2,4-Cl
2-Ph 133-134
14
i C-Me NHCH(CH
2OEt)
2 2,4-Cl
2-Ph grease 15jC-Me NH-3-amyl group 2,4-Cl2-Ph 139-140
16
k C-Me NMePh 2,4-Cl
2-Ph 60-62
17
l C-Me NPr
2 2,4-Cl
2-Ph grease 18mC-Me NH-3-hexyl 2,4-Cl2-Ph 130-132 19 C-Me morpholinoes 2,4-Cl2-Ph
20 C-Me N(CH
2Ph)CH
2CH
2CMe 2,4-Cl
2-Ph
21 C-Me NHCH(CH
2Ph)CH
2OMe 2,4-Cl
2-Ph 22 C-Me NH-4-THP trtrahydropyranyls 2,4-Cl2-Ph 23 C-Me NH-cyclopenta 2,4-Cl2-Ph 24 C-Me 1,2,3,4-tetrahydro isoquinolyl 2,4-Cl2-Ph
25 C-Me CH
2-(1,2,3,4-tetrahydro isoquinolyl) 2,4-Cl2-Ph
26
n C-Me OEt 2,4-Cl
2-Ph 141-143
27 C-Me OCH(Et)CH
2OMe 2,4-Cl
2-Ph
28 C-Me OCH
2Ph 2,4-Cl
2-Ph 29 C-Me O-3-amyl groups 2,4-Cl2-Ph
30 C-Me SEt 2,4-Cl
2-Ph
31 C-Me S(O)Et 2,4-Cl
2-Ph
32 C-Me SO
2Et 2,4-Cl
2-Ph
33 C-Me CH(CO
2Et)
2 2,4-Cl
2-Ph
34 C-Me C(Et)(CO
2Et)
2 2,4-Cl
2-Ph
35 C-Me CH(Et)CH
2OH 2,4-Cl
2-Ph
36 C-Me CH(Et)CH
2OMe 2,4-Cl
2-Ph
37 C-Me CONMe
2 2,4-Cl
2-Ph
38 C-Me COCH
3 2,4-Cl
2-Ph
39 C-Me CH(OH)CH
3 2,4-Cl
2-Ph 40 C-Me C (OH) Ph-3-pyridine radicals 2,4-Cl2-Ph
41 C-Me Ph 2,4-Cl
2-Ph
42 C-Me 2-CF
3-Ph 2,4-Cl
2-Ph
43 C-Me 2-Ph-Ph 2,4-Cl
2-Ph 44 C-Me 3-amyl groups 2,4-Cl2-Ph 45 C-Me cyclobutyl 2,4-Cl2-Ph 46 C-Me 3-pyridine radicals 2,4-Cl2-Ph
47 C-Me CH(Et)CH
2CONMe
2 2,4-Cl
2-Ph
48 C-Me CH(Et)CH
2CH
2NMe
2 2,4-Cl
2-Ph
49
o C-Me NHCH(CH
2OMe)
2 2,4,6-Me
3-Ph 125-127
50 C-Me NHCHPr
2 2,4,6-Me
3-Ph
51 C-Me NEtBu 2,4,6-Me
3-Ph
52 C-Me NPr(CH
2-c-C
3H
5) 2,4,6-Me
3-Ph
53
ae C-Me N(CH
2CH
2OMe)
2 2,4,6-Me
3-Ph 123-124 54 C-Me NH-3-heptyl 2,4,6-Me3-Ph
55
ac C-Me NHCH(Et)CH
2OMe 2,4,6-Me
3-Ph 145-146
56
ah C-Me NEt
2 2,4,6-Me
3-Ph 88-90
57
ai C-Me NHCH(CH
2OEt)
2 2,4,6-Me
3-Ph 132-134
58
adC-Me NH-3-amyl group 2,4,6-Me3-Ph 134-135
59 C-Me NMePh 2,4,6-Me
3-Ph
60 C-Me NPr
2 2,4,6-Me
3-Ph 61 C-Me NH-3-hexyls 2,4,6-Me3-Ph 62 C-Me morpholinoes 2,4,6-Me3-Ph
63 C-Me N(CH
2Ph)CH
2CH
2OMe 2,4,6-Me
3-Ph
64 C-Me NHCH(CH
2Ph)CH
2OMe 2,4,6-Me
3-Ph 65 C-Me NH-4-THP trtrahydropyranyls 2,4,6-Me3-Ph 66 C-Me NH-cyclopenta 2,4,6-Me3-Ph 67 C-Me 1,2,3,4-tetrahydro isoquinolyl 2,4,6-Me3-Ph
68 C-Me CH
2-(1,2,3,4-tetrahydro isoquinolyl) 2,4,6-Me3-Ph
69 C-Me OEt 2,4,6-Me
3-Ph
70 C-Me OCH(Et)CH
2OMe 2,4,6-Me
3-Ph
71 C-Me OCH
2Ph 2,4,6-Me
3-Ph 72 C-Me O-3-amyl groups 2,4,6-Me3-Ph
73 C-Me SEt 2,4,6-Me
3-Ph
74 C-Me S(O)Et 2,4,6-Me
3-Ph
75 C-Me SO
2E 2,4,6-Me
3-Ph
76 C-Me CH(CO
2Et)
2 2,4,6-Me
3-Ph
77 C-Me C(Et)(CO
2Et)
2 2,4,6-Me
3-Ph
78 C-Me CH(Et)CH
2OH 2,4,6-Me
3-Ph
79 C-Me CH(Et)OH
2OMe 2,4,6-Me
3-Ph
80 C-Me CONMe
2 2,4,6-Me
3-Ph
81 C-Me COCH
3 2,4,6-Me
3-Ph
82 C-Me CH(OH)CH
3 2,4,6-Me
3-Ph 83 C-Me C (OH) Ph-3-pyridine radicals 2,4,6-Me3-Ph
84 C-Me Ph 2,4,6-Me
3-Ph
85 C-Me 2-CF
3-Ph 2,4,6-Me
3-Ph
86 C-Me 2-Ph-Ph 2,4,6-Me
3-Ph 87 C-Me 3-amyl groups 2,4,6-Me3-Ph 88 C-Me cyclobutyl 2,4,6-Me3-Ph 89 C-Me 3-pyridine radicals 2,4,6-Me3-Ph
90 C-Me CH(Et)CH
2CONMe
2 2,4,6-Me
3-Ph
91 C-Me CH(Et)CH
2CH
2NMe
2 2,4,6-Me
3-Ph
92
p C-Me NHCH(CH
2OMe)
2 2,4-Me
2-Ph 44-45
93
q C-Me N(CH
2CH
2OMe)
2 2,4-Me
2-Ph grease 94r C-Me NHCH(Et)CH
2OMe 2,4-Me
2-Ph 102-104
95
sC-Me NH-3-amyl group 2,4-Me2-Ph 102-104
96
t C-Me NEt
2 2,4-Me
2-Ph grease 97u C-Me N(CH
2CN)
2 2,4-Me
2-Ph 148-150
98
v C-Me NHCH(Me)CH
2OMe 2,4-Me
2-Ph 102-104
99
w C-Me OCH(Et)CH
2OMe 2,4-Me
2-Ph grease 100x C-Me NPr-c-C
3H
5 2,4-Me
2-Ph grease 101y C-Me NHCH(Me)CH
2NMe
2 2,4-Me
2-Ph 47-48
102
z C-Me N(c-C
3H
5)CH
2CH
2CN 2,4-Me
2-Ph 117-118
103
aa C-Me N(Pr)CH
2CH
2CN 2,4-Me
2-Ph grease 104ab C-Me N(Bu)CH
2CH
2CN 2,4-Me
2-Ph grease 105 C-Me NHCHPr2 2,4-Me
2-Ph
106 C-Me NEtBu 2,4-Me
2-Ph
107 C-Me NPr(CH
2-c-C
3H
5) 2,4-Me
2-Ph 108 C-Me NH-3-heptyl 2,4-Me2-Ph
109 C-Me NEt
2 2,4-Me
2-Ph
110 C-Me NHCH(CH
2OEt)
2 2,4-Me
2-Ph 111 C-Me NH-3-amyl groups 2,4-Me2-Ph
112 C-Me NMePh 2,4-Me
2-Ph
113 C-Me NPr
2 2,4-Me
2-Ph 114 C-Me NH-3-hexyls 2,4-Me2-Ph 115 C-Me morpholinoes 2,4-Me2-Ph
116 C-Me N(CH
2Ph)CH
2CH
2OMe 2,4-Me
2-Ph
117 C-Me NHCH(CH
2Ph)CH
2OMe 2,4-Me
2-Ph 118 C-Me NH-4-THP trtrahydropyranyls 2,4-Me2-Ph 119 C-Me NH-cyclopenta 2,4-Me2-Ph 120 C-Me 1,2,3,4-tetrahydro isoquinolyl 2,4-Me2-Ph
121 C-Me CH
2-(1,2,3,4-tetrahydro isoquinolyl) 2,4-Me2-Ph
122 C-Me OEt 2,4-Me
2-Ph
123 C-Me OCH(Et)CH
2OMe 2,4-Me
2-Ph
124 C-Me OCH
2Ph 2,4-Me
2-Ph 125 C-Me O-3-amyl groups 2,4-Me2-Ph 126 C-Me SEt 2,4-Me2-Ph
127 C-Me S(O)Et 2,4-Me
2-Ph
128 C-Me SO
2Et 2,4-Me
2-Ph
3 C-Me CH(CO
2Et)
2 2,4-Me
2-Ph 50-52
129 C-Me C(Et)(CO
2Et)
2 2,4-Me
2-Ph
130 C-Me CH(Et)CH
2OH 2,4-Me
2-Ph
131 C-Me CH(Et)CH
2OMe 2,4-Me
2-Ph
132 C-Me CH(Et)CH
2OEt 2,4-Me
2-Ph
133 C-Me CONMe
2 2,4-Me
2-Ph
134 C-Me COCH
3 2,4-Me
2-Ph
135 C-Me CH(OH)CH
3 2,4-Me
2-Ph 136 C-Me C (OH) Ph-3-pyridine radicals 2,4-Me2-Ph
137 C-Me Ph 2,4-Me
2-Ph
138 C-Me 2-CF
3-Ph 2,4-Me
2-Ph
139 C-Me 2-Ph-Ph 2,4-Me
2-Ph 140 C-Me 3-amyl groups 2,4-Me2-Ph 141 C-Me cyclobutyl 2,4-Me2-Ph 142 C-Me 3-pyridine radicals 2,4-Me2-Ph
143 C-Me CH(Et)CH
2CONMe
2 2,4-Me
2-Ph
144 C-Me CH(Et)CH
2CH
2NMe
2 2,4-Me
2-Ph
145
bc C-Me NHCH(CH
2OMe)
2 2-Me-4-MeO-Ph 45-46
146
bd C-Me N(CH
2CH
2OMe)
22-Me-4-MeO-Ph grease 147be C-Me NHCH(Et)CH
2OMe 2-Me-4-MeO-Ph 86-88
148
bf C-Me N(Pr)CH
2CH
2CN 2-Me-4-MeO-Ph grease 149 C-Me OCH (Et) CH2OMe 2-Me-4-MeO-Ph
150
af C-Me NHCH(CH
2OMe)
2 2-Br-4-MeO-Ph 88-90
151
al C-Me N(CH
2CH
2OMe)
22-Br-4-MeO-Ph grease 152ag C-Me NHCH(Et)CH
2OMe 2-Br-4-MeO-Ph 95-97
153 C-Me N(Pr)CH
2CH
2CN 2-Br-4-MeO-Ph
154 C-Me OCH(Et)CH
2OMe 2-Br-4-MeO-Ph
155 C-Me NHCH(CH
2OMe)
2 2-Me-4-NMe
2-Ph
156 C-Me N(CH
2CH
2OMe)
2 2-Me-4-NMe
2-Ph grease 157 C-Me NHCH (Et) CH2OMe 2-Me-4-NMe
2-Ph
158 C-Me N(Pr)CH
2CH
2CN 2-Me-4-NMe
2-Ph
159 C-Me OCH(Et)CH
2OMe 2-Me-4-NMe
2-Ph
160 C-Me NHCH(CH
2OMe)
2 2-Br-4-NMe
2-Ph
161 C-Me N(CH
2CH
2OMe)
2 2-Br-4-NMe
2-Ph
162 C-Me NHCH(Et)CH
2OMe 2-Br-4-NMe
2-Ph
163 C-Me N(Pr)CH
2CH
2CN 2-Br-4-NMe
2-Ph
164 C-Me OCH(Et)CH
2OMe 2-Br-4-NMe
2-Ph
165 C-Me NHCH(CH
2OMe)
2 2-Br-4-i-Pr-Ph
166 C-Me N(CH
2CH
2OMe)
2 2-Br-4-i-Pr-Ph
167 C-Me NHCH(Et)CH
2OMe 2-Br-4-i-Pr-Ph
168 C-Me N(Pr)CH
2CH
2CN 2-Br-4-i-Pr-Ph
169 C-Me OCH(Et)CH
2OMe 2-Br-4-i-Pr-Ph
170 C-Me NHCH(CH
2OMe)
2 2-Br-4-Me-Ph
171 C-Me N(CH
2CH
2OMe)
2 2-Br-4-Me-Ph
172 C-Me NHCH(Et)CH
2OMe 2-Br-4-Me-Ph
173 C-Me N(Pr)CH
2CH
2CN 2-Br-4-Me-Ph
174 C-Me OCH(Et)CH
2OMe 2-Br-4-Me-Ph
175
ar C-Me NHCH(CH
2OMe)
2 2-Me-4-Br-Ph 108-109
176 C-Me N(CH
2CH
2OMe)
2 2-Me-4-Br-Ph
177 C-Me NHCH(Et)CH
2OMe 2-Me-4-Br-Ph
178 C-Me N(Pr)CH
2CH
2CN 2-Me-4-Br-Ph
179 C-Me OCH(Et)CH
2OMe 2-Me-4-Br-Ph
180 C-Me NHCH(CH
2OMe)
2 2-Cl-4,6-Me
2-Ph
181 C-Me N(CH
2CH
2OMe)
2 2-Cl-4,6-Me
2-Ph
182 C-Me NHCH(CH
2OMe)
2 4-Br-2,6-(Me)
2-Ph
183 C-Me N(CH
2CH
2OMe)
2 4-Br-2,6-(Me)
2-Ph
184 C-Me NHCH(CM
2OMe)
2 4-i-Pr-2-SMe-Ph
185 C-Me N(CH
2CH
2OMe)
2 4-i-Ph-2-SMe-Ph
186 C-Me NHCH(CH
2OMe)
2 2-Br-4-CF
3-Ph
187 C-Me N(CH
2CH
2OMe)
2 2-Br-4-CF
3-Ph
188 C-Me NHCH(CH
2OMe)
2 2-Br-4,6-(MeO)
2-Ph
189 C-Me N(CH
2CH
2OMe)
2 2-Br-4,6-(MeO)
2-Ph
190 C-Me NHCH(CH
2OMe)
2 2-Cl-4,6-(MeO)
2-Ph
191 C-Me N(CH
2CH
2OMe)
2 2-Cl-4,6-(MeO)
2-Ph
192 C-Me NHCH(CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
193 C-Me N(CH
2CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
194 C-Me NHCH(CH
2OMe)
2 4-(COMe)-2-Br-Ph
195 C-Me N(CH
2CH
2OMe)
2 4-(COMe)-2-Br-Ph
196 C-Me NHCH(CH
2OMe)
2 2,4,6-Me
3-pyridin-3-yl 197 C-Me N (CH2CH
2OMe)
2 2,4,6-Me
3-pyridin-3-yl 198 C-Me NHCH (CH2OMe)
2 2,4-(Br)
2-Ph
199 C-Me N(CH
2CH
2OMe)
2 2,4-(Br)
2-Ph
200 C-Me NHCH(CH
2OMe)
2 4-i-Pr-2-SMe-Ph
201 C-Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SMe-Ph
202 C-Me NHCH(CH
2OMe)
2 4-i-Pr-2-SO
2Me-Ph
203 C-Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SO
2Me-Ph
204 C-Me NHCH(CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
205 C-Me N(CH
2CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
206 C-Me NHCH(CH
2OMe)
2 2,6-(Me)
2-4-SO
2Me-Ph
207 C-Me N(CH
2CH
2OMe)
2 2,6-(Me)
2-4-SO
2Me-Ph
208 C-Me NHCH(CH
2OMe)
2 2-I-4-i-Pr-Ph
209 C-Me N(CH
2CH
2OMe)
2 2-I-4-i-Pr-Ph
210 C-Me NHCH(CH
2OMe)
2 2-Br-4-N(Me)
2-6-MeO-Ph
211 C-Me N(CH
2CH
2OMe)
2 2-Br-4-N(Me)
2-6-MeO-Ph
212 C-Me NHCH(CH
2OMe)
2 2,4-[SMe]2-Ph
213 C-Me N(CH
2CH
2OMe)
2 2,4-[SMe]2-Ph
214 C-Me NHCH(CH
2OMe)
2 2,4-[SO
2Me]2-Ph
215 C-Me N(CH
2CH
2OMe)
2 2,4-[SO
2Me]2-Ph
216 C-Me NHCH(CH
2OMe)
2 4-i-Pr-2-SMe-Ph
217 C-Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SMe-Ph
218 C-Me NHCH(CH
2OMe)
2 4-i-Pr-2-SO
2Me-Ph
219 C-Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SO
2Me-Ph
220 C-Me NHCH(CH
2OMe)
2 2-N(Me)
2-4-Me-Ph
221 C-Me N(CH
2CH
2OMe)
2 2-N(Me)
2-4-Me-Ph
222 C-Me NHCH(CH
2OMe)
2 2-MeS-4,6-(Me)
2-Ph
223 C-Me N(CH
2CH
2OMe)
2 2-MeS-4,6-(Me)
2-Ph
224 C-Me NHCH(CH
2OMe)
2 2-(CH
3CO)-4,6-(Me)
2-Ph
225 C-Me N(CH
2CH
2OMe)
2 2-(CH
3CO)-4,6-(Me)
2-Ph
226 H NHCH(CH
2OMe)
1 2,4-Me
2-Ph
227 H NHCH(CH
2OMe)
2 2,4-Me
2-Ph
228 CF3 N(CH
2CH
2OMe)
2 2,4-Me
2-Ph
229 CF3 N(CH
2CH
2OMe)
2 2,4-Me
2-Ph
230 N NHCH(CH
2OMe)
2 2,4,6-Me
3-Ph
231 N NHCHPr
2 2,4,6-Me
3-Ph
232 N NEtBu 2,4,6-Me
3-Ph
233 N NPr(CH
2-c-C
3H
5)2,4,6-Me
3-Ph
234 N N(CH
2CH
2OMe)
2 2,4,6-Me
3-Ph 235 N NH-3-heptyl 2,4,6-Me3-Ph
236 N NHCH(Et)CH
2OMe 2,4,6-Me
3-Ph
237 N NEt
2 2,4,6-Me
3-Ph
238 N NHCH(CH
2OEt)
2 2,4,6-Me
3-Ph 239 N NH-3-amyl groups 2,4,6-Me3-Ph
240 N NMePh 2,4,6-Me
3-Ph
241 N NPr
2 2,4,6-Me
3-Ph 242 N NH-3-hexyls 2,4,6-Me3-Ph 243 N morpholinoes 2,4,6-Me3-Ph
244 N N(CH
2Ph)CH
2CH
2OMe 2,4,6-Me
3-Ph
245 N NHCH(CH
2Ph)CH
2OMe 2,4,6-Me
3-Ph 246 N NH-4-THP trtrahydropyranyls 2,4,6-Me3-Ph 247 N NH-cyclopenta 2,4,6-Me3-Ph 248 N 1,2,3,4-tetrahydro isoquinolyl 2,4,6-Me3-Ph
249 N CH
2-(1,2,3,4-tetrahydro isoquinolyl) 2,4,6-Me3-Ph
250 N OEt 2,4,6-Me
3-Ph
251 N OCH(Et)CH
2OMe 2,4,6-Me
3-Ph
252 N OCH
2Ph 2,4,6-Me
3-Ph 253 N O-3-amyl groups 2,4,6-Me3-Ph
254 N SEt 2,4,6-Me
3-Ph
255 N S(O)Et 2,4,6-Me
3-Ph
256 N SO
2Et 2,4,6-Me
3-Ph
257 N CH(CO
2Et)
2 2,4,6-Me
3-Ph
258 N C(Et)(CO
2Et)
2 2,4,6-Me
3-Ph
259 N CH(Et)CH
2OH 2,4,6-Me
3-Ph
260 N CH(E-)CH
2OMe 2,4,6-Me
3-Ph
261 N CONMe
2 2,4,6-Me
3-Ph
262 N COCH
3 2,4,6-Me
3-Ph
263 N CH(OH)CH
3 2,4,6-Me
3-Ph 264 N C (OH) Ph-3-pyridine radicals 2,4,6-Me3-Ph
265 N Ph 2,4,6-Me
3-Ph
266 N 2-CF
3-Ph 2,4,6-Me
3-Ph
267 N 2-Ph-Ph 2,4,6-Me
3-Ph 268 N 3-amyl groups 2,4,6-Me3-Ph 269 N cyclobutyl 2,4,6-Me3-Ph 270 N 3-pyridine radicals 2,4,6-Me3-Ph
271 N CH(Et)CH
2CONMe
2 2,4,6-Me
3-Ph
272 N CH(Et)CH
2CH
2NMe
2 2,4,6-Me
3-Ph
273 N NHCH(CH
2OMe)
2 2,4-Me
2-Ph
274 N NHCHPr
2 2,4-Me
2-Ph
275 N NEtBu 2,4-Me
2-Ph
276 N NPr(CH
2-c-C
3H
5) 2,4-Me
2-Ph
277 N N(CH
2CH
2OMe)
2 2,4-Me
2-Ph 278 N NH-3-heptyl 2,4-Me2-Ph
279 N NHCH(Et)CH
2OMe 2,4-Me
2-Ph
280 N NEt
2 2,4-Me
2-Ph
281 N NHCH(CH
2OEt)
2 2,4-Me
2-Ph 282 N NH-3-amyl groups 2,4-Me2-Ph
283 N NMePh 2,4-Me
2-Ph
284 N NPr
2 2,4-Me
2-Ph 285 N NH-3-hexyls 2,4-Me2-Ph 286 N morpholinoes 2,4-Me2-Ph
287 N N(CH
2Ph)CH
2CH
2OMe 2,4-Me
2-Ph
288 N NHCH(CH
2Ph)CH
2OMe 2,4-Me
2-Ph 289 N NH-4-THP trtrahydropyranyls 2,4-Me2-Ph 290 N NH-cyclopenta 2,4-Me2-Ph 291 N 1,2,3,4-tetrahydro isoquinolyl 2,4-Me2-Ph
292 N CH
2-(1,2,3,4-tetrahydro isoquinolyl) 2,4-Me2-Ph
293 N OEt 2,4-Me
2-Ph
294 N OCH(Et)CH
2OMe 2,4-Me
2-Ph
295 N OCH
2Ph 2,4-Me
2-Ph 296 N O-3-amyl groups 2,4-Me2-Ph
297 N SEt 2,4-Me
2-Ph
298 N S(O)Et 2,4-Me
2-Ph
299 N SO
2Et 2,4-Me
2-Ph
300 N CH(CO
2Et)
2 2,4-Me
2-Ph
301 N C(Et)(CO
2Et)
2 2,4-Me
2-Ph
302 N CH(Et)CH
2OH 2,4-Me
2-Ph
303 N CH(Et)CH
2OMe 2,4-Me
2-Ph
304 N CONMe
2 2,4-Me
2-Ph
305 N COCH
3 2,4-Me
2-Ph
306 N CH(OH)CH
3 2,4-Me
2-Ph 307 N C (OH) Ph-3-pyridine radicals 2,4-Me2-Ph
308 N Ph 2,4-Me
2-Ph
309 N 2-CF
3-Ph 2,4-Me
2-Ph
310 N 2-Ph-Ph 2,4-Me
2-Ph 311 N 3-amyl groups 2,4-Me2-Ph 312 N cyclobutyl 2,4-Me2-Ph 313 N 3-pyridine radicals 2,4-Me2-Ph
314 N CH(Et)CH
2CONMe
2 2,4-Me
2-Ph
315 N CH(Et)CH
2CH
2NMe
2 2,4-Me
2-Ph
316
an C-Me NEt
22-Br-4-MeO-Ph grease 317amC-Me NH-3-amyl group 2-Br-4-MeO-Ph grease 318aj C-Me NHCH(CH
2CH
2OMe)CH
2OMe 2,4,6-Me
3-Ph 101-103
319
ao C-Me NH(c-C
3H
5) 2,4-Me
2-Ph grease 320akC-Me morpholino 2,4,6-Me3-Ph 139-141
321
ap C-Me NHCH(CH
2OMe)
2 2-CN-4-Me-Ph 152-153
322
aq C-Me N(c-C
3H
5)CH
2CH
2CN 2,4,6-Me
3-Ph 149-151
324
as C-Me NHCH(CH
2CH
2OMe)CH
2OMe 2-Me-4-Br-Ph 115-117
325
at C-Me NHCH(CH
2OMe)
2 2,5-Me
2-4-MeO-Ph 55-57
326
au C-Me N(CH
2CH
2OMe)
2 2,5-Me
2-4-MeO-Ph 72
327
avC-Me NH-3-amyl group 2,5-Me2-4-MeO-Ph 45-47
328
aw C-Me NEt
2 2,5-Me
2-4-MeO-Ph grease 329ax C-Me NHCH(CH
2OMe)
2 2-Cl-4-MePh 80-91
330
ay C-Me NCH(Et)CH
2OMe 2-Cl-4-MePh 77-79
331
az C-Me N(CH
2CH
2OMe)
22-Cl-4-MePh grease 332ba C-Me (S)-NHCH(CH
2CH
2OMe)CH
2OMe 2-Cl-4-MePh 139-140
333
bb C-Me N(c-C
3H
5)CH
2CH
2CN 2,5-Me
2-4-MeOPh 120-122
334
bg C-Me NEt
22-Me-4-MeOPh grease 335bhC-Me OEt 2-Me-4-MeOPh grease 336bi C-Me (S)-NHCH(CH
2CH
2OMe)CH
2OMe 2-Me-4-MeOPh grease 337bj C-Me N(c-C
3H
5)CH
2CH
2CN 2-Me-4-MeOPh 129
338
bk C-Me NHCH(CH
2CH
2OEt)
2The amorphous 339 C-Me N (c-C of 2-Me-4-MeOPh3H
5)CH
2CH
2CN 2,4-Cl
2-Ph 109-110
340 C-Me (S)-NHCH(CH
2CH
2OMe)CH
2OMe 2,4-Cl
2-Ph 93-94 341 C-Me NH-3-amyl group 2-Me-4-BrPh 118-119 342 C-Me N (CH2CH
2OMe)
22-Me-4-BrPh grease 343 C-Me NHCH (CH2-iPr)CH
2OMe 2,4-Me
2-Ph grease 344 C-Me NHCH (Pr) CH2OMe 2,4-Me
2-Ph 94-95
345 C-Me MHCH(Et)CH
2OEt 2,4-Me
2-Ph 76-77
346 C-Me NHCH(CH
2OMe)CH
2CH
2OMe 2-Me-4-Me
2NPh grease 347 C-Me NEt22-Me-4-ClPh grease 348 C-Me NH-3-amyl group 2-Me-4-ClPh 122-124 349 C-Me N (CH2CH
2OMe)
22-Me-4-ClPh grease 350 C-Me NHCH (CH2OMe)
2 2-Me-4-ClPh 122-123
351 C-Me NEt
22-Me-4-ClPh grease 352 C-Me NEt22-Cl-4-MePh grease 353 C-Me NH-3-amyl group 2-Cl-4-MePh 120-121 354 C-Me NHCH (CH2OMe)
2 2-Cl-4-MeOPh
355
bl C-Me N(CH
2CH
2OMe)
22-Cl-4-MeOPh grease 356bm C-Me NHCH(Et)CH
2OMe 2-Cl-4-MeOPh 108-110
357
bn C-Me N(c-Pr)CH
2CH
2CN 2-Cl-4-MeOPh 127-129
358
bo C-Me NEt
22-Cl-4-MeOPh grease 359bpC-Me NH-3-amyl group 2-Cl-4-MeOPh 77-79 360 C-Me NHCH (Et) CH2CH
2OMe 2-Cl-4-MeOPh
361 C-Me NHCH(Me)CH
2CH
2OMe 2-Cl-4-MeOPh
362 C-Me NHCH(Et)CH
2CH
2OMe 2-Br-4-MeOPh
363 C-Me NHCH(Me)CH
2CH
2OMe 2-Br-4-MeOPh
364 C-Me MHCH(Et)CH
2CH
2OMe 2-Me-4-MeOPh
365 C-Me NHCH(Me)CH
2CH
2OMe 2-Me-4-MeOPh
366 C-Me NHCH(CH
2OMe)
2 2-Cl-4,5-(MeO)
2Ph
367 C-Me N(CH
2CH
2OMe)
2 2-Cl-4,5-(MeO)
2Ph
368 C-Me NHCH(Et)CH
2OMe 2-Cl-4,5-(MeO)
2Ph
369 C-Me N(c-Pr)CH
2CH
2CN 2-Cl-4,5-(MeO)
2Ph
370 C-Me NEt
2 2-Cl-4,5-(MeO)
2Ph 371 C-Me NH-3-amyl group 2-Cl-4,5-(MeO)2Ph
372 C-Me NHCH(Et)CH
2CH
2OMe 2-Cl-4,5-(MeO)
2Ph
373 C-Me NHCH(Me)CH
2CH
2OMe 2-Cl-4,5-(MeO)
2Ph
374
bq C-Me NHCH(CH
2OMe)
2 2-Br-4,5-(MeO)
2Ph 137-138
375 C-Me N(CH
2CH
2OMe)
2 2-Br-4,5-(MeO)
2Ph
376
br C-Me NHCH(Et)CH
2OMe 2-Br-4,5-(MeO)
2Ph 147-148
377 C-Me N(c-Pr)CH
2CH
2CN 2-Br-4,5-(MeO)
2Ph
378
bs C-Me NEt
2 2-Br-4,5-(MeO)
2Ph 52-58 379 C-Me NH-3-amyl group 2-Br-4,5-(MeO)2Ph
380 C-Me NHCH(Et)CH
2CH
2OMe 2-Br-4,5-(MeO)
2Ph
381 C-Me NHCH(Me)CH
2CH
2OMe 2-Br-4,5-(MeO)
2Ph
382 C-Me NHCH(CH
2OMe)
2 2-Cl-4,6-(MeO)
2Ph
383 C-Me N(CH
2CH
2OMe)
2 2-Cl-4,6-(MeO)
2Ph
384 C-Me NHCH(Et)CH
2OMe 2-Cl-4,6-(MeO)
2Ph
385 C-Me N(c-Pr)CH
2CH
2CN 2-Cl-4,6-(MeO)
2Ph
396 C-Me NEt
2 2-Cl-4,6-(MeO)
2Ph 387 C-Me NH-3-amyl group 2-Cl-4,6-(MeO)2Ph
388 C-Me NHCH(Et)CH
2CH
2OMe 2-Cl-4,6-(MeO)
2Ph
389 C-Me NHCH(Me)CH
2CH
2OMe 2-Cl-4,6-(MeO)
2Ph
390 C-Me NHCH(CH
2OMe)
2 2-Me-4,6-(MeO)
2Ph
391 C-Me N(CH
2CH
2OMe)
2 2-Me-4,6-(MeO)
2Ph
392 C-Me NHCH(Et)CH
2OMe 2-Me-4,6-(MeO)
2Ph
393 C-Me N(c-Pr)CH
2CH
2CN 2-Me-4,6-(MeO)
2Ph
395 C-Me NEt
2 2-Me-4,6-(MeO)
2Ph 396 C-Me NH-3-amyl group 2-Me-4,6-(MeO)2Ph
397 C-Me NHCH(Et)CH
2CH
2OMe 2-Me-4,6-(MeO)
2Ph
398 C-Me NHCH(Me)CH
2CH
2OMe 2-Me-4,6-(MeO)
2Ph
399 C-Me N(c-Pr)CH
2CH
2CN 2-Br-4,6-(MeO)
2Ph
400 C-Me NEt
2 2-Br-4,6-(MeO)
2Ph 401 C-Me NH-3-amyl group 2-Br-4,6-(MeO)2Ph
402 C-Me NHCH(Et)CH
2CH
2OMe 2-Br-4,6-(MeO)
2Ph
403 C-Me NHCH(Me)CH
2CH
2OMe 2-Br-4,6-(MeO)
2Ph
404 C-Me NHCH(Et)CH
2CH
2OMe 2-Me-4-MeOPh
405 C-Me NHCH(Me)CH
2CH
2OMe 2-Me-4-MeOPh
406 C-Me NHCH(CH
2OMe)
2 2-Me0-4-MePh
407 C-Me N(CH
2CH
2OMe)
2 2-Me0-4-MePh
408 C-Me NHCH(Et)CH
2OMe 2-Me0-4-MePh
409 C-Me N(c-Pr)CH
2CH
2CN 2-Me0-4-MePh
410 C-Me NEt
22-Me0-4-MePh 411 C-Me NH-3-amyl group 2-Me0-4-MePh 412 C-Me NHCH (Et) CH2CH
2OMe 2-Me0-4-MePh
413 C-Me NHCH(Me)CH
2CH
2OMe 2-Me0-4-MePh
414 C-Me NHCH(CH
2OMe)
2 2-Me0-4-MePh
415 C-Me N(CH
2CH
2OMe)
2 2-Me0-4-MePh
416 C-Me NHCH(Et)CH
2OMe 2-Me0-4-MePh
417 C-Me N(c-Pr)CH
2CH
2CN 2-Me0-4-MePh
418 C-Me NEt
22-Me0-4-MePh 419 C-Me NH-3-amyl group 2-Me0-4-MePh 420 C-Me NHCH (Et) CH2CH
2OMe 2-Me0-4-MePh
421 C-Me NHCH(Me)CH
2CH
2OMe 2-Me0-4-MePh
423
bt C-Me NHCH(CH
2OMe)
22-Me0-4-ClPh grease 424 C-Me N (CH2CH
2OMe)
2 2-Me0-4-ClPh
425 C-Me NHCH(Et)CH
2OMe 2-Me0-4-ClPh
426 C-Me N(c-Pr)CH
2CH
2CN 2-Me0-4-ClPh
427 C-Me NEt
22-Me0-4-ClPh 428 C-Me NH-3-amyl group 2-Me0-4-ClPh 429 C-Me NHCH (Et) CH2CH
2OMe 2-Me0-4-ClPh
430 C-Me NHCH(Me)CH
2CH
2OMe 2-Me0-4-ClPh
Table 1 note 1: a) analytical calculation value: C, 52.69, H, 5.17, N, 17.07, Cl,
17.28; Measured value: C, 52.82, H, 5.06, N, 16.77, Cl,
17.50.b) CI-HRMS: calculated value: 406.1565, measured value: 405.1573 (M+H);
Analytical calculation value: C:59.11; H:6.20; N:17.23; Cl:
17.45; Measured value: C:59.93; H:6.34; N:16.50; Cl:
16.95;
NMR(CDCl
3,300MHz):0.95(t,J=8,4H),1.30-
1.40(m,4H),1.50-1.75(m,4H),2.35(s,3H),2.48
(s,3H),4.30-4.45(m,1H),6.15(d,J=8,1H),
7.30 (s, 2H), 7.50 (s, 1H) c) CI-HRMS: calculated value: 392.1409, measured value: 392.1388 (M+H);
NMR(CDCl
3,300MHz):1.00(t,J=8,3H),1.35(t,
J=8,3H),1.41(q,J=8,2H),1.65-1.85(m,2H),
2.30(s,3H),2.40(s,3H),3.85-4.20(m,4H),7.30
(s, 2H), 7.50 (s, 1H) .d) CI-HRMS: calculated value: 404.1409, measured value: 404.1408 (M+H);
NMR(CDCl
3,300MHz):0.35-0.45(m,2H),0.52-0.62
(m,2H),0.98(t,J=8,3H),1.70-1.90(m,2H),
2.30(s,3H),2.40(s,3H),3.85-4.02(m,2H),
4.02-4.20 (m, 2H), 7.30 (s, 2H), 7.50 (s, 1H) .e) CI-HRMS: calculated value: 424.1307, measured value: 424.1307 (M+H):
NMR(CDCl
3,300MHz):2.28(s,3H),2.40(s,3H),
3.40(s,6H),3.75(t,J=8,4H),4.20-4.45(m,
4H), 7.30 (s, 2H), 7.50 (s, 1H) .f) CI-HRMS: calculated value: 406.1565, measured value: 406.1578 (M+H);
NMR(CDCl
3,300MHz):0.90(t,J=8,3H),1.00(t,
J=8,3H),1.28-1.45(m,4H),1.50-1.80(m,4H),
2.35(s,3H),2.50(s,3H),4.20-4.35(m,1H),
6.10-6.23 (m, 1H), 7.30 (s, 2H), 7.50 (s, 1H) .g) CI-HRMS: calculated value: 394.1201, measured value: 394.1209 (M+H);
NMR(CDCl
3,300MHz):1.02(t,J=8,3H),1.65-
1.90(m,2H),2.35(s,3H),2.48(s,3H),3.40(s,
3H),3.50-3.60(m,2H),4.35-4.45(brs,1H),6.50-
6.60 (m, 1H), 7.30 (s, 2H), 7.50 (s, 1H) .h) CI-HRMS: calculated value: 364.1096, measured value: 364.1093 (M+H);
Analytical calculation value: C:56.05; H:5.27; N:19.23; Cl:
19.46; Measured value: C:55.96; H:5.24; N:18.93; Cl:
19.25;
NMR(CDCl
3,300MHz):1.35(t,J=8,6H),2.30(3,
3H),2.40(s,3H),3.95-4.15(m,4H),7.30(s,2H),
(7.50 d, J=1,1H) .i) CI-HRMS: calculated value: 438.1464, measured value: 438.1454 (M+H);
NMR(CDCl
3,300MHz):1.22(t,J=8,6H),2.35(s,
3H),2.47(s,3H),3.39(q,J=8,4H),3.65(dd,J
=8,1,2H),3.73(dd,J=8,1,2H),4.55-4.65(m,
1H),6.75(d,J=8,1H),7.30(d,J=1,2H),7.50
(s, 1H) .j) CI-HRMS: calculated value: 378.1252, measured value: 378.1249 (M+H);
Analytical calculation value: C:57.15; H:5.61; N:18.51; Cl:
1.8.74; Measured value: C:57.56; H:5.65; N:18.35; Cl:
18.45;
NMR(CDCl
3,300MHz):1.00(t,J=8,6H),1.55-
1.70(m,2H),1.70-1.85(m,2H),2.35(s,3H),2.50
(s,3H),4.15-4.25(m,1H),6.18(d,J=8,1H),
7.30 (s, 2H), 7.50 (s, 1H) .k) CI-HRMS: calculated value: 398.0939, measured value: 398.0922 (M+H);
Analytical calculation value: C:60.31; H:4.30; N:17.58; Cl:
17.80; Measured value: C:60.29; H:4.59; N:17.09; Cl:
17.57;
NMR(CDCl
3,300MHz):2.05(s,3H),2.50(s,3H),
3.78(s,3H),7.20-7.45(m,7H),7.50(d,J=1,
1H) .l) CI-HRMS: calculated value: 392.1409, measured value: 392.1391 (M+H);
NMR(CDCl
3,300MHz):0.98(t,J=8,6H),1.70-
1.85(m,4H),2.30(s,3H),2.40(s,3H),3.80-4.10
(m, 4H), 7.30 (s, 2H), 7.50 (d, J=1,1H) .m) CI-HRMS: calculated value: 392.1409, measured value: 392.1415 (M+H);
Analytical calculation value: C:58.17; H:5.92; N:17.85; Cl:
18.07; Measured value: C:58.41; H:5.85:N:18.10; Cl:
17.75;
NMR(CDCl
3,300MHz):0.90-1.05(m,6H),1.35-1.55
(m,2H),1.55-1.85(m,4H),2.35(s,3H),2.48(s,
3H),4.20-4.35(m,1H),6.15(d,J=8,1H),7.30
(s, 2H), 7.50 (d, J=1,1H) .n) CI-HRMS: calculated value: 337.0623, measured value: 337.0689 (M+H);
Analytical calculation value: C:53.43; H:4.18; N:16.62; Cl:
21.03, measured value: C:53.56; H:4.33; N:16.56; Cl:
20.75;
NMR(CDCl
3,300MHz):1.60(t,J=8,3H),2.40(s,
3H),2.55(s,3H),4.80(q,J=8,2H),7.30(d,J
=8,1H),7.35(dd,J=8,1,1H),7.55(d,J=1,
1H) .o) CI-HRMS: calculated value: 383.2321, measured value: 383.2309 (M+H);
NMR(CDCl
3,300MHz):2.00(s,6H),2.20(s,3H),
2.30(s,3H),2.45(s,3H),3.45(s,6H),3.61(dd,
J=8,8,2H),3.70(dd,J=8,8,2H),4.60-4.70
(m, 1H), 6.70 (d, J=8,1H), and 6.94 (s, 2H) .p) CI-HRMS: calculated value: 370.2243, measured value: 370.2246 (M+H);
Analytical calculation value: C:65.02; H:7.38; N:18.96;
Measured value: C:65.22; H:7.39; N:18.71;
NMR(CDCl
3,300MHz):2.18(s,3H),2.30(s,3H),
2.45(s,3H),3.45(s,6H),3.60(dd,J=8,8,
2H),3.69(dd,J=8,8,2H),4.60-4.70(m,1H),
6.70(d,J=8,1H),7.05(d,J=8,1H),7.07(d,
J=8,1H), 7.10 (s, 1H) .q) CI-HRMS: calculated value: 384.2400, measured value: 384.2393 (M+H);
NMR(CDCl
3,300MHz):2.16(s,3H),2.25(s,3H),
2.35(s,3H),2.39(s,3H),3.40(s,6H),3.77(t,
J=8,4H),4.20-4.45(m,4H),7.02(d,J=8,1H)
7.05 (s, 1H), 7.10 (d, J=7,1H) .r) CI-HRMS: calculated value: 354.2294, measured value: 354.2271 (M+H);
Analytical calculation value: C:67.96; H:7.71; N:19.81;
Measured value: C:67.56; H:7.37; N:19.60;
NMR(CDCl
3,300MHz):1.03(t,J=8,3H),1.65-
1.88(m,2H),2.17(s,3H),2.30(s,3H),2.35(s,
3H),2.45(s,3H),3.40(s,3H),3.50-3.62(m,2H),
4.30-4.45(m,1H),6.51(d,J=8,1H),7.04(d,J
=8,1H), 7.10 (d, J=8,1H), and 7.12 (s, 1H) .s) CI-HRMS: calculated value: 338.2345, measured value: 338.2332 (M+H);
Analytical calculation value: C:71.18; H:8.06; N:20.75;
Measured value: C:71.43; H:7.80; N:20.70;
NMR(CDCl
3,300MHz):1.00(t,J=8,6H),1.55-
1.70(m,2H),1.70-1.85(m,2H),2.19(s,3H),2.30
(s,3H),2.35(s,3H),2.46(s,3H),4.15-4.26(m,
1H),6.17(d,J=8,1H),7.06(d,J=8,1H),7.10
(d, J=1,1H), and 7.13 (s, 1H) .t) CI-HRMS: calculated value: 324.2188, measured value: 324.2188 (M+H);
NMR(CDCl
3,300MHz):1.25(t,J=8,6H),2.16(s,
3H),2.28(s,3H),2.35(s,3H),2.40(s,3H),
3.95-4.20(m,4H),7.05(dd,J=8,1,1H),7.07
(s, 1H), 7.10 (d, J=1,1H) u) CI-HRMS: calculated value: 346.1780, measured value: 346.1785 (M+H);
Analytical calculation value: C:66.07; H:5.54; N:28.39;
Measured value: C:66.07; H:5.60; N:27.81;
NMR(CDCl
3,300MHz):2.15(s,3H),2.32(s,3H)
2.17(s,3H),2.52(s,3H),5.25-5.35(m,4H),7.08
(s, 2H), 7.15 (s, 1H) .v) CI-HRMS: calculated value: 340.2137, measured value: 340.2137 (M+H);
Analytical calculation value: C:67.23; H:7.42; N:20.63;
Measured value: C:67.11; H:7.39; N:20.26;
NMR(CDCl
3,300MHz):1.40(d,J=8,3H),2.16(s,
3H),2.32(s,3H),2.35(s,3H),2.47(s,3H),3.42
(s,3H),3.50-3.60(m,2H),4.50-4.15(m,1H),6.56
(d, J=8,1H), and 7.00-7.15 (m, 3H) .w) CI-HRMS: calculated value: 355.2134, measured value: 355.2134 (M+H);
NMR(CDCl
3,300MHz):1.05(t,J=8,3H),1.85-
2.00(m,2H),2.17(s,3H),2.36(s,6H),2.50(s,
3H),3.41(s,3H),3.45(dd,J=8,3,1H),3.82
(dd,J=8,1,1H),5.70-5.80(m,1H),7.00-7.20
(m, 3H) .x) CI-HRMS: calculated value: 364.2501, measured value: 364.2501 (M+H);
NMR(CDCl
3,300MHz):0.35-0.43(m,2H),0.50-0.60
(m,2H),0.98(t,J=8,3H),1.20-1.30(m,1H),
1.72-1.90(m,2H),2.18(s,3H)2.28(s,3H),2.35
(s,3H),2.40(s,3H),3.88-4.03(m,2H),4.03-4.20
(m, 2H), 7.00-7.15 (m, 3H) .y) CI-HRMS: calculated value: 353.2454, measured value: 353.2454 (M+H);
Analytical calculation value: C:68.15; H:8.02; N:23.84;
Measured value: C:67.43; H:7.81; N:23.45;
NMR(CDCl
3.300MHz):1.38(d,J=8,3H),2.18(s,
3H),2.30-2.40(m,12H),2.47 93,3H),2.60-2.75
(m,2H),4.30-4.50(m,1H),6.60-6.70(m,1H),
(7.00-7.15 m, 3H) .z) CI-HRMS: calculated value: 361.2140, measured value: 361.2128 (M+H);
NMR(CDCl
3.300MHz):0.75-0.83(m,2H),1.00-1.10
(m,2H),2.17(s,3H),2.30(s,3H),2.36(s,3H),
2.47(s,3H),2.85(t,J=8,2H),3.30-3.40(m,
1H), and 4.40-4.55 (m, 2H), 7.00-7.18 (m, 3H) .aa) CI-HRMS: calculated value: 363.2297, measured value: 363.2311 (M+H);
NMR(CDCl
3,300MHz):1.01(t,3H,J=8),1.75-1.90
(m,2H),2.15(s,3H),2.19(s,3H),2.35(s,3H),
2.40(s,3H),2.40(s,3H),2.98(t,2H,J=8),
3.97-4.15(m,2H),4.15-4.30(m,2H),7.03(d,1H,
1H), 7.08 (d, 1H, J=8), and 7.10 (s, 1H) .ab) CI-HRMS: calculated value: 363.2297, measured value: 363.2295 (M+H);
NMR(CDCl
3,300MHz):1.01(t,3H,J=8),1.35-
1.55(m,2H),1.75-1.90(m,2H),2.15(s,3H),2.30
(s,3H),2.36(s,3H),2.46(s,3H),4.10-4.30(m,
2H),4.95-5.10(br s,2H),7.05(d,1H,J=8),
7.10 (d, 1H, J=8), and 7.15 (s, 1H) .ac) CI-HRMS: calculated value: 368.2450, measured value: 368.2436;
Analytical calculation value: C, 68.62, H, 7.95, N, 19.06;
Measured value: C, 68.73, H, 7.97, N, 19.09; NMR (CDCl
3, 300
MHz):1.05(t,J=8,3H),1.70-1.90(m,2H),2.01
(d,J=3,6H),2.20(s,3H),2.30(s,3H),2.46,
2.465(s,s,3H),3.42,3.48(s,s,3H),3.53-3.63
(m,2H),4.35-4.45(m,1H),6.73(d,J=8,1H),
6.97 (s, 2H). (ad) CI-HRMS: calculated value: 352.2501, measured value: 352.2500 (M+
H): analytical calculation value: C:71.76; H:8.33; N:19.92,
Measured value: C:71.55; H:8.15; N:19.28;
NMR(CDCl
3,300MHz):1.01(t,J=8,6H),1.58
-1.70(m,2H),1.70-1.85(m,2H),2.02(s,6H),
2.19(s,3H),2.4 5(s,3H),4.12-4.28(m,1H),6.18
(d, J=8,1H), 6.95 (s, 2H). (ae) CI-HRMS: calculated value: 398.2556, measured value: 398.2551 (M+
H); Analytical calculation value: C:66.47; H:7.86; N:17.62,
Measured value: C:66.74; H:7.79; N:17.70;
NMR(CDCl
3,300MHz):2.00(s,6H),2.12(s,3H),
2.30(s,3H),2.37(s,3H),3.40(s,6H),3.78(t,
J=8,4H), 4.25-4.40 (m, 4H), 6.93 (s, 2H). (af) CI-HRMS: calculated value: 450.1141, measured value: 450.1133 (M+H);
Analytical calculation value: C:50.67; H:5.37; N:15.55; Br:
17.74; Measured value: C:52.36; H:5.84; N:14.90; Br:
17.44;
NMR(CDCl
3,300MHz):2.32(s,3H),2.57(s,3H),
3.42(s,6H),3.60(q,J=8,2H),3.69(q,J=8,
2H),3.82(s,3H),4.60-4.70(m,1H),6.73(d,J=
8,1H),6.93(dd,J=8,1,1H),7.22(d,J=8,
1H) .ag) CI-HRMS: calculated value: 434.1192, measured value: 434.1169 (M+H);
Analytical calculation value: C:52.54; H:5.58; N:16.12; Br:
18.40; Measured value: C:52.57; H:5.60; N:15.98; Br:
18.22;
NMR(CDCl
3,300MHz):1.00-1.07(m,3H),1.65-1.85
(m,2H),2.35(s,3H),2.46,2.47(s,s,3H),3.40,
3.45(s,s,3H),3.83(s,3H),4.35-4.45(m,1H),
6.55(d,J=8,1H),6.92(dd,J=8,1,1H),7.20-
(7.30 m, 2H) .ah) CI-HRMS: calculated value: 337.2266, measured value: 337.2251 (M+H);
Analytical calculation value: C:70.18; H:8.06; N:20.75;
Measured value: C:70.69; H:7.65; N:20.34;
NMR(CDCl
3,300MHz):1.35(t,J=8,6H),2.01(s,
6H),2.15(s,3H),2.30(s,3H),2.38(s,3H),4.07
(q, J=8,4H), and 6.93 (s, 2H) .ai) CI-HRMS: calculated value: 412.2713, measured value: 412.2687 (M+H);
Analytical calculation value: C:67.13; H:8.08; N:17.02;
Measured value: C:67.22; H:7.85; N:17.13;
NMR(CDCl
3,300MHz):1.24(t,J=8,6H),2.00(s,
6H),2.20(s,3H),2.30(s,3H),2.43(s,3H),3.60
(q,J=8,4H),3.66(dd,J=8,3,2H),3.75(dd,
J=8,3,2H),4.55-4.65(m,1H),6.75(d,J=8,
1H), 6.95 (s, 2H) .aj) CI-HRMS: calculated value: 398.2556, measured value: 398.2545 (M+H);
Analytical calculation value: C:66.47; H:7.86; N:17.62;
Measured value: C:66.87; H:7.62; N:17.75;
NMR(CDCl
3,300MHz):1.95-2.10(m,8H),2.20(s,
3H),2.32(s,3H),2.44(s,3H),3.38(s,3H),3.42
(s,3H),3.50-3.70(m,4H),4.58-4.70(m,1H),6.87
(d, J=8,1H), and 6.95 (s, 2H) .ak) CI-HRMS: calculated value: 338.1981, measured value: 338.1971 (M+H);
Analytical calculation value: C:67.63; H:6.87; N:20.06;
Measured value: C:67.67; H:6.82; N:20.31;
NMR(CDCl
3,300MHz):2.15(s,3H),2.29(s,3H),
2.35(s,3H),2.43(s,3H),3.90(t,J=8,4H),
4.35-4.45 (m, 4H), 7.00-7.15 (m, 3H) .al) CI-HRMS: calculated value: 464.1297, measured value: 464.1297 (M+H);
NMR(CDCl
3,300MHz):2.28(s,3H),2.40(s,3H),
3.40(s,6H),3.75(t,J=8,4H),3.83(s,3H),
4.20-4.50(m,4H),6.93(dd,J=8,1,1H),7.20
(s, 1H), 7.24 (d, J=1,1H) .am) CI-HRMS: calculated value: 418.1242, measured value: 418.1223 (M+H);
NMR(CDCl
3,300MHz):1.00(t,d,J=8,1,6H),
1.55-1.75(m,4H),2.34(s,3H),2.49(s,3H),2.84
(s,3H),4.15-4.27(m,1H),6.19(d,J=8,1H),
6.93 (dd, J=8,1,1H), and 7.21-7.30 (m, 2H) .an) CI-HRMS: calculated value: 404.1086, measured value: 404.1079 (M+H);
NMR(CDCl
3,300MHz):1.35(t,J=8,6H),2.28(s,
3H),2.40(s,3H),3.83(s,3H),3.90-4.08(m,2H),
4.08-4.20(m,2H),6.92(dd,J=8,1,1H),7.20-
(7.25 m, 2H) .ao) CI-HRMS: calculated value: 308.1875, measured value: 308.1872 (M+H);
NMR(CDCl
3,300MHz):0.75-0.80(m,2H),0.93-1.00
(m,2H),2.16(s,3H),2.28(s,3H),2.35(s,3H),
2.53(s,3H),3.00-3.10(m,1H),6.50-6.55(m,1H),
(7.00-7.15 m, 3H) .ap) CI-HRMS: calculated value: 397.1988, measured value: 397.1984 (M+H);
NMR(CDCl
3,300MHz):2.43(s,3H),2.50(s,3H),
3.43(s,3H),3.61(dd,J=8,8,2H),3.69(dd,J=
8,8,2H),3.88(s,3H),4.58-4.70(m,1H),6.75
(d,J=8,1H),7.20(dd,J=8,1,1H),7.25(d,J
=1,1H), 7.40 (s, 1H) .aq) CI-HRMS: calculated value: 375.2297, measured value: 375.2286 (M+H);
Analytical calculation value: C:70.56; H:7.01; N:22.44;
Measured value: C:70.49; H:6.99; N:22.45;
NMR(CDCl
3,300MHz):0.79-0.85(m,2H),1.00-1.05
(m,1H),2.00(s,6H),2.19(s,3H),2.32(s,3H),
2.44(s,3H),2.84(t,J=8,2H),3.30-3.40(m,
1H), 4.50 (t, J=8,2H), and 6.95 (s, 2H) .ar) CI-HRMS: calculated value: 434.1192, measured value: 434.1189 (M+H);
Analytical calculation value: C:52.54; H:5.58; N:16.12; Br:
18.40; Measured value: C:52.75; H:5.59; N:16.09; Bt:
18.67;
NMR(CDCl
3,300MHz):2.19(s,3H),2.30(s,3H),
2.47(s,3H),3.43(s,6H),3.60(dd,J=8,8,
2H),3.70(dd,J=8,8,2H),4.58-4.70(m,1H),
6.71(d,J=8,1H),7.08(d,J=8,1H),7.37(dd,
J=8,1,1H), and 7.45 (d, J=1,1H) .as) CI-HRMS: calculated value: 448.1348, measured value: 448.1332 (M+H);
Analytical calculation value: C:53.58; H:5.85; N:16.62; Br:
17.82; Measured value: C:53.68; H:5.74; N:15.52; Br:
13.03;
NMR(CDCl
3,300MHz):1.95-2.10(m,2H),2.20(s,
3H),2.30(s,3H),2.47(s,3H),3.28(s,3H),3.41
(s,3H),3.50-3.67(m,4H),4.55-4.70(m,1H),6.89
(d,J=8,1H),7.05(d,J=8,1H),7.35(dd,J=
8,1,1H), 7.47 (d, J=1,1H) .at) CI-HRMS: calculated value: 400.2349, measured value: 400.2348 (M+H);
Analytical calculation value: C:C:63.14; H:7.32; N:17.53;
Measured value: C:63.40; H:7.08; N:17.14;
NMR(CDCl
3,300MHz):2.16(s,3H),2.20(s,3H),
2.30(s,3H),2.46(s,3H),3.42(s,6H),3.60(q,
J=8,2H),3.70(q,J=8,2H),3.85(s,3H),
4.59-4.70(m,1H),6.70(d,J=8,1H),6.76(s,
1H), 6.96 (s, 1H) .au) CI-HRMS: calculated value: 414.2505, measured value: 414.2493 (M+H);
NNR(CDCl
3,300MHz):2.15(s,3H),2.19(s,3H),
2.25(s,3H),2.40(s,3H),3.40(s,6H),3.76(t,
J=8,4H),3.84(s,3H),4.20-4.45(m,4H),6.77
(s, 1H), 6.93 (s, 1H) .av) CI-HRMS: calculated value: 368.2450, measured value: 368.2447 (M+H);
NMR(CDCl
3,300MHz):1.00(t,J=8,6H),1.55-
1.85(m,4H),2.19(s,3H),2.20(s,3H),2.30(s,
3H),2.47(s,3H),3.88(s,3H),4.10-4.30(m,1H),
6.15 (d, J=8,1H), 6.78 (s, 1H), 6.98 (s, 1H) .aw) CI-HRMS: calculated value: 353.2216, measured value: 353.2197 (M+H);
NMR(CDCl
3,300MHz):1.35(t,J=8,6H),2.17(s,
3H),2.19(s,3H),2.28(s,3H),2.40(s,3H),3.85
(s,3H),3.90-4.20(m,4H),6.78(s,1H),6.95(s,
1H) .ax) CI-HRMS: calculated value: 390.1697, measured value: 390.1688 (M+H);
Analytical calculation value: C:58.53; H:6.20; N:17.96; Cl:
9.09; Measured value: C:58.95; H:6.28; N:17.73; Cl:9.15;
NMR(CDCl
3,300MHz):2.35(s,3H),2.37(s,3H),
2.48(s,3H),3.42(s,6H),3.60(dd,J=8,8,2H)
3.68(dd,J=8,8,2H),4.59-4.72(m,1H),6.72
(d,J=8,1H),7.12(d,J=8,1H),7.23(d,J=
8,1H), 7.32 (s, 1H) .ay) CI-HRMS: calculated value: 374.1748, measured value: 374.1735 (M+H);
Analytical calculation value: C:61.04; H:6.47; N:18.73; Cl:
9.48; Measured value: C:61.47; H:6.54; N:18.23; Cl:9.61;
NMR(CDCl
3,300MHz):1.01(t,J=8,3H),1.62-
1.88(m,4H),2.35(s,3H),2.37(s,3H),2.48(d,
J=1,3H),3.40,3.45(s,s,3H),3.50-3.64(m,
2H),4.38-4.47(m,1H),6.53(d,J=8,1H),7.12
(d, J=8,1H), 7.07 (d, J=8,1H), and 7.12 (s, 1H) .az) CI-HRMS: calculated value: 404.1853, measured value: 404.1939 (M+H);
NMR(CDCl
3,300MHz):2.29(s,3H),2.38(s,3H),
2.40(s,3H),3.40(s,6H),3.76(t,J=8,4H),
4.20-4.45(m,4H),7.11(d,J=8,1H),7.22(d,J
=8,1H), 7.31 (s, 1H) .ba) CI-HRMS: calculated value: 404.1853, measured value: 404.1859 (M+H);
Analytical calculation value: C:59.47; H:6.50; N:17.34; Cl:8.79;
Measured value: C:59.73; H:6.46; N:17.10; Cl:8.73;
NMR(CDCl
3,300MHz):1.95-2.08(m,2H),2.35(s,
3H),2.38(s,3H),2.46(s,3H),3.38(s,3H),3.41
(s,3H),3.50-3.65(m,4H),4.56-4.70(m,1H),6.85
(d,J=8,1H),7.12(d,J=8,1H),7.45(d,J=
8,1H), 7.32 (s, 1H) .bb) CI-HRMS: calculated value: 391.2246, measured value: 391.2258 (M+H);
Analytical calculation value: C:67.67; H:6.71; N:21.52; Measured value: C:
67.93;H:6.70;N:21.48;
NMR(CDCl
3,300MHz):0.76-0.84(m,2H),0.84-0.91
(m,2H),1.00-1.08(m,2H),2.15(s,3H),2.20(s,
3H),2.29(s,3H),2.45(s,3H),2.85(t,J=8,
2H),3.28-3.30(m,1H),3.85(s,3H),6.78(s,1H),
(6.95 s, 1H) .bc) CI-HRMS: calculated value: 386.2192, measured value: 386.2181 (M+H);
Analytical calculation value: C:62.32; H:7.06; N:18.17; Measured value: C:
62.48;H:6.83;N:18.15;
NMR(CDCl
3,300MHz):7.1(d,1H,J=8),6.9(d,
1H,J=1),6.8(dd,1H,J=8,1),6.7(br.d,1H,
J=8),4.7-4.6(m,1H),3.85(s,3H),3.70-3.55
(m,4H),3.45(s,6H),2.5(s,3H),2.3(s,3H),
(2.15 s, 3H) .bd) CI-HRMS: calculated value: 400.2349, measured value: 400.2336 (M+H);
NMR(CDCl
3,300MHz):7.1(d,1H,J=7),6.85(d,
1H,J=1),6.75(dd,1H,J=7,1),4.45-4.25
(br.s,4H),3.75(t,4H,J=7),3.4(s,6H),2.4
(s, 3H), 2.25 (s, 3H), 2.15 (s, 3H) .be) CI-HRMS: calculated value: 370.2243, measured value: 370.2247 (M+H);
Analytical calculation value: C:65.02; H:7.38; N:18.96; Measured value: C:
65.28;H:7.27;N:18.71:
NMR(CDCl
3,300MHz):7.1(d,1H,J=8),6.85(d,
1H,J=1),6.8(dd,1H,J=8,1),6.5(br.d,1H,
J=1),4.5-4.3(m,1H),3.85(s,3H),3.65-3.5(m,
2H),3.4(s,2H),2.5(s,3H),2.3(s,3H),2.2(s,
3H), and 1.9-1.7 (m, 2H), 1.05 (t, 3H, J=7) .bf) CI-HRMS: calculated value: 379.2246, measured value: 379.2248 (M+H);
NMR(CDCl
3,300MHz):7.1(d,1H,J=8),6.85(d,
1H,J=1),6.8(dd,1H,J=8,1),4.3-4.0(m,4H),
3.85(s,3H),3.0(t,2H,J=7),2.45(s,3H),2.3
(s,3H),2.2(s,3H),1.9-1.8(m,2H),1.0(t,3H,
J=7) CI-HRMS .bg): calculated value: 340.2137, measured value: 340.2122 (M+H);
NMR(CDCl
3,300MHz):7.1(d,1H,J=8),6.85(d,
1H,J=1),6.75(dd,1H,J=8,1),4.2-4.0(br.m,
4H),3.85(s,3H,2.4(s,3H),2.3(s,3H),2.2
(s, 3H), 1.35 (t, 6H, J=7) .bh) CI-HRMS: calculated value: 313.1665, measured value: CI-HRMS 313.6664 (M+H) .bi): calculated value: 400.2349, measured value: 400.2346 (M+H);
NMR(CDCl
3,300MHz):7.1(d,1H,J=7),6.9-6.75
(m,3H),4.7-4.55(m,1H),3.8(s,3H),3.7-3.5(m,
4H),3.45(s,3H),3.35(s,3H),2.5(s,3H),2.3
(s, 3H), 2.2 (s, 3H), 2.1-1.95 (m, 2H) .bj) CI-HRMS: calculated value: 377.2090, measured value: 377.2092 (M+H);
Analytical calculation value: C:67.00; H:6.44; N:22.32; Measured value: C:
67.35;H:6.44;N:22.23;
NMR(CDCl
3,300MHz):7.1(d,1H,J=8),6.9(d,
1H,J=1),6.8(dd,1H,J=8,1),4.55-4.4(m,
2H),3.85(s,3H),3.4-3.3(m,1H),2.85(t,2H,J
=7),2.5(s,3H),2.3(s,3H),2.2(s,3H),1.1-
1.0 (m, 2H), 0.85-0.75 (m, 2H) .bk) CI-HRMS: calculated value: 413.2427, measured value: 413.2416 (M+H);
NMR(CDCl
3,300Hz):7.1(d,1H,J=8),6.85(d,
1H,J=1),6.75(dd,1H,J=8,1),4.6(m,1H),
3.85(s,3H),3.75-3.6(m,4H),3.6(q,4H,J=7),
2.5(s,3H),2.3(s,3H),2.2(s,3H),1.25(t,6H,
J=7) CI-HRMS .bl): calculated value: 420.1802, measured value: 420.1825 (M+H); Bm) CI-HRMS: calculated value: 390.1697, measured value: 390.1707 (M+H); Bn) CI-HRMS: calculated value: 397.1465, measured value: 397,1462 (M+H); Bo) CI-HRMS: calculated value: 360.1513, measured value: 360.1514 (M+H); Bp) CI-HRMS: calculated value: 374.1748, measured value: 374.1737 (M+H); Bq) CI-HRMS: calculated value: 479.1155, measured value: 479.1154 (M+H); Br) CI-HRMS: calculated value: 463.1219, measured value: 463.1211 (M+H);
Analytical calculation value: C:51.96, H:5.23, N, 15.15, Br:
17.28; Measured value: C:52.29, H:5.62, N:14.79, Br:
17.47bs) CI-HRMS: calculated value: 433.1113, measured value: 433.1114 (M,
79Br); Bt) NH
3-CI MS: calculated value: 406, measured value: 406 (M+H)+; NMR (CDCl
3, 300MHz): δ 7.28 (d, J=10Hz, 1H), 7.03 (d, J=8Hz, 1H), 6.96 (s, 1H), 6.7 (d, J=9,1H), 4.63 (m, 1H), 3.79 (s, 3H), 3.6 (m, 4H), 3.42 (s, 6H), 2.47 (s, 3H), 2.32 (s, 3H).
Embodiment 431
2,4, the preparation of 7-dimethyl-8-(4-methoxyl group-2-aminomethyl phenyl) [1,5-a]-pyrazolo-1,3,5-triazines
(formula 1, wherein R
3Be CH
3, R
1Be CH
3, Z is C-CH
3, Ar is 2, the 4-3,5-dimethylphenyl)
(602mg 2mmol) mixes with saturated sodium hydrogen carbonate solution (10ml) with 5-ethanamidine base-4-(4-methoxyl group-2-aminomethyl phenyl)-3-methylpyrazole acetate.With ethyl acetate this water soluble mixt is extracted three times.Organic layer through dried over mgso merges filters and vacuum concentration.Residue is dissolved in the toluene (10ml), in this suspension, add trimethyl orthoacetate (0.36g, 3mmol).Under nitrogen environment, this reaction mixture is heated to reflux temperature, and stirred 16 hours.After being cooled to room temperature, this reaction mixture of vacuum concentration obtains the oily solid.(chloroform: methyl alcohol=9: 1), vacuum obtains yellow sticking oily matter (R after removing solvent to column chromatography
f=0.6,210mg, 37% productive rate): NMR (CDCl
3, 300MHz), 7.15 (d, 1H, J=8), 6.9 (d, 1H, J=1), 6.85 (dd, 1H, J=8,1), 3.85 (s, 3H), 2.95 (s, 3H), 2.65 (s, 3H), 2.4 (s, 3H), 2.15 (s, 3H); CI-HRMS: calculated value: 283.1559, measured value: 283.1554 (M+H).
Embodiment 432
7-hydroxy-5-methyl base-3-(2-chloro-4-aminomethyl phenyl) pyrazolo [1,5-a] pyrimidine
(formula 1, wherein A is CH, R
1Be Me, R
3Be OH, Z is C-Me, and Ar is a 2-chloro-4-aminomethyl phenyl)
Under agitation, with 5-amino-4-(2-chloro-4-aminomethyl phenyl)-(1.86g 8.4mmol) is dissolved in the glacial acetic acid (30ml) the 3-methylpyrazole.In the solution that produces, drip then methyl aceto acetate (1.18ml, 9.2mmol).Then this reaction mixture is heated to reflux temperature, stirred 16 hours, be cooled to room temperature.Add ether (100ml), filter and collect the precipitation that produces.Vacuum-drying obtains white solid (1.0g, 42% productive rate): NMR (CDCl
3, 300MHz), 8.70 (br.s1H), 7.29 (s, 1H), 7.21-7.09 (m, 2H), 5.62 (s, 1H), 2.35 (s, 6H), 2.29 (s, 3H); CI-MS:288 (M+H).
Embodiment 433
7-chloro-5-methyl-3-(2-chloro-4-aminomethyl phenyl) pyrazolo [1,5-a] pyrimidine
(formula 1, wherein A is CH, R
1Be Me, R
3Be Cl, Z is C-Me, and Ar is a 2-chloro-4-aminomethyl phenyl)
Under reflux temperature, with 7-hydroxy-5-methyl base-3-(2-chloro-4-aminomethyl phenyl) pyrazolo [1,5-a] pyrimidine (1.0g, 3.5mmol), phosphoryl chloride (2.7g, 1.64ml, 17.4mmol), N, N-Diethyl Aniline (0.63g, 0.7ml, 4.2mmol) and toluene (20ml) mixture stirred 3 hours, be cooled to room temperature then.Vacuum is removed volatile matter.Residue is through flash chromatography (ethyl acetate: hexane=1: 2) obtain 7-chloro-5-methyl-3-(2-chloro-4-aminomethyl phenyl) pyrazolo [1,5-a] pyrimidine (900mg, 84% productive rate), be yellow oil: NMR (CDCl
3, 300MHz): 7.35 (s, 1H), 7.28-7.26 (m, 1H), 71.6 (d, 1H, J=7), 6.80 (s, 1H), 2.55 (s, 3H), 2.45 (s, 3H), 2.40 (s, 3H); CI-MS:306 (M+H).
Embodiment 434
7-(amyl group-3-amino)-5-methyl-3-(2-chloro-4-aminomethyl phenyl) pyrazolo [1,5-a] pyrimidine
(formula 1, wherein A is CH, R
1Be Me, R
3Be amyl group-3-amino, Z is C-Me, and Ar is a 2-chloro-4-aminomethyl phenyl)
In 150 ℃, (394mg, 6.5mmol) (200mg, (DMSO, 10ml) solution stirring is 2 hours, is cooled to room temperature then for dimethyl sulfoxide (DMSO) 0.65mmol) with 7-chloro-5-methyl-3-(2-chloro-4-aminomethyl phenyl) pyrazolo [1,5-a] pyrimidine with the 3-amylamine.Then this reaction mixture is inclined to water (100ml), and mix.With dichloromethane extraction three times, the organic layer that merges with the salt water washing through dried over mgso, filters and vacuum is removed solvent, obtains yellow solid.Through flash chromatography (ethyl acetate: hexane=1: 4) obtain white solid (140mg, 60% productive rate):
Mp 139-141 ℃; NMR (CDCl
3, 300Hz): 7.32 (s, 1H), 7.27 (d, 1H, J=8), 7.12 (d, 1H, J=7), 6.02 (d, 1H, J=9), 5.78 (s, 1H), 3.50-3.39 (m, 1H), 2.45 (s, 3H), 2.36 (s, 6H), 1.82-1.60 (m, 4H), 1.01 (t, 6H, J=8); Analytical calculation value C
20H
25ClN
4: C, 67.31, H, 7.06, N, 15.70, Cl:9.93; Measured value: C, 67.32, H, 6.95, N, 15.50, Cl, 9.93.
According to embodiment 1A, 1B, 432,433,434 described methods, can prepare the compound of the described embodiment of table 2.Commonly used is abbreviated as: Ph is a phenyl, and Pr is a propyl group, and Me is a methyl, and Et is an ethyl, and Bu is a butyl, and Ex is embodiment, and EtOAc is an ethyl acetate.
Table 2
Ex Z R3 Ar Mp (℃)435
bC-Me N (CH
2CH
2OMe)
22,4-Cl
2-Ph 71-73436
cC-Me N (Bu) Et 2,4-Cl
2-Ph 86-87437
dC-Me NHCH (Et) CH
2OMe 2,4-Cl
2-Ph 110-111438
eC-Me N (Pr) CH
2CH
2CN 2,4-Cl
2-Ph 83-85439
fC-Me NH-3-amyl group 2,4-Cl
2-Ph 175-176440
gC-Me NHCH (CH
2OMe)
22,4-Cl
2-Ph 107441
hC-Me NHCH (Et)
22,4-Me
2-Ph oily matter 442
iC-Me NHCH (CH
2OMe)
22,4-Me
2-Ph 103-105443
jC-Me N (CH
2CH
2OMe)
22,4-Me
2-Ph 87-89444
kC-Me N (c-Pr) CH
2CH
2CN 2,4-Me
2-Ph 133 (dec) 445
lC-Me N (CH
2CH
2OMe)
22-Cl, 4-MePh 77-78446
mC-Me NHCH (CH
2OMe)
22-Cl, 4-MePh 131-133447
nC-Me NHCH (Et)
22-Cl, 4-MePh 139-141448
oC-Me NEt
22,4-Me
2-Ph 92-94449
pC-Me N (Pr) CH
2CH
2CN 2,4-Me
2-Ph 143-144450
qC-Me N (Bu) CH
2CH
2CN 2,4-Me
2-Ph 115-117451
rC-Me NHCH (Et) CH
2OMe 2,4-Me
2-Ph oily matter 452
sC-Me NHCH (Et)
22-Me, 4-MeOPh 104-106453
tC-Me NHCH (CH
2OMe)
22-Me, 4-MeOPh 115-116454
uC-Me N (CH
2CH
2OMe)
22-Me, 4-MeOPh oily matter 455
vC-Me (S)-NHCH (CH
2CH
2OMe)-and 2-Me, 4-MeOPh oily matter
(CH
2OMe) 456
wC-Me (S)-NHCH (CH
2CH
2OMe)-2,4-Me
2-Ph oily matter
(CH
2OMe) 457
xC-Me N (CH
2CH
2OMe)
22-Me, 4-ClPh oily matter 458
yC-Me NHEt 2,4-Me
2-Ph oily matter 459
zC-Me NHCH (Et)
22-Me, 4-ClPh 94-96460
AaC-Me NHCH (CH
2OMe)
22-Me, 4-ClPh 113-114461
AbC-Me N (Ac) Et 2,4-Me
2-Ph oily matter 462
AcC-Me (S)-NHCH (CH
2CH
2OMe)-and 2-Me, 4-ClPh oily matter
(CH
2OMe)463
ad C-Me N(Pr)CH
2CH
2CN 2-Me,4-MeOPh 118-119464
ae C-Me NEt
2 2-Me,4-MeOPh 97-99465
af C-Me (S)-NHCH(CH
2CH
2OMe)- 2-Cl,4-MePh 101-103
(CH
2OMe)
466
ag C-Me NEt
2 2-Cl,4-MePh 129-130
467
ah C-Me N(c-Pr)CH
2CH
2CN 2-Me,4-MeOPh 177-178
468
ai C-Me N(c-Pr)CH
2CH
2CN 2-Cl,4-MePh 162-163
469
aj C-Me NHCH(Et)CH
2OMe 2-Me, 4-MeOPh grease 470ak C-Me NHCH(Et)CH
2OMe 2-Cl,4-MePh 111-113
471 C-Me NHCH(CH
2OMe)
2 2-Cl-4-MeOPh
472 C-Me N(CH
2CH
2OMe)
2 2-Cl-4-MeOPh
473 C-Me NHCH(Et)CH
2OMe 2-Cl-4-MeOPh
474 C-Me N(c-Pr)CH
2CH
2CN 2-Cl-4-MeOPh
475 C-Me NEt
22-Cl-4-MeOPh 476 C-Me NH-3-amyl group 2-Cl-4-MeOPh 477 C-Me NHCH (Et) CH2CH
2OMe 2-Cl-4-MeOPh
478 C-Me NHCH(Me)CH
2CH
2OMe 2-Cl-4-MeOPh
479 C-Me NHCH(Et)CH
2CH
2OMe 2-Er-4-MeOPh
480 C-Me NHCH(Me)CH
2CH
2OMe 2-Br-4-MeOPh
481 C-Me NHCH(Et)CH
2CH
2OMe 2-Me-4-MeOPh
482 C-Me NHCH(Me)CH
2CH
2OMe 2-Me-4-MeOPh
483 C-Me NHCH(CH
2OMe)
2 2-Cl-4,5-(MeO)
2Ph
484 C-Me N(CH
2CH
2OMe)
2 2-Cl-4,5-(MeO)
2Ph
485 C-Me NHCH(Et)CH
2OMe 2-Cl-4,5-(MeO)
2Ph
486 C-Me N(c-Pr)CH
2CH
2CN 2-Cl-4,5-(MeO)
2Ph
487 C-Me NEt
2 2-Cl-4,5-(MeO)
2Ph 99-101 488 C-Me NH-3-amyl group 2-Cl-4,5-(MeO)2Ph 169-170
489 C-Me NHCH(Et)CH
2CH
2OMe 2-Cl-4,5-(MeO)
2Ph
490 C-Me NHCH(Me)CH
2CH
2OMe 2-Cl-4,5-(MeO)
2Ph
491 C-Me NHCH(CH
2OMe)
2 2-Br-4,5-(MeO)
2Ph 90-93
492 C-Me N(CH
2CH
2OMe)
2 2-Br-4,5-(MeO)
2Ph 110
493 C-Me NHCH(Et)CH
2OMe 2-Br-4,5-(MeO)
2Ph
494 C-Me N(c-Pr)CH
2CH
2CN 2-Br-4,5-(MeO)
2Ph
495 C-Me NEt
2 2-Br-4,5-(MeO)
2Ph 496 C-Me NH-3-amyl group 2-Br-4,5-(MeO)2Ph
497 C-Me NHCH(Et)CH
2CH
2OMe 2-Br-4,5-(MeO)
2Ph
498 C-Me NHCH(Me)CH
2CH
2OMe 2-Br-4,5-(MeO)
2Ph
499 C-Me NHCH(CH
2OMe)
2 2-Cl-4,6-(MeO)
2Ph
500 C-Me N(CH
2CH
2OMe)
2 2-Cl-4,6-(MeO)
2Ph
501 C-Me NHCH(Et)CH
2OMe 2-Cl-4,6-(MeO)
2Ph
502 C-Me N(c-Pr)CH
2CH
2CN 2-Cl-4,6-(MeO)
2Ph
503 C-Me NEt
2 2-Cl-4,6-(MeO)
2Ph 504 C-Me NH-3-amyl group 2-Cl-4,6-(MeO)2Ph
505 C-Me NHCH(Et)CH
2CH
2OMe 2-Cl-4,6-(MeO)
2Ph
506 C-Me NHCH(Me)CH
2CH
2OMe 2-Cl-4,6-(MeO)
2Ph
507 C-Me NHCH(CH
2OMe)
2 2-Me-4,6-(MeO)
2Ph
508 C-Me N(CH
2CH
2OMe)
2 2-Me-4,6-(MeO)
2Ph
509 C-Me NHCH(Et)CH
2OMe 2-Me-4,6-(MeO)
2Ph
510 C-Me N(c-Pr)CH
2CH
2CN 2-Me-4,6-(MeO)
2Ph
511 C-Me NEt
2 2-Me-4,6-(MeO)
2Ph 512 C-Me NH-3-amyl group 2-Me-4,6-(MeO)2Ph
513 C-Me NHCH(Et)CH
2CH
2OMe 2-Me-4,6-(MeO)
2Ph
514 C-Me NHCH(Me)CH
2CH
2OMe 2-Me-4,6-(MeO)
2Ph
515 C-Me N(c-Pr)CM
2CH
2CN 2-Br-4,6-(MeO)
2Ph
516 C-Me NEt
2 2-Br-4,6-(MeO)
2Ph 517 C-Me NH-3-amyl group 2-Br-4,6-(MeO)2Ph
518 C-Me NHCH(Et)CH
2CH
2OMe 2-Br-4,6-(MeO)
2Ph
519 C-Me NHCH(Me)CH
2CH
2OMe 2-Br-4,6-(MeO)
2Ph
520 C-Me NHCH(Et)CH
2CH
2OMe 2-Me-4-MeOPh
521 C-Me NHCH(Me)CH
2CH
2OMe 2-Me-4-MeOPh
522 C-Me NHCH(CH
2OMe)
2 2-Me0-4-MePh
523 C-Me N(CH
2CH
2OMe)
2 2-Me0-4-MePh
524 C-Me NHCH(Et)CH
2OMe 2-Me0-4-MePh
525 C-Me N(c-Pr)CH
2CH
2CN 2-Me0-4-MePh
526 C-Me NEt
22-Me0-4-MePh 527 C-Me NH-3-amyl group 2-Me0-4-MePh 528 C-Me NHCH (Et) CH2CH
2OMe 2-Me0-4-MePh
529 C-Me NHCH(Me)CH
2CH
2OMe 2-Me0-4-MePh
530 C-Me NHCH(CH
2OMe)
2 2-Me0-4-MePh
531 C-Me N(CH
2CH
2OMe)
2 2-Me0-4-MePh
532 C-Me NHCH(Et)CH
2OMe 2-Me0-4-MePh
533 C-Me N(c-Pr)CH
2CH
2CN 2-Me0-4-MePh
534 C-Me NEt
22-Me0-4-MePh 535 C-Me NH-3-amyl group 2-Me0-4-MePh 536 C-Me NHCH (Et) CH2CH
2OMe 2-Me0-4-MePh
537 C-Me NHCH(Me)CH
2CH
2OMe 2-Me0-4-MePh
538 C-Me NHCH(CH
2OMe)
2 2-Me0-4-ClPh
539 C-Me N(CH
2CH
2OMe)
2 2-Me0-4-ClPh
540 C-Me NHCH(Et)CH
2OMe 2-Me0-4-ClPh
541 C-Me N(c-Pr)CH
2CH
2CN 2-Me0-4-ClPh
542 C-Me NEt
22-Me0-4-ClPh 543 C-Me NH-3-amyl group 2-Me0-4-ClPh 544 C-Me NHCH (Et) CH2CH
2OMe 2-Me0-4-ClPh
545 C-Me NHCH(Me)CH
2CH
2OMe 2-Me0-4-ClPh
Table 2 note b) CI-HRMS: calculated value: 423.1355; Measured value: analytical calculation value: C 423.1337 (M+H) .c), 61.38, H, 6.18, N, 14.32:
Measured value: C, 61.54, H, 6.12, N, 14.37.d) analytical calculation value: C:58.02, H, 5.65, N, 14.24;
Measured value: C, 58.11, H, 5.52, N, 14.26.e) analytical calculation value: C, 59.71, H, 5.26,14.85;
Measured value: C, 59.94, H, 5.09, N, 17.23.f) analytical calculation value: C, 60.48H, 5.89, N, 14.85,
Measured value: C, 60.62, H, 5.88, N, 14.82.h) CI-HRMS: calculated value: 337.2388; Measured value: analytical calculation value: C 337.2392 (M+H) .i), 68.45, H, 7.669, N, 15.21,
Measured value: C, 68.35, H, 7.49 N, 14.91.j) analytical calculation value: C, 69.08, H, 7.915, N, 14.65,
Measured value: C, 68.8 5, H, 7.83, N, 14.54.k) analytical calculation value: C, 73.51, H, 7.01, N, 19.48,
Measured value: C, 71.57, H, 7.15, N, 19.12.l) CI-HRMS: calculated value: 403.1899; Measured value: analytical calculation value: C 403.1901 (M+H) .m), 61.77, H, 6.49, N, 14.41, Cl.
9.13; Measured value: C, 61.90, H, 6.66, N, 13.62, Cl, 9.25.n) analytical calculation value: C, 67.31, H, 7.06, N, 15.70, Cl.
9.93; Measured value: C, 67.32, H, 6.95, N, 15.50, Cl, 9.93.o) analytical calculation value: C, 74.50, H, 8.14, N, 17.38,
Measured value: C, 74.43, H, 7.59, N, 17.16.p) analytical calculation value: C, 73.1O, H, 7.54, N, 19.37,
Measured value: C, 73.18, H, 7.59, N, 18.81.q) analytical calculation value: C, 73.57, H, 7.78, N, 18.65,
Measured value: C, 73.55, H, 7.79, N, 18.64.r) CI-HRMS: calculated value: 353.2333; Measured value: analytical calculation value: C 353.2341 (M+H) .s), 71.56, H, 8.02, N, 15.90,
Measured value: C, 71.45, H, 7.99, N, 15.88.t) analytical calculation value: C, 65.60, H, 7.34, N, 14.57,
Measured value: C, 65.42, H, 7.24, N, 14.37.u) CI-HRMS: calculated value: 399.2398; Measured value: CI-HRMS 399.2396 (M+H) .v): calculated value: 399.2398; Measured value: CI-HRMS 399.2396 (M+H) .w): calculated value: 383.2450; Measured value: CI-HRMS 383.2447 (M+H) .x): calculated value: 403.1887; Measured value: CI-HRMS 403.1901 (M+H) .y): calculated value: 295.1919; Measured value: analytical calculation value: C 295.1923 (M+H) .z), 67.31, H, 7.06, N, 15.70,
Measured value: C, 67.12, H, 6.86, N, 15.53.aa) analytical calculation value: C, 61.77, H, 6.49, N, 14.41, Cl,
9.13; Measured value: C, 62.06, H, 6.37, N, 14.25, Cl, 9.12.ab) CI-HRMS: calculated value: 337.2017; Measured value: CI-HRMS 337.2028 (M+H) .ac): calculated value: 403.1893; Measured value: analytical calculation value: C 403.1901 (M+H) .ad), 70.00, H, 7.22, N, 18.55,
Measured value: C, 7O.05, H, 7.22, N, 18.36.ae) analytical calculation value: C, 70.98, H, 7.74, N, 16.55,
Measured value: C, 71.15, H, 7.46, N, 16.56.ag) analytical calculation value: C, 66.59, H, 6.76, N, 16.34,
Measured value: C, 66.69, H, 6.82, N, 16.20.ah) analytical calculation value: C, 70.38, H, 6.71, N, 18.65,
Measured value: C, 7O.35, H, 6.82, N, 18.83.ai) analytical calculation value: C, 66.39, H, 5.85, N, 18.44, Cl,
9.33;
Measured value: C, 66.29, H, 5.51, N, 18.36, Cl, 9.31.aj) CI-HRMS: calculated value: 369.2278; Measured value: analytical calculation value: C 369.2291 (M+H) .ak), 64.42, H, 6.77, N, 15.02,
Measured value: C, 64.59, H, 6.51, N, 14.81.
According to embodiment 1,2,3 or 6 described methods, can prepare the compound of the described embodiment of table 3.Commonly used is abbreviated as: Ph is a phenyl, and Pr is a propyl group, and Me is a methyl, and Et is an ethyl, and Bu is a butyl, and Ex is embodiment.
Table 3
Ex Z R3 Ar Mp (℃)546
aC-Me NHCH (Et)
22-Me-4-Me
2N-Ph 164-166547
bC-Me S-NHCH (CH
2CH
2OMe) 2,4-Me
2-Ph oily matter
-CH
2OMe548
cC-Me S-NHCH (CH
2CH
2OMe) 2-Me-4-Cl-Ph oily matter
-CH
2OMe
549
d C-Me N(c-Pr)CH
2CH
2CN 2-Me-4-Cl-Ph 115-116
550
e C-Me NHCH(Et)CH
2CN 2-Me-4-Cl-Ph 131-132
551
f C-Me N(Et)
2 2,3-Me
2-4-OMe-Ph grease 552g C-Me N(CH
2CH
2OMe)CH
2CH
2OH 2,4-Cl
2-Ph grease 553h C-Me N(CH
2CH
2OMe)
2 2,3-Me
2-4-OMe-Ph grease 554i C-Me NHCH(Et)
2 2,3-Me
2-4-OMePh 123-124
555
j C-Me N(CH
2-c-Pr) Pr 2-Me-4-Cl-Ph grease 556k C-Me N(c-Pr)CH
2CH
2CN 2,3-Me
2-4-OMePh 158-160
557 C-Me N(c-Pr)Et 2-Cl-4-OMePh
558 C-Me N(c-Pr)Me 2-Cl-4-OMePh
559 C-Me N(c-Pr)Pr 2-Cl-4-OMePh
560 C-Me N(c-Pr)Bu 2-Cl-4-OMePh
561
l C-Me N(Et)
2 2-Cl-4-CN-Ph 115-117
562 C-Me N(c-Pr)
2 2-Cl-4-OMe 127-129
563
m C-Me NHCH(CH
2OH)
2 2,4-Cl
2-Ph 128-129
564 C-Me N(c-Pr)Et 2-Br-4,5-(MeO)2Ph
565 C-Me N(c-Pr)Me 2-Br-4,5-(MeO)2Ph
566 C-Me NH-c-Pr 2-Me-4-MeOPh 126-128
567 C-Me NHCH(Et)CH2OH 2-Me-4-MeOPh 60-62
568 C-Me NMe
2 2-Br-4,5-(MeO)2Ph
569 C-Me NHCH(Et)
22-Me-4-MeOPh 103-105 570 C-Me N (c-Pr) Et 2-Me-4-MeOPh 173-174 571 C-Me NH-2-amyl groups 2,4-Cl2-Ph 118-120
572 C-Me NHCH(Et)CH2CN 2,4-Cl
2-Ph 141-142
573 C-Me NHCH(Pr)CH2OMe 2,4-Cl
2-Ph 87-88
574 C-Me NHCH(CH2-iPr)CH2OMe 2,4-Cl
2The amorphous 575 C-Me NH-2-butyl 2 of-Ph, 4-Me2-Ph grease 576 C-Me NH-2-amyl groups 2,4-Me2-Ph grease 577 C-Me NH-2-hexyls 2,4-Me2-Ph grease 578 C-Me NHCH (i-Pr) Me 2,4-Me2-Ph grease 579 C-Me NHCH (Me) CH2-iPr 2,4-Me2-Ph grease 580 C-Me NHCH (Me)-c-C6H11 2,4-Me2-Ph grease 581 C-Me NH-2-(2,3-indanyl) 2,4-Me2-Ph grease 582 C-Me NH-1-(2,3-indanyl) 2,4-Me2-Ph grease 583 C-Me NHCH (Me) Ph 2,4-Me2-Ph grease 584 C-Me NHCH (Me) CH2-(4-ClPh) 2,4-Me
2-Ph grease 585 C-Me NHCH (Me) CH2COCH
3 2,4-Me
2-Ph grease 586 C-Me NHCH (Ph) CH2Ph 2,4-Me
2-Ph grease 587 C-Me NHCH (Me) (CH2)3NEt
2 2,4-Me
2-Ph grease 588 C-Me NH-(2-Ph-c-C3H
4) 2,4-Me
2-Ph grease 589 C-Me NHCH (Et) CH2CN 2,4-Me
2-Ph 119-120 590 C-Me NH-3-hexyls 2,4-Me2-Ph grease 591n C-Me NEt
22-MeO-4-ClPh grease 592o C-Me NHCH(Et)
22-MeO-4-ClPh grease 593p C-Me NHCH(Et)CH
2OMe 2-MeO-4-ClPh. grease 594 C-Me NMe22-MeO-4-ClPh grease 595q C-Me NHCH(Et)
22-OMe-4-MePh grease 596r C-Me NEt
22-OMe-4-MePh grease 597s C-c-Pr NHCH(CH
2OMe)
2 2,4-Cl
2-Ph grease 598 C-Me N (c-Pr) E 2,4-Me2-Ph
599 C-Me N(c-Pr)E 2,4-Cl
2-Ph
600 C-Me N(c-Pr)E 2,4,6-Me
3-Ph
601 C-Me N(c-Pr)Et 2-Me-4-Cl-Ph
602 C-Me N(c-Rr)Et 2-Cl-4-Me-Ph
603 C-Me NHCH(c-Pr)
2 2,4-Cl
2-Ph
604 C-Me NHCH(c-Pr)
2 2,4-Me
2-Ph
605 C-Me NHCH(c-Pr)
2 2-Me-4-Cl-Ph
606 C-Me NHCH(c-Pr)
2 2-Cl-4-Me-Ph
607 C-Me NHCH(c-Pr)
2 2-Me-4-OMe-Ph
608 C-Me NHCH(c-Pr)
2 2-Cl-4-OMe-Ph
609 C-Me NHCH(CH
2OMe)
2 2-Cl-5-F-OMePh
610 C-Me NEt
2 2-Cl-5-F-OMePh
611 C-Me N(c-Pr)CH
2CH
2CN 2-Cl-5-F-OMePh
612 C-Me NHCH(Et)
2 2-Cl-5-F-OMePh
613 C-Me N(CH
2CH
2OMe)
2 2-Cl-5-F-OMePh
614 C-Me NEt
2 2,6-Me
2-pyridin-3-yl 615 C-Me N (c-Pr) CH2CH
2CN 2,6-Me
2-pyridin-3-yl 616 C-Me NHCH (Et)2 2,6-Me
2-pyridin-3-yl 617 C-Me N (CH2CH
2OMe)
2 2,6-Me
2-pyridin-3-yl 618 C-OH NHCH (CH2OMe)
2 2,4-Me
2-Ph
619 C-OH NEt
2 2,4-Me
2-Ph
620 C-OH N(c-Pr)CH
2CH
2CN 2,4-Me
2-Ph
621 C-OH NHCH(Et)
2 2,4-Me
2-Ph
623 C-OH N(CH
2CH
2OMe)
2 2,4-Me
2-Ph
624 C-NEt
2 NHCH(CH
2OMe)
2 2,4-Me
2-Ph
625 C-NEt
2 NEt
2 2,4-Me
2-Ph
626 C-NEt
2 N(c-Pr)CH
2CH
2CN 2,4-Me
2-Ph
627 C-NEt
2 NHCH(Et)
2 2,4-Me
2-Ph
628 C-NEt
2 N(CH
2CH
2OMe)
2 2,4-Me
2-Ph
629 C-Me NHCH(Et)
2 2-Me-4-CN-Ph
630 C-Me N(CH
2CH
2OMe)
2 2-Me-4-CN-Ph
Table 3 note: a) CI-HRMS: calculated value: 367.2610, measured value: 367.2607 (M+H); B) CI-HRMS: calculated value: 384.2400, measured value: 384.2393 (M-H); C) CI-HRMS: calculated value: 404.1853, measured value: 404.1844 (M+H); D) CI-HRMS: calculated value: 381.1594, measured value: 381.1596 (M+H);
Analytical calculation value: C:63.07, H, 5.57, N, 22.07, Cl,
9.32;
Measured value: C:63.40, H, 5.55, N, 21.96, Cl:9.15e) CI-HRMS: calculated value: 369.1594, measured value: 369.1576 (M+H); F) CI-HRMS: calculated value: 354.2216, measured value: 354.2211 (M+H); G) CI-HRMS: calculated value: 410.1072, measured value: 410.1075 (M+H); H) CI-HRMS: calculated value: 414.2427, measured value: 414.2427 (M+H); I) CI-HRMS: calculated value: 368.2372, measured value: 368.2372 (M+H); J) CI-HRMS: calculated value: 384.1955, measured value: 384.1947 (M+H); K) CI-HRMS: calculated value: 391.2168, measured value: 391.2160 (M+H); L) CI-HRMS: calculated value: 335.1984, measured value: 335.1961 (M+H); M) CI-HRMS: calculated value: 382.0759, measured value: 382.0765 (M+H); N) NH
3-CI MS: calculated value: 360, measured value: 360 (M+H)+o) NH
3-CI MS: calculated value: 374, measured value: 374 (M+H)+;
NMR(CDCl
3,300MHz):δ7.29(d,J=8.4Hz,1H),7.04
(dd,J=1.8,8Hz,1H),6.96(d,J=1.8Hz,1H),6.15
(d,J=10,1H),4.19(m,1H),3.81(s,3H),2.47(s,
3H),2.32(s,3H),1.65(m,4H),0.99(t,J=7.32Hz,
6H) p) NH
3-CI MS: calculated value: 390, measured value: 390 (M+H)-;
NMR(CDCl
3,300MHz):δ7.28(d,J=8Hz,1H),7.03
(d,J=8Hz,1H),6.96(s,H),6.52(d,J=9Hz,1H),
4.36(m,1H),3.8(s,3H),3.55(m,2H),3.39(s,
3H),2.47(s,3H),2.32(s,3H),1.76(m,2H),1.01
(t, J=7.32Hz, 3H) .q) CI-HRMS: calculated value: 354.2294, measured value: 354.2279 (M+H)+r) CI-HRMS: calculated value: 340.2137, measured value: 340.2138 (M+H)+s) CI-HRMS: calculated value: 436.1307, measured value: 436.1296 (M+H)+
According to embodiment 1A, 1B, 432,433,434 described methods, can prepare the compound of the described embodiment of table 4.Commonly used is abbreviated as: Ph is a phenyl, and Pr is a propyl group, and Me is a methyl, and Et is an ethyl, and Bu is a butyl, and Ex is embodiment, and EtOAc is an ethyl acetate.
Table 4
Ex Z R3 Ar Mp (℃)631 C-Me NHCH (Et)
22-Br-4,5-(MeO)
2Ph 160-161632 C-Me NHCH (Et)
22-Br-4-MeOPh 110-111633 C-Me N (CH
2CH
2OMe)
22-Br-4-MeOPh 74-76634 C-Me NHCH (CH
2OMe)
22-Br-4-MeOPh 128-130635 C-Me N (Et)
22-Me-4-ClPh 113-114636 C-Me N (c-Pr) Et 2,4-Cl
2Ph637 C-Me N (c-Pr) Et 2,4-Me
2Ph638 C-Me N (c-Pr) Et 2,4,6-Me
3Ph639 C-Me N (c-Pr) Et 2-Me-4-MeOPh640 C-Me N (c-Pr) Et 2-Cl-4-MeOPh641 C-Me N (c-Pr) Et 2-Cl-4-MePh642 C-Me N (c-Pr) Et 2-Me-4-ClPh643 C-Me NHCH (c-Pr)
22,4-Cl
2-Ph644 C-Me NHCH (c-Pr)
22,4-Me
2-Ph645 C-Me NHCH (c-Pr)
22-Me-4-Cl-Ph646 C-Me NHCH (c-Pr)
22-Cl-4-Me-Ph647 C-Me NHCH (c-Pr)
22-Me-4-OMe-Ph648 C-Me NHCH (c-Pr)
22-Cl-4-OMe-Ph649 C-Me NHCH (CH
2OMe)
22-Cl-5-F-OMePh650 C-Me NEt
22-Cl-5-F-OMePh651 C-Me N (c-Pr) CH
2CH
2CN 2-Cl-5-F-OMePh652 C-Me NHCH (Et)
22-Cl-5-F-OMePh653 C-Me N (CH
2CH
2OMe)
22-Cl-5-F-OMePh654 C-Me NEt
22,6-Me
2-pyridin-3-yl 655 C-Me N (c-Pr) CH
2CH
2CN 2,6-Me
2-pyridin-3-yl 656 C-Me NHCH (Et)
22,6-Me
2-pyridin-3-yl 657 C-Me N (CH
2CH
2OMe)
22,6-Me
2-pyridin-3-yl 658 C-OH NHCH (CH
2OMe)
22,4-Me
2-Ph659 C-OH NEt
22,4-Me
2-Ph660 C-OH N (c-Pr) CH
2CH
2CN 2,4-Me
2-Ph661 C-OH NHCH (Et)
22,4-Me
2-Ph662 C-OH N (CH
2CH
2OMe)
22,4-Me
2-Ph663 C-NEt2 NHCH (CH
2OMe)
22,4-Me
2-Ph664 C-NEt2 NEt
22,4-Me
2-Ph665 C-NEt2 N (c-Pr) CH
2CH
2CN 2,4-Me
2-Ph666 C-NEt2 NHCH (Et)
22,4-Me
2-Ph667 C-NEt2 N (CH
2CH
2OMe)
22,4-Me
2-Ph668 C-Me NHCH (Et)
22-Me-4-CN-Ph669 C-Me N (CH
2CH
2OMe)
22-Me-4-CN-Ph
According to embodiment 1A, 1B, 2,3,6,431,432,433,434 described methods or their appropriate combination, can prepare the compound of table 5 or 6 described embodiment.Commonly used is abbreviated as: Ph is a phenyl, and Pr is a propyl group, and Me is a methyl, and Et is an ethyl, and Bu is a butyl, and Ex is embodiment.
Table 5
Ex
R14
R3
Ar
670 Me NHCH(CH
2OMe)
2 2,4-Cl
2-Ph
671 Me NHCHPr
2 2,4-Cl
2-Ph
672 Me NEtBu 2,4-Cl
2-Ph
673 Me NPr(CH
2-c-C
3H
5) 2,4-Cl
2-Ph
674 Me N(CH
2CH
2OMe)
2 2,4-Cl
2-Ph 675 Me NH-3-heptyl 2,4-Cl2-Ph
676 Me NHCH(Et)CH
2OMe 2,4-Cl
2-Ph
677 Me NEt
2 2,4-Cl
2-Ph
678 Me NHCH(CH
2OEt)
2 2,4-Cl
2-Ph 679 Me NH-3-amyl groups 2,4-Cl2-Ph
680 Me NMePh 2,4-Cl
2-Ph
681 Me NPr
2 2,4-Cl
2-Ph 682 Me NH-3-hexyls 2,4-Cl2-Ph 683 Me morpholinoes 2,4-Cl2-Ph
684 Me N(CH
2Ph)CH
2CH
2OMe 2,4-Cl
2-Ph
685 Me NHCH(CH
2Ph)CH
2OMe 2,4-Cl
2-Ph 686 Me NH-4-THP trtrahydropyranyls 2,4-Cl2-Ph 687 Me NH-cyclopenta 2,4-Cl2-Ph
688 Me OEt 2,4-Cl
2-Ph
689 Me OCH(Et)CH
2OMe 2,4-Cl
2-Ph
690 Me OCH
2Ph 2,4-Cl
2-Ph 691 Me O-3-amyl groups 2,4-Cl2-Ph
692 Me SEt 2,4-Cl
2-Ph
693 Me S(O)Et 2,4-Cl
2-Ph
694 Me SO
2Et 2,4-Cl
2-Ph
695 Me Ph 2,4-Cl
2-Ph
696 Me 2-CF
3-Ph 2,4-Cl
2-Ph
697 Me 2-Ph-Ph 2,4-Cl
2-Ph 698 Me 3-amyl groups 2,4-Cl2-Ph 699 Me cyclobutyl 2,4-Cl2-Ph 700 Me 3-pyridine radicals 2,4-Cl2-Ph
701 Me CH(Et)CH
2CONMe
2 2,4-Cl
2-Ph
702 Me CH(Et)CH
2CH
2NMe
2 2,4-Cl
2-Ph
703 Me NHCH(CH
2OMe)
2 2,4,6-Me
3-Ph
704 Me MHCHPr
2 2,4,6-Me
3-Ph
705 Me NEtBu 2,4,6-Me
3-Ph
706 Me NPr(CH
2-c-C
3H
5) 2,4,6-Me
3-Ph
707 Me N(CH
2CH
2OMe)
2 2,4,6-Me
3-Ph 708 Me NH-3-heptyl 2,4,6-Me3-Ph
709 Me NHCH(Et)CH
2OMe 2,4,6-Me
3-Ph
710 Me NEt
2 2,4,6-Me
3-Ph
711 Me NHCH(CH
2OEt)
2 2,4,6-Me
3-Ph 712 Me NH-3-amyl groups 2,4,6-Me3-Ph
713 Me NMePh 2,4,6-Me
3-Ph
714 Me NPr
2 2,4,6-Me
3-Ph 715 Me NH-3-hexyls 2,4,6-Me3-Ph 716 Me morpholinoes 2,4,6-Me3-Ph
717 Me N(CH
2Ph)CH
2CH
2OMe 2,4,6-Me
3-Ph
718 Me NHCH(CH
2Ph)CH
2OMe 2,4,6-Me
3-Ph 719 Me NH-4-THP trtrahydropyranyls 2,4,6-Me3-Ph 720 Me NH-cyclopenta 2,4,6-Me3-Ph
721 Me OEt 2,4,6-Me
3-Ph
722 Me OCH(Et)CH
2OMe 2,4,6-Me
3-Ph
723 Me OCH
2Ph 2,4,6-Me
3-Ph 724 Me O-3-amyl groups 2,4,6-Me3-Ph
725 Me SEt 2,4,6-Me
3-Ph
726 Me S(O)Et 2,4,6-Me
3-Ph
727 Me SO
2Et 2,4,6-Me
3-Ph
728 Me CH(CO
2Et)
2 2,4,6-Me
3-Ph
729 Me C(Et)(CO
2Et)
2 2,4,6-Me
3-Ph
730 Me CH(Et)CH
2OH 2,4,6-Me
3-Ph
731 Me CH(Et)CH
2OMe 2,4,6-Me
3-Ph
732 Me CONMe
2 2,4,6-Me
3-Ph
733 Me COCH
3 2,4,6-Me
3-Ph
734 Me CH(OH)CH
3 2,4,6-Me
3-Ph 735 Me C (OH) Ph-3-pyridine radicals 2,4,6-Me3-Ph
736 Me Ph 2,4,6-Me
3-Ph
737 Me 2-Ph-Ph 2,4,6-Me
3-Ph 738 Me 3-amyl groups 2,4,6-Me3-Ph 739 Me cyclobutyl 2,4,6-Me3-Ph 740 Me 3-pyridine radicals 2,4,6-Me3-Ph
741 Me CH(Et)CH
2CONMe
2 2,4,6-Me
3-Ph
742 Me CH(E-)CH
2CH
2NMe
2 2,4,6-Me
3-Ph
743 Me NHCH(CH
2OMe)
2 2,4-Me
2-Ph
744 Me N(CH
2CH
2OMe)
2 2,4-Me
2-Ph
745 Me NHCH(Et)CH
2OMe 2,4-Me
2-Ph 746 Me NH-3-amyl groups 2,4-Me2-Ph
747 Me NEt
2 2,4-Me
2-Ph
748 Me N(CH
2CN)
2 2,4-Me
2-Ph
749 Me NHCH(Me)CH
2OMe 2,4-Me
2-Ph
750 Me OCH(Et)CH
2OMe 2,4-Me
2-Ph
751 Me NPr-c-C
3H
5 2,4-Me
2-Ph
752 Me NHCH(Me)CH
2NMe
2 2,4-Me
2-Ph
753 Me N(c-C
3H
5)CH
2CH
2CN 2,4-Me
2-Ph
754 Me N(Pr)CH
2CH
2CN 2,4-Me
2-Ph
755 Me N(Bu)CH
2CH
2CN 2,4-Me
2-Ph
756 Me NHCHPr
2 2,4-Me
2-Ph
757 Me NEtBu 2,4-Me
2-Ph
758 Me NPr(CH
2-c-C
3H
5) 2,4-Me
2-Ph 759 Me NH-3-heptyl 2,4-Me2-Ph
760 Me NEt
2 2,4-Me
2-Ph
761 Me NHCH(CH
2OEt)
2 2,4-Me
2-Ph 762 Me NH-3-amyl groups 2,4-Me2-Ph
763 Me NMePh 2,4-Me
2-Ph
764 Me NPr
2 2,4-Me
2-Ph 765 Me NH-3-hexyls 2,4-Me2-Ph 766 Me morpholinoes 2,4-Me2-Ph
767 Me N(CH
2Ph)CH
2CH
2OMe 2,4-Me
2-Ph
768 Me NHCH(CH
2Ph)CH
2OMe 2,4-Me
2-Ph 769 Me NH-4-THP trtrahydropyranyls 2,4-Me2-Ph 770 Me NH-cyclopenta 2,4-Me2-Ph
771 Me NHCH(CH
2OMe)
2 2-Me-4-MeO-Ph
772 Me N(CH
2CH
2OMe)
2 2-Me-4-MeO-Ph
773 Me NHCH(Et)CH
2OMe 2-Me-4-MeO-Ph
774 Me N(Pr)CH
2CH
2CN 2-Me-4-MeO-Ph
775 Me OCH(Et)CH
2OMe 2-Me-4-MeO-Ph
776 Me NHCH(CH
2OMe)
2 2-Br-4-MeO-Ph
777 Me N(CH
2CH
2OMe)
2 2-Br-4-MeO-Ph
778 Me NHCH(Et)CH
2OMe 2-Br-4-MeO-Ph
779 Me N(Pr)CH
2CH
2CN 2-Br-4-MeO-Ph
780 Me OCH(Et)CH
2OMe 2-Br-4-MeO-Ph
781 Me NHCH(CH
2OMe)
2 2-Me-4-NMe
2-Ph
782 Me N(CH
2CH
2OMe)
2 2-Me-4-NMe
2-Ph
783 Me NHCH(Et)CH
2OMe 2-Me-4-NMe
2-Ph
784 Me N(Pr)CH
2CH
2CN 2-Me-4-NMe
2-Ph
785 Me OCH(Et)CH
2OMe 2-Me-4-Me
2-Ph
786 Me NHCH(CH
2OMe)
2 2-Br-4-NMe
2-Ph
787 Me N(CH
2CH
2OMe)
2 2-Br-4-NMe
2-Ph
788 Me NHCH(Et)CH
2OMe 2-Br-4-NMe
2-Ph
789 Me N(Pr)CH
2CH
2CN 2-Br-4-NMe
2-Ph
790 Me OCH(Et)CH
2OMe 2-Br-4-NMe
2-Ph
791 Me NHCH(CH
2OMe)
2 2-Br-4-i-Pr-Ph
792 Me N(CH
2CH
2OMe)
2 2-Br-4-i-Pr-Ph
793 Me NHCH(Et)CH
2OMe 2-Br-4-i-Pr-Ph
794 Me N(Pr)CH
2CH
2CN 2-Br-4-i-Pr-Ph
795 Me OCH(Et)CH
2OMe 2-Br-4-i-Pr-Ph
796 Me NHCH(CH
2OMe)
2 2-Br-4-Me-Ph
797 Me N(CH
2CH
2OMe)
2 2-Br-4-Me-Ph
798 Me NHCH(Et)CH
2OMe 2-Br-4-Me-Ph
799 Me N(Pr)CH
2CH
2CN 2-Br-4-Me-Ph
800 Me OCH(Et)CH
2OMe 2-Br-4-Me-Ph
801 Me NHCH(CH
2OMe)
2 2-Me-4-Br-Ph
802 Me N(CH
2CH
2OMe)
2 2-Me-4-Br-Ph
803 Me NHCH(Et)CH
2OMe 2-Me-4-Br-Ph
804 Me N(Pr)CH
2CH
2CN 2-Me-4-Br-Ph
805 Me OCH(Et)CH
2OMe 2-Me-4-Br-Ph
806 Me NHCH(CH
2OMe)
2 2-Cl-4,6-Me
2-Ph
807 Me N(CH
2CH
2OMe)
2 2-Cl-4,6-Me
2-Ph
808 Me NHCH(CH
2OMe)
2 4-Br-2,6-(Me)
2-Ph
809 Me N(CH
2CH
2OMe)
2 4-Br-2,6-(Me)
2-Ph
810 Me NHCH(CH
2OMe)
2 4-i-Pr-2-SMe-Ph
811 Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SMe-Ph
812 Me NHCH(CH
2OMe)
2 2-Br-4-CF
3-Ph
813 Me N(CH
2CH
2OMe)
2 2-Br-4-CF
3-Ph
814 Me NHCH(CH
2OMe)
2 2-Br-4,6-(MeO)
2-Ph
815 Me N(CH
2CH
2OMe)
2 2-Br-4,6-(MeO)
2-Ph
816 Me NHCH(CH
2OMe)
2 2-Cl-4,6-(MeO)
2-Ph
817 Me N(CH
2CH
2OMe)
2 2-Cl-4,6-(MeO)
2-Ph
818 Me NHCH(CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
819 Me N(CH
2CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
820 Me NHCH(CH
2OMe)
2 4-(COMe)-2-Br-Ph
821 Me N(CH
2CH
2OMe)
2 4-(COMe)-2-Br-Ph
822 Me NHCH(CH
2OMe)
2 2,4,6-Me
3-pyridin-3-yl 823 Me N (CH2CH
2OMe)
2 2,4,6-Me
3-pyridin-3-yl 824 Me NHCH (CH2OMe)
2 2,4-(Br)
2-Ph
825 Me N(CH
2CH
2OMe)
2 2,4-(Br)
2-Ph
826 Me NHCH(CH
2OMe)
2 4-i-Pr-2-SMe-Ph
827 Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SMe-Ph
828 Me NHCH(CH
2OMe)
2 4-i-Pr-2-SO
2Me-Ph
829 Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SO
2Me-Ph
830 Me NHCH(CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
831 Me N(CH
2CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
832 Me NHCH(CH
2OMe)
2 2,6-(Me)2-4-SO
2Me-Ph
833 Me N(CH
2CH
2OMe)
2 2,6-(Me)2-4-SO
2Me-Ph
834 Me NHCH(CH
2OMe)
2 2-I-4-i-Pr-Ph
835 Me N(CH
2CH
2OMe)
2 2-I-4-i-Pr-Ph
836 Me NHCH(CH
2OMe)
2 2-Br-4-N(Me)
2-6-MeO-Ph
837 Me N(CH
2CH
2OMe)
2 2-Br-4-N(Me)
2-6-MeO-Ph
838 Me NEt
22-Br-4-MeO-Ph 839 Me NH-3-amyl group 2-Br-4-MeO-Ph 840 Me NHCH (CH2OMe)
2 2-CN-4-Me-Ph
841 Me N(c-C
3H
5)CH
2CH
2CN 2,4,6-Me
3-Ph
842 Me NHCH(CH
2CH
2OMe)CH
2OMe 2-Me-4-Br-Ph
843 Me NHCH(CH
2OMe)
2 2,5-Me
2-4-MeO-Ph
844 Me N(CH
2CH
2OMe)
2 2,5-Me
2-4-MeO-Ph 845 Me NH-3-amyl groups 2,5-Me2-4-MeO-Ph
846 Me NEt
2 2,5-Me
2-4-MeO-Ph
847 Me NHCH(CH
2OMe)
2 2-Cl-4-MePh
848 Me NCH(Et)CH
2OMe 2-Cl-4-MePh
849 Me N(CH
2CH
2OMe)
2 2-Cl-4-MePh
850 Me (S)-NHCH
4(CH
2CH
2OMe)CH
2OMe 2-Cl-4-MePh
851 Me N(c-C
3H
5)CH
2CH
2CN 2,5-Me
2-4-MeOPh
852 Me NEt
2 2-Me-4-MeOPh
853 Me OEt 2-Me-4-MeOPh
854 Me (S)-NHCH(CH
2CH
2OMe)CH
2OMe 2-Me-4-MeOPh
855 Me N(c-C
3H
5)CH
2CH
2CN 2-Me-4-MeOPh
856 Me NHCH(CH
2CH
2OEt)
2 2-Me-4-MeOPh
857 Me N(c-C
3H
5)CH
2CH
2CN 2,4-Cl
2-Ph
858 Me NEt
22-Me-4-ClPh 859 Me NH-3-amyl group 2-Me-4-ClPh 860 Me N (CH2CH
2OMe)
2 2-Me-4-ClPh
861 Me NHCH(CH
2OMe)
2 2-Me-4-ClPh
862 Me NEt
2 2-Me-4-ClPh
863 Me NEt
22-Cl-4-MePh 864 Me NH-3-amyl group 2-Cl-4-MePh 865 Me NHCH (CH2OMe)
2 2-Cl-4-MeOPh
866 Me N(CH
2CH
2OMe)
2 2-Cl-4-MeOPh
867 Me NHCH(Et)CH
2OMe 2-Cl-4-MeOPh
868 Me N(c-Pr)CH
2CH
2CN 2-Cl-4-MeOPh
869 Me NEt
22-Cl-4-MeOPh 870 Me NH-3-amyl group 2-Cl-4-MeOPh 871 Me NHCH (Et) CH2CH
2OMe 2-Cl-4-MeOPh
872 Me NHCH(Me)CH
2CH
2OMe 2-Cl-4-MeOPh
873 Me NHCH(Et)CH
2CH
2OMe 2-Br-4-MeOPh
874 Me NHCH(Me)CH
2CH
2OMe 2-Br-4-MeOPh
875 Me NHCH(Et)CH
2CH
2OMe 2-Me-4-MeOPh
876 Me NHCH(Me)CH
2CH
2OMe 2-Me-4-MeOPh
877 Me NHCH(CH
2OMe)
2 2-Cl-4,5-(MeO)
2Ph
878 Me N(CH
2CH
2OMe)
2 2-Cl-4,5-(MeO)
2Ph
879 Me NHCH(Et)CH
2OMe 2-Cl-4,5-(MeO)
2Ph
880 Me N(c-Pr)CH
2CH
2CN 2-Cl-4,5-(MeO)
2Ph
881 Me NEt
2 2-Cl-4,5-(MeO)
2Ph 882 Me NH-3-amyl group 2-Cl-4,5-(MeO)2Ph
883 Me NHCH(Et)CH
2CH
2OMe 2-Cl-4,5-(MeO)
2Ph
884 Me NHCH(Me)CH
2CH
2OMe 2-Cl-4,5-(MeO)
2Ph
885 Me NHCH(CH
2OMe)
2 2-Br-4,5-(MeO)
2Ph
886 Me N(CH
2CH
2OMe)
2 2-Br-4,5-(MeO)
2Ph
887 Me NHCH(Et)CH
2OMe 2-Br-4,5-(MeO)
2Ph
888 Me N(c-Pr)CH
2CH
2CN 2-Br-4,5-(MeO)
2Ph
889 Me NEt
2 2-Br-4,5-(MeO)
2Ph 890 Me NH-3-amyl group 2-Br-4,5-(MeO)2Ph
891 Me NHCH(CH
2OMe)
2 2-Cl-4,6-(MeO)
2Ph
892 Me N(CH
2CH
2OMe)
2 2-Cl-4,6-(MeO)
2Ph
893 Me NEt
2 2-Cl-4,6-(MeO)
2Ph 894 Me NH-3-amyl group 2-Cl-4,6-(MeO)2Ph
895 Me NHCH(CH
2OMe)
2 2-Me-4,6-(MeO)
2Ph
896 Me N(CH
2CH
2OMe)
2 2-Me-4,6-(MeO)
2Ph
897 Me NHCH(Et)CH
2OMe 2-Me-4,6-(MeO)
2Ph
898 Me NEt
2 2-Me-4,6-(MeO)
2Ph 899 Me NH-3-amyl group 2-Me-4,6-(MeO)2Ph
900 Me NHCH(Et)CH
2CH
2OMe 2-Me-4-MeOPh
901 Me NHCH(Me)CH
2CH
2OMe 2-Me-4-MeOPh
902 Me NHCH(CH
2OMe)
2 2-Me0-4-MePh
903 Me N(CH
2CH
2OMe)
2 2-Me0-4-MePh
904 Me NHCH(Et)CH
2OMe 2-Me0-4-MePh
905 Me N(c-Pr)CH
2CH
2CN 2-Me0-4-MePh
906 Me NEt
22-Me0-4-MePh 907 Me NH-3-amyl group 2-Me0-4-MePh 908 Me NHCH (Et) CH2CH
2OMe 2-Me0-4-MePh
909 Me NHCH(Me)CH
2CH
2OMe 2-Me0-4-MePh
910 Me NHCH(CH
2OMe)
2 2-Me0-4-MePh
911 Me N(CH
2CH
2OMe)
2 2-Me0-4-MePh
912 Me NHCH(Et)CH
2OMe 2-Me0-4-MePh
913 Me N(c-Pr)CH
2CH
2CN 2-Me0-4-MePh
914 Me NEt
22-Me0-4-MePh 915 Me NH-3-amyl group 2-Me0-4-MePh 916 Me NHCH (CH2OMe)
2 2-Me0-4-ClPh
917 Me N(CH
2CM
2OMe)
2 2-Me0-4-ClPh
918 Me NHCH(Et)CH
2OMe 2-Me0-4-ClPh
919 Me NEt
22-Me0-4-ClPh 920 Me NH-3-amyl group 2-Me0-4-ClPh
Table 6 Ex
R14
R3
Ar
921 Me NHCH(CH
2OMe)
2 2,4-Cl
2-Ph
922 Me NHCHPr
2 2,4-Cl
2-Ph
923 Me NEtBu 2,4-Cl
2-Ph
924 Me NPr(CH
2-c-C
3H
5) 2,4-Cl
2-Ph
925 Me N(CH
2CH
2OMe)
2 2,4-Cl
2-Ph 926 Me NH-3-heptyl 2,4-Cl2-Ph
927 Me NHCH(Et)CH
2OMe 2,4-Cl
2-Ph
928 Me NEt
2 2,4-Cl
2-Ph
929 Me NHCH(CH
2OEt)
2 2,4-Cl
2-Ph 930 Me NH-3-amyl groups 2,4-Cl2-Ph
931 Me NMePh 2,4-Cl
2-Ph
932 Me NPr
2 2,4-Cl
2-Ph 933 Me NH-3-hexyls 2,4-Cl2-Ph 934 Me morpholinoes 2,4-Cl2-Ph
935 Me N(CH
2Ph)CH
2CH
2OMe 2,4-Cl
2-Ph
936 Me NHCH(CH
2Ph)CH
2OMe 2,4-Cl
2-Ph 937 Me NH-4-THP trtrahydropyranyls 2,4-Cl2-Ph 938 Me NH-cyclopenta 2,4-Cl2-Ph
939 Me OEt 2,4-Cl
2-Ph
940 Me OCH(Et)CH
2OMe 2,4-Cl
2-Ph
941 Me OCH
2Ph 2,4-Cl
2-Ph 942 Me O-3-amyl groups 2,4-Cl2-Ph
943 Me SEt 2,4-Cl
2-Ph
944 Me S(O)Et 2,4-Cl
2-Ph
945 Me SO
2Et 2,4-Cl
2-Ph
946 Me Ph 2,4-Cl
2-Ph
947 Me 2-CF
3-Ph 2,4-Cl
2-Ph
948 Me 2-Ph-Ph 2,4-Cl
2-Ph
949 Me 3-pentyl 2,4-Cl
2-Ph 950 Me cyclobutyl 2,4-Cl2-Ph 951 Me 3-pyridine radicals 2,4-Cl2-Ph
952 Me CH(Et)CH
2CONMe
2 2,4-Cl
2-Ph
953 Me CH(Et)CH
2CH
2NMe
2 2,4-Cl
2-Ph
954 Me NHCH(CH
2OMe)
2 2,4,6-Me
3-Ph
955 Me NHCHPr
2 2,4,6-Me
3-Ph
956 Me NEtBu 2,4,6-Me
3-Ph
957 Me NPr(CH
2-c-C
3H
5) 2,4,6-Me
3-Ph
958 Me N(CH
2CH
2OMe)
2 2,4,6-Me
3-Ph 959 Me NH-3-heptyl 2,4,6-Me3-Ph
960 Me NHCH(Et)CH
2OMe 2,4,6-Me
3-Ph
961 Me NEt
2 2,4,6-Me
3-Ph
962 Me NHCH(CH
2OEt)
2 2,4,6-Me
3-Ph 963 Me NH-3-amyl groups 2,4,6-Me3-Ph
964 Me NMePh 2,4,6-Me
3-Ph
965 Me NPr
2 2,4,6-Me
3-Ph 966 Me NH-3-hexyls 2,4,6-Me3-Ph 967 Me morpholinoes 2,4,6-Me3-Ph
968 Me N(CH
2Ph)CH
2CH
2OMe 2,4,6-Me
3-Ph
969 Me NHCH(CH
2Ph)CH
2OMe 2,4,6-Me
3-Ph 970 Me NH-4-THP trtrahydropyranyls 2,4,6-Me3-Ph 971 Me NH-cyclopenta 2,4,6-Me3-Ph
972 Me OEt 2,4,6-Me
3-Ph
973 Me OCH(Et)CH
2OMe 2,4,6-Me
3-Ph
974 Me OCH
2Ph 2,4,6-Me
3-Ph 975 Me O-3-amyl groups 2,4,6-Me3-Ph
976 Me SEt 2,4,6-Me
3-Ph
977 Me S(O)Et 2,4,6-Me
3-Ph
978 Me SO
2Et 2,4,6-Me
3-Ph
979 Me CH(CO
2Et)
2 2,4,6-Me
3-Ph
980 Me C(Et)(CO
2Et)
2 2,4,6-Me
3-Ph
981 Me CH(Et)CH
2OH 2,4,6-Me
3-Ph
982 Me CH(Et)CH
2OMe 2,4,6-Me
3-Ph
983 Me CONMe
2 2,4,6-Me
3-Ph
984 Me COCH
3 2,4,6-Me
3-Ph
985 Me CH(OH)CH
3 2,4,6-Me
3-Ph 986 Me C (OH) Ph-3-pyridine radicals 2,4,6-Me3-Ph
987 Me Ph 2,4,6-Me
3-Ph
988 Me 2-Ph-Ph 2,4,6-Me
3-Ph 989 Me 3-amyl groups 2,4,6-Me3-Ph 990 Me cyclobutyl 2,4,6-Me3-Ph 991 Me 3-pyridine radicals 2,4,6-Me3-Ph
992 Me CH(Et)CH
2CONMe
2 2,4,6-Me
3-Ph
993 Me CH(Et)CH
2CH
2NMe
2 2,4,6-Me
3-Ph
994 Me NHCH(CH
2OMe)
2 2,4-Me
2-Ph
995 Me N(CH
2CH
2OMe)
2 2,4-Me
2-Ph
996 Me NHCH(Et)CH
2OMe 2,4-Me
2-Ph 997 Me NH-3-amyl groups 2,4-Me2-Ph
998 Me NEt
2 2,4-Me
2-Ph
999 Me N(CH
2CN)
2 2,4-Me
2-Ph
1000 Me NHCH(Me)CH
2OMe 2,4-Me
2-Ph
1001 Me OCH(Et)CH
2OMe 2,4-Me
2-Ph
1002 Me NPr-c-C
3H
5 2,4-Me
2-Ph
1003 Me NHCH(Me)CH
2NMe
2 2,4-Me
2-Ph
1004 Me N(c-C
3H
5)CH
2CH
2CN 2,4-Me
2-Ph
1005 Me N(Pr)CH
2CH
2CN 2,4-Me
2-Ph
1006 Me N(Bu)CH
2CH
2CN 2,4-Me
2-Ph
1007 Me NHCHPr
2 2,4-Me
2-Ph
1008 Me NEtBu 2,4-Me
2-Ph
1009 Me NPr(CH
2-c-C
3H
5) 2,4-Me
2-Ph 1010 Me NH-3-heptyl 2,4-Me2-Ph
1011 Me NEt
2 2,4-Me
2-Ph
1012 Me NHCH(CH
2OEt)
2 2,4-Me
2-Ph 1013 Me NH-3-amyl groups 2,4-Me2-Ph
1014 Me NMePh 2,4-Me
2-Ph
1015 Me NPr
2 2,4-Me
2-Ph
1016 Me NH-3-hexyl 2,4-Me
2-Ph
1017 Me morpholino 2,4-Me
2-Ph
1018 Me N(CH
2Ph)CH
2CH
2OMe 2,4-Me
2-Ph
1019 Me NHCH(CH
2Ph)CH
2OMe 2,4-Me
2-Ph 1020 Me NH-4-THP trtrahydropyranyls 2,4-Me2-Ph 1021 Me NH-cyclopenta 2,4-Me2-Ph
1022 Me NHCH(CH
2OMe)
2 2-Me-4-MeO-Ph
1023 Me N(CH
2CH
2OMe)
2 2-Me-4-MeO-Ph
1024 Me NHCH(Et)CH
2OMe 2-Me-4-MeO-Ph
1025 Me N(Pr)CH
2CH
2CN 2-Me-4-MeO-Ph
1026 Me OCH(Et)CH
2OMe 2-Me-4-MeO-Ph
1027 Me NHCH(CH
2OMe)
2 2-Br-4-MeO-Ph
1028 Me N(CH
2CH
2OMe)
2 2-Br-4-MeO-Ph
1029 Me NHCH(Et)CH
2OMe 2-Br-4-MeO-Ph
1030 Me N(Pr)CH
2CH
2CN 2-Br-4-MeO-Ph
1031 Me OCH(Et)CH
2OMe 2-Br-4-MeO-Ph
1032 Me NHCH(CH
2OMe)
2 2-Me-4-NMe
2-Ph
1033 Me N(CH
2CH
2OMe)
2 2-Me-4-NMe
2-Ph
1034 Me NHCH(Et)CH
2OMe 2-Me-4-NMe
2-Ph
1035 Me N(Pr)CH
2CH
2CN 2-Me-4-NMe
2-Ph
1036 Me OCH(Et)CH
2OMe 2-Me-4-NMe
2-Ph
1037 Me NHCH(CH
2OMe)
2 2-Br-4-NMe
2-Ph
1038 Me N(CH
2CH
2OMe)
2 2-Br-4-NMe
2-Ph
1039 Me NHCH(Et)CH
2OMe 2-Br-4-NMe
2-Ph
1040 Me N(Pr)CH
2CH
2CN 2-Br-4-NMe
2-Ph
1041 Me OCH(Et)CH
2OMe 2-Br-4-NMe
2-Ph
1042 Me NHCH(CH
2OMe)
2 2-Br-4-i-Pr-Ph
1043 Me N(CH
2CH
2OMe)
2 2-Br-4-i-Pr-Ph
1044 Me NHCH(Et)CH
2OMe 2-Br-4-i-Pr-Ph
1045 Me N(Pr)CH
2CH
2CN 2-Br-4-i-Pr-Ph
1046 Me OCH(Et)CH
2OMe 2-Br-4-i-Pr-Ph
1047 Me NHCH(CH
2OMe)
2 2-Br-4-Me-Ph
1048 Me N(CH
2CH
2OMe)
2 2-Br-4-Me-Ph
1049 Me NHCH(Et)CH
2OMe 2-Br-4-Me-Ph
1050 Me N(Pr)CH
2CH
2CN 2-Br-4-Me-Ph
1051 Me OCH(Et)CH
2OMe 2-Br-4-Me-Ph
1052 Me NHCH(CH
2OMe)
2 2-Me-4-Br-Ph
1053 Me N(CH
2CH
2OMe)
2 2-Me-4-Br-Ph
1054 Me NHCH(Et)CH
2OMe 2-Me-4-Br-Ph
1055 Me N(Pr)CH
2CH
2CN 2-Me-4-Br-Ph
1056 Me OCH(Et)CH
2OMe 2-Me-4-Br-Ph
1057 Me NCH(CH
2OMe)
2 2-Cl-4,6-Me
2-Ph
1058 Me N(CH
2CH
2OMe)
2 2-Cl-4,6-Me
2-Ph
1059 Me NHCH(CH
2OMe)
2 4-Br-2,6-(Me)
2-Ph
1060 Me N(CH
2CH
2OMe)
2 4-Br-2,6-(Me)
2-Ph
1061 Me NHCH(CH
2OMe)
2 4-i-Pr-2-SMe-Ph
1062 Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SMe-Ph
1063 Me NHCH(CH
2OMe)
2 2-Br-4-CF
3-Ph
1064 Me N(CH
2CH
2OMe)
2 2-Br-4-CF
3-Ph
1065 Me NHCH(CH
2OMe)
2 2-Br-4,6-(MeO)
2-Ph
1066 Me N(CH
2CH
2OMe)
2 2-Br-4,6-(MeO)
2-Ph
1067 Me NHCH(CH
2OMe)
2 2-Cl-4,6-(MeO)
2-Ph
1068 Me N(CH
2CH
2OMe)
2 2-Cl-4,6-(MeO)
2-Ph
1069 Me NHCH(CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
1070 Me N(CH
2CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
1071 Me NHCH(CH
2OMe)
2 4-(COMe)-2-Br-Ph
1072 Me N(CH
2CH
2OMe)
2 4-(COMe)-2-Br-Ph
1073 Me NHCH(CH
2OMe)
2 2,4,6-Me
3-pyridin-3-yl 1074 Me N (CH2CH
2OMe)
2 2,4,6-Me
3-pyridin-3-yl 1075 Me NHCH (CH2OMe)
2 2,4-(Br)
2-Ph
1076 Me N(CH
2CH
2OMe)
2 2,4-(Br)
2-Ph
1077 Me NHCH(CH
2OMe)
2 4-i-Pr-2-SMe-Ph
1078 Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SMe-Ph
1079 Me NHCH(CH
2OMe)
2 4-i-Pr-2-SO
2Me-Ph
1080 Me N(CH
2CH
2OMe)
2 4-i-Pr-2-SO
2Me-Ph
1081 Me NHCH(CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
1082 Me N(CH
2CH
2OMe)
2 2,6-(Me)
2-4-SMe-Ph
1083 Me NHCH(CH
2OMe)
2 2,6-(Me)2-4-SO
2Me-Ph
1084 Me N(CH
2CH
2OMe)
2 2,6-(Me)2-4-SO
2Me-Ph
1085 Me NHCH(CH
2OMe)
2 2-I-4-i-Pr-Ph
1086 Me N(CH
2CH
2OMe)
2 2-I-4-i-Pr-Ph
1087 Me NHCH(CH
2OMe)
2 2-Br-4-N(Me)
2-6-MeO-Ph
1088 Me N(CH
2CH
2OMe)
2 2-Br-4-N(Me)
2-6-MeO-Ph
1089 Me NEt
22-Br-4-MeO-Ph 1090 Me NH-3-amyl group 2-Br-4-MeO-Ph 1091 Me NHCH (CH2OMe)
2 2-CN-4-Me-Ph
1092 Me N(c-C
3H
5)CH
2CH
2CN 2,4,6-Me
3-Ph
1093 Me NHCH(CH
2CH
2OMe)CH
2OMe 2-Me-4-Br-Ph
1094 Me NHCH(CH
2OMe)
2 2,5-Me
2-4-MeO-Ph
1095 Me N(CH
2CH
2OMe)
2 2,5-Me
2-4-MeO-Ph 1096 Me NH-3-amyl groups 2,5-Me2-4-MeO-Ph
1097 Me NEt
2 2,5-Me
2-4-MeO-Ph
1098 Me NHCH(CH
2OMe)
2 2-Cl-4-MePh
1099 Me NCH(Et)CH
2OMe 2-Cl-4-MePh
1100 Me N(CH
2CH
2OMe)
2 2-Cl-4-MePh
1101 Me (S)-NHCH(CH
2CH
2OMe)CH
2OMe 2-Cl-4-MePh
1102 Me N(c-C
3H
5)CH
2CH
2CN 2,5-Me2-4-MeOPh
1103 Me NEt
2 2-Me-4-MeOPh
1104 Me OEt 2-Me-4-MeOPh
1105 Me (S)-NHCH(CH
2CH
2OMe)CH
2OMe 2-Me-4-MeOPh
1106 Me N(c-C
3H
5)CH
2CH
2CN 2-Me-4-MeOPh
1107 Me NHCH(CH
2CH
2OEt)
2 2-Me-4-MeOPh
1108 Me N(c-C
3H
5)CH
2CH
2CN 2,4-Cl
2-Ph
1109 Me NEt
22-Me-4-ClPh 1110 Me NH-3-amyl group 2-Me-4-ClPh 1111 Me N (CH2CH
2OMe)
2 2-Me-4-ClPh
1112 Me NHCH(CH
2OMe)
2 2-Me-4-ClPh
1113 Me NEt
2 2-Me-4-ClPh
1114 Me NEt
22-Cl-4-MePh 1115 Me NH-3-amyl group 2-Cl-4-MePh 1116 Me NHCH (CH2OMe)
2 2-Cl-4-MeOPh
1117 Me N(CH
2CH
2OMe)
2 2-Cl-4-MeOPh
1118 Me NHCH(Et)CH
2OMe 2-Cl-4-MeOPh
1119 Me N(c-Pr)CH
2CH
2CN 2-Cl-4-MeOPh
1120 Me NEt
22-Cl-4-MeOPh 1121 Me NH-3-amyl group 2-Cl-4-MeOPh 1123 Me NHCH (Et) CH2CH
2OMe 2-Cl-4-MeOPh
1124 Me NHCH(Me)CH
2CH
2OMe 2-Cl-4-MeOPh
1125 Me NHCH(Et)CH
2CH
2OMe 2-Br-4-MeOPh
1126 Me NHCH(Me)CH
2CH
2OMe 2-Br-4-MeOPh
1127 Me NHCH(Et)CH
2CH
2OMe 2-Me-4-MeOPh
1128 Me NHCH(Me)CH
2CH
2OMe 2-Me-4-MeOPh
1129 Me NHCH(CH
2OMe)
2 2-Cl-4,5-(MeO)
2Ph
1130 Me N(CH
2CH
2OMe)
2 2-Cl-4,5-(MeO)
2Ph
1131 Me NHCH(Et)CH
2OMe 2-Cl-4,5-(MeO)
2Ph
1132 Me N(c-Pr)CH
2CH
2CN 2-Cl-4,5-(MeO)
2Ph
1133 Me NEt
2 2-Cl-4,5-(MeO)
2Ph 1134 Me NH-3-amyl group 2-Cl-4,5-(MeO)2Ph
1135 Me NHCH(Et)CH
2CH
2OMe 2-Cl-4,5-(MeO)
2Ph
1136 Me MHCH(Me)CH
2CH
2OMe 2-Cl-4,5-(MeO)
2Ph
1137 Me NHCH(CH
2OMe)
2 2-Br-4,5-(MeO)
2Ph
1138 Me N(CH
2CH
2OMe)
2 2-Br-4,5-(MeO)
2Ph
1139 Me NHCH(Et)CH
2OMe 2-Br-4,5-(MeO)
2Ph
1140 Me N(c-Pr)CH
2CH
2CN 2-Br-4,5-(MeO)
2Ph
1141 Me NEt
2 2-Br-4,5-(MeO)
2Ph 1142 Me NH-3-amyl group 2-Br-4,5-(MeO)2Ph
1143 Me NHCH(CH
2OMe)
2 2-Cl-4,6-(MeO)
2Ph
1144 Me N(CH
2CH
2OMe)
2 2-Cl-4,6-(MeO)
2Ph
1145 Me NEt
2 2-Cl-4,6-(MeO)
2Ph 1146 Me NH-3-amyl group 2-Cl-4,6-(MeO)2Ph
1147 Me NHCH(CH
2OMe)
2 2-Me-4,6-(MeO)
2Ph
1148 Me N(CH
2CH
2OMe)
2 2-Me-4,6-(MeO)
2Ph
1149 Me NHCH(Et)CH
2OMe 2-Me-4,6-(MeO)
2Ph
1150 Me NEt
2 2-Me-4,6-(MeO)
2Ph 1151 Me NH-3-amyl group 2-Me-4,6-(MeO)2Ph
1152 Me NHCH(Et)CH
2CH
2OMe 2-Me-4-MeOPh
1153 Me NHCH(Me)CH
2CH
2OMe 2-Me-4-MeOPh
1154 Me NHCH(CH
2OMe)
2 2-Me0-4-MePh
1155 Me N(CH
2CH
2OMe)
2 2-Me0-4-MePh
1156 Me NHCH(Et)CH
2OMe 2-Me0-4-MePh
1157 Me N(c-Pr)CH
2CH
2CN 2-Me0-4-MePh
1158 Me NEt
22-Me0-4-MePh 1159 Me NH-3-amyl group 2-Me0-4-MePh 1160 Me NHCH (Et) CH2CH
2OMe 2-Me0-4-MePh
1161 Me NHCH(Me)CH
2CH
2OMe 2-Me0-4-MePh
1162 Me NHCH(CH
2OMe)
2 2-Me0-4-MePh
1163 Me N(CH
2CH
2OMe)
2 2-Me0-4-MePh
1164 Me NHCH(Et)CH
2OMe 2-Me0-4-MePh
1165 Me N(c-Pr)CH
2CH
2CN 2-Me0-4-MePh
1166 Me NEt
22-Me0-4-MePh 1167 Me NH-3-amyl group 2-Me0-4-MePh 1168 Me NHCH (CH2OMe)
2 2-Me0-4-ClPh
1169 Me N(CH
2CH
2OMe)
2 2-Me0-4-ClPh
1170 Me NHCH(Et)CH
2OMe 2-Me0-4-ClPh
1171 Me NEt
22-Me0-4-ClPh 1172 Me NH-3-amyl group 2-Me0-4-ClPh
Utilizability
Estimating bioactive CRF-R1 receptors bind measures
Classify as down and be used for standard in conjunction with the description of the people CRF-R1 recipient cell membrane sepn of measuring that contains the clone and the description of mensuration itself.
Separate messenger RNA(mRNA) by the people hippocampus.Carry out the reverse transcription of described mRNA with oligomeric (dt) 12-18, by initiator codon to terminator codon increased in the coding region with PCR.With the PCR fragment cloning that produces in the EcoRV site of pGEMV, and reclaim inserting fragment with XhoI+XbaI, and clone thus in the XhoI+XbaI site of carrier pm3ar (the Epstein-Barr virus starting point and the hygromycin selectable marker that contain CMV promotor, SV40 ' t ' montage and early stage poly-a-signal, duplicate).The expression vector that is called phchCRFR that produces dyes at the 293EBNA transit cell, and selects keeping episomal described cell in the presence of 400 μ M Totomycin.Be incorporated under the Totomycin cell of selecting 4 weeks of survival, adapt in suspension growth and be used to produce following in conjunction with the film of measuring.To contain then and have an appointment 1 * 10
8Each equal portions of individual suspension cell are centrifugal, form settling and freezing.
During mensuration, (50mM HEPES damping fluid, pH7.0 contains 10mM MgCl in the ice-cold tissue buffer solution of 10ml with the freezing settling of the above-mentioned 293EBNA cell that contains the transfection of useful hCRFR1 acceptor
2, 2mM EGTA, 1 μ g/L presses down enzyme peptide, 1 μ g/ml leupeptin and 1 μ g/ml pepstatin) middle homogenize.With homogenize thing centrifugal 12 minutes, with the settling homogenize again in the 10ml tissue buffer solution that produces with 40000xg., after centrifugal 12 minutes settling is used for measuring with protein concentration 360 μ g/ml suspension with 40000xg again.
Carrying out combination on 96 well culture plates measures; Every pore capacities is 300 μ l.Adding 50 μ l in every hole is subjected to reagent thing diluent (the medicine final concentration is 10
-10To 10
-5M), 100 μ l
125I-sheep-CRF (
125I-o-CRF) (final concentration is 150pM) and the above-mentioned cell homogenize of 150 μ l thing.Then culture plate was hatched under room temperature 2 hours, then filter through GF/F filter (soaking with 0.3% polymine in advance) and hatch thing with suitable cell capture instrument.With the filter washed twice, take out independent filter with ice-cold mensuration damping fluid, on gamma counter, they are carried out radioactivity and measure.
By iteration curve fitting procedure LIGAND[P.J.Munson and D.Rodbard, Anal.Biochem.107:220 (1980)] to analyze the various reagent thing diluents that are subjected to right
125I-o-CRF combines the curve that suppresses with cytolemma, this curve can provide the K of inhibition
iValue is used to estimate biological activity with this value then.
If the K of compound in CRF suppresses
iValue is lower than about 10000nM, thinks that so this compound is activated.
The inhibition of the adenylate cyclase activity that CRF-stimulates
Can carry out the inhibition of the adenylate cyclase activity of CRF-stimulation and measure according to (Synapse 1:572 (1987)) described methods such as G.Battaglia.In brief, at 37 ℃, contain 100mM Tris-HCl (pH7.4,37 ℃), 10mM MgCl in 200ml
2, 0.4mMEGTA, 0.1%BSA, 1mM isobutyl methylxanthine (IBMX), 250 units/ml creatine phosphokinase, 5mM phosphocreatine, 100mM guanosine 5 '-triphosphoric acid, 100nMoCRF, (concentration range is 10 to antagonist peptide
-9To 10
-6M) and in the damping fluid of the initial weight in wet base tissue of 0.8mg (about 40-60mg albumen) reacted 10 minutes.By adding 1mMATP/[
32P] ATP (about 2-4mCi/ pipe) begins reaction, adds 100ml 50mM Tris-HCl, 45mM ATP and 2% sodium lauryl sulphate termination reaction.Be the rate of recovery of monitoring cAMP, in the every pipe of separate forward, add 1 μ l[
3H] cAMP (about 40000 dpm).The order with Dowex separate with alumina column [
32P] cAMP with [
32P] ATP.
Biological activity in the body
All can estimate the activity in vivo of The compounds of this invention with the existing also acceptable bioassay method in any this area.The illustrative example of these tests comprises that startle test, climbing test and chronic administration of the sense of hearing measure.These and other some model that is used to measure The compounds of this invention are seen the Brain Research Reviews (15:71 (1990)) of C.W.Berridge and A.J.Dunn.Can test these compounds with the rodent or the small mammal of any kind.
Compound of the present invention has utilizability when treating the imbalance relevant with the corticotropin releasing factor(CRF) abnormal level in the patient who suffers from dysthymia disorders, affective disorder and/or anxiety disorder.
Can give compound of the present invention, unusual by active substance is contacted treat these with the action site of intravital this material of Mammals.Can use the described compound of the method afford that is used for administration of any routine, perhaps as independent medicine, perhaps in the mode of medicine composition.Can they are individually dosed, but usually with the pharmaceutical carrier administration according to route of administration and standard preparation choice of practice.
The dosage of administration is according to for example kind, the frequency of treatment and the required variations such as effect of the character of the mode of pharmacodynamic profile, the administration of certain drug and approach, patient's age, body weight and healthy state, symptom and severity, treatment simultaneously of purposes and known factor.When being used for the treatment of described disease or disorder, compound of the present invention can be with dosage oral administration every day of 0.002-200mg/kg body weight activeconstituents.Usually with divided dose administration every day of 0.01-10mg/kg 1-4 time, perhaps obtain required pharmacological action effectively with sustained release preparation.
Formulation (composition) per unit that is suitable for administration contains the about 100mg activeconstituents of the 1mg-that has an appointment.In these medicinal compositionss, described activeconstituents generally exists with about 0.5-95% (weight) of composition total weight.
Can be with solid dosage, for example capsule, tablet or powder agent are perhaps with liquid dosage form for example elixir, syrup and/or the described activeconstituents of suspension agent orally give.Also can give compound of the present invention with sterile liquid formulation parenteral.
Can use the gelatine capsule agent that contains activeconstituents and appropriate carriers, described carrier is (but being not limited to) lactose, starch, Magnesium Stearate, stearic acid or derivatived cellulose for example.Similarly thinner can be used to prepare compressed tablets.Tablet and capsule all can be made the slowly-releasing product, so that the continuous release of medicine in for some time to be provided.Compressed tablets can be sugar coating sheet or bag film coated tablet, covering undesirable taste, or is used to protect described activeconstituents not to be subjected to environmental disruption, or makes tablet in the disintegration of gi tract selectivity.
The liquid dosage form of oral administration can contain tinting material or correctives, to increase patient's acceptability.
Generally speaking, water, pharmaceutically acceptable oil, salt solution, dextran (glucose) aqueous solution and relevant sugar soln and polyvalent alcohol are the carriers that is fit to of parenteral solution as propylene glycol or polyoxyethylene glycol.The solution of parenteral admin preferably contains the water-soluble salt of activeconstituents, suitable stablizer and (if desired) buffer substance.Oxidation inhibitor is the stablizer that is fit to as sodium bisulfite, S-WAT or xitix (alone or in combination).Also can use citric acid and its salt and EDTA.In addition, parenteral solution can contain sanitas, for example geramine, methyl p-hydroxybenzoate or propylparaben and chlorobutanol.
" Remington ' s Pharmaceutical Sciences " (A.Osol, canonical reference book of this area) seen and be set forth in to suitable pharmaceutical carrier.
The useful pharmaceutical dosage form of following explanation The compounds of this invention administration: capsule
The Powdered activeconstituents of 100mg, 150mg lactose, 50mg Mierocrystalline cellulose and 6mg Magnesium Stearate are filled in two portions hard gelatin capsule of standard, can prepare many unit capsule.Gelseal
The preparation activeconstituents is at the digestible oil mixture in soya-bean oil, Oleum Gossypii semen or the sweet oil for example, and injects by positive metathetical mode, pumps into and forms the soft gelatin capsule that contains the 100mg activeconstituents in the gelatin.Washing and dry capsule.Tablet
Prepare many tablets with ordinary method, make dose unit contain 100mg activeconstituents, 0.2mg colloid silica, 5mg Magnesium Stearate, 275mg Microcrystalline Cellulose, 11mg starch and 98.8mg lactose.Can carry out suitable dressing to increase palatability or delayed absorption.
Compound of the present invention also can be used as reagent or standard substance in the Biochemical Research of neural function, imbalance and disease.
Although describe and the present invention that demonstrated with the part embodiment preferred, other embodiment is conspicuous to those skilled in the art.Therefore, the invention is not restricted to specific embodiment described and demonstration, but can make amendment or change and do not depart from aim of the present invention it, complete scope of the present invention be described in appending claims.
Claims (21)
1. formula (50) compound and pharmacy acceptable salt thereof:
This compound of formula (50) is selected from: R wherein
3For-N (Et) (n-Bu), R
4aBe Cl, R
4bBe H, R
4cBe Cl, R
4dBe H, R
4eFormula (50) compound for H; R wherein
3For-N (n-Pr) (CH
2CPr), R
4aBe Cl, R
4bBe H, R
4cBe Cl, R
4dBe H, R
4eFormula (50) compound for H; R wherein
3For-NHCH (CH
2OMe)
2, R
4aBe Cl, R
4bBe H, R
4cBe Cl, R
4dBe H, R
4eFormula (50) compound for H; R wherein
3For-N (n-Pr)
2, R
4aBe Cl, R
4bBe H, R
4cBe Cl, R
4dBe H, R
4eFormula (50) compound for H; R wherein
3For-N (Et)
2, R
4aBe Br, R
4bBe H, R
4cBe OMe, R
4dBe H, R
4eFormula (50) compound for H; R wherein
3For-N (CH
2CH
2OMe)
2, R
4aBe Me, R
4bBe H, R
4cBe OMe, R
4dBe Me, R
4eFormula (50) compound for H; R wherein
3For-N (Et)
2, R
4aBe Me, R
4bBe H, R
4cBe OMe, R
4dBe Me, R
4eFormula (50) compound for H; R wherein
3For-N (CH
2CH
2OMe)
2, R
4aBe Me, R
4bBe H, R
4cBe Br, R
4dBe H, R
4eFormula (50) compound for H; R wherein
3For-N (Et)
2, R
4aBe Cl, R
4bBe H, R
4cBe OMe, R
4dBe H, R
4eFormula (50) compound for H; R wherein
3For-N (CH
2CH
2OMe)
2, R
4aBe Cl, R
4bBe H, R
4cBe OMe, R
4dBe H, R
4eFormula (50) compound for H; R wherein
3Be N (CH
2CH
2OMe)
2, R
4aBe Me, R
4bBe H, R
4cBe OMe, R
4dBe H, R
4eFormula (50) compound for H.
2. the compound of claim 1 and pharmacy acceptable salt thereof, wherein said compound is selected from:
4-(N-ethyl-N-fourth amino)-2,7-dimethyl-8-(2,4 dichloro benzene base)-[1,5-a]-pyrazoles-1,3,5-triazines;
4-(N-n-propyl-N-(cyclopropyl) methylamino-)-2,7-dimethyl-8-(2,4 dichloro benzene base)-[1,5-a]-pyrazoles-1,3,5-triazines;
4-(1,3-dimethoxy third-2-base is amino)-2,7-dimethyl-8-(2,4 dichloro benzene base)-[1,5-a]-pyrazoles-1,3,5-triazines;
4-dipropyl amino-2,7-dimethyl-8-(2,4 dichloro benzene base)-[1,5-a]-pyrazoles-1,3,5-triazines;
4-diethylin-2,7-dimethyl-8-(2-bromo-4-p-methoxy-phenyl)-[1,5-a]-pyrazoles-1,3,5-triazines;
4-diethylin-2,7-dimethyl-8-(2,5-dimethyl-4-p-methoxy-phenyl)-[1,5-a]-pyrazoles-1,3,5-triazines;
4-(two-(2-methoxy ethyl) amino)-2,7-dimethyl-8-(4-bromo-2-aminomethyl phenyl)-[1,5-a]-pyrazoles-1,3,5-triazines;
4-diethylin-2,7-dimethyl-8-(2-chloro-4-p-methoxy-phenyl)-[1,5-a]-pyrrolo--1,3,5-triazines;
4-(two-(2-methoxy ethyl) amino)-2,7-dimethyl-8-(2-chloro-4-p-methoxy-phenyl)-[1,5-a]-pyrazoles-1,3,5-triazines;
4-(two-(2-methoxy ethyl) amino)-2,7-dimethyl-8-(2-methyl-4-p-methoxy-phenyl)-[1,5-a]-pyrazoles-1,3,5-triazines;
4-(two-(2-methoxy ethyl) amino)-2,7-dimethyl-8-(2,5-dimethyl-4-p-methoxy-phenyl)-[1,5-a]-pyrazoles-1,3,5-triazines.
3. the compound of claim 1 and pharmacy acceptable salt thereof, wherein said compound is a 4-diethylin-2,7-dimethyl-8-(2,5-dimethyl-4-p-methoxy-phenyl)-[1,5-a]-pyrazoles-1,3,5-triazines.
4. the compound of claim 1 and pharmacy acceptable salt thereof, wherein said compound is 4-(N-ethyl-N-fourth amino)-2,7-dimethyl-8-(2,4 dichloro benzene base)-[1,5-a]-pyrazoles-1,3,5-triazines.
5. the compound of claim 1 and pharmacy acceptable salt thereof, wherein said compound is 4-(N-n-propyl-N-(cyclopropyl) methylamino-)-2,7-dimethyl-8-(2,4 dichloro benzene base)-[1,5-a]-pyrazoles-1,3,5-triazines.
6. the compound of claim 1 and pharmacy acceptable salt thereof, wherein said compound is 4-(two-(2-methoxy ethyl) amino)-2,7-dimethyl-8-(2-methyl-4-p-methoxy-phenyl)-[1,5-a]-pyrazoles-1,3,5-triazines.
7. the compound of claim 1 and pharmacy acceptable salt thereof, wherein said compound is 4-(two-(2-methoxy ethyl) amino)-2,7-dimethyl-8-(2,5-dimethyl-4-p-methoxy-phenyl)-[1,5-a]-pyrazolo-1,3,5-triazines.
8. medicinal compositions, said composition contain the compound of the claim 1 of pharmaceutically acceptable carrier and treatment significant quantity.
9. medicinal compositions, said composition contain the compound of the claim 2 of pharmaceutically acceptable carrier and treatment significant quantity.
10. medicinal compositions, said composition contain the compound of the claim 3 of pharmaceutically acceptable carrier and treatment significant quantity.
11. a medicinal compositions, said composition contain the compound of the claim 4 of pharmaceutically acceptable carrier and treatment significant quantity.
12. a medicinal compositions, said composition contain the compound of the claim 5 of pharmaceutically acceptable carrier and treatment significant quantity.
13. a medicinal compositions, said composition contain the compound of the claim 6 of pharmaceutically acceptable carrier and treatment significant quantity.
14. a medicinal compositions, said composition contain the compound of the claim 7 of pharmaceutically acceptable carrier and treatment significant quantity.
15. the purposes of the compound of claim 1 in the medicine of preparation treatment Mammals anxiety disorder or dysthymia disorders.
16. the purposes of the compound of claim 2 in the medicine of preparation treatment Mammals anxiety disorder or dysthymia disorders.
17. the purposes of the compound of claim 3 in the medicine of preparation treatment Mammals anxiety disorder or dysthymia disorders.
18. the purposes of the compound of claim 4 in the medicine of preparation treatment Mammals anxiety disorder or dysthymia disorders.
19. the purposes of the compound of claim 5 in the medicine of preparation treatment Mammals anxiety disorder or dysthymia disorders.
20. the purposes of the compound of claim 6 in the medicine of preparation treatment Mammals anxiety disorder or dysthymia disorders.
21. the purposes of the compound of claim 7 in the medicine of preparation treatment Mammals anxiety disorder or dysthymia disorders.
Applications Claiming Priority (6)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| US68604796A | 1996-07-24 | 1996-07-24 | |
| US2329096P | 1996-07-24 | 1996-07-24 | |
| US08/686,047 | 1996-07-24 | ||
| US60/023,290 | 1996-07-24 | ||
| US08/899,242 US6124289A (en) | 1996-07-24 | 1997-07-23 | Azolo triazines and pyrimidines |
| US08/899,242 | 1997-07-23 |
Related Child Applications (2)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CN 01120849 Division CN1250223C (en) | 1996-07-24 | 2001-05-30 | Pyrrolo-triazine and pyrimidine compounds |
| CN 02118589 Division CN1388126A (en) | 1996-07-24 | 2002-04-25 | Pyrrolotriazine and pyrimidine compound |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| CN1225637A CN1225637A (en) | 1999-08-11 |
| CN1104432C true CN1104432C (en) | 2003-04-02 |
Family
ID=27362048
Family Applications (3)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CN97196525A Expired - Lifetime CN1104432C (en) | 1996-07-24 | 1997-07-23 | Pyrrole triazines and pyrimidines |
| CN 01120849 Expired - Lifetime CN1250223C (en) | 1996-07-24 | 2001-05-30 | Pyrrolo-triazine and pyrimidine compounds |
| CN 02118589 Pending CN1388126A (en) | 1996-07-24 | 2002-04-25 | Pyrrolotriazine and pyrimidine compound |
Family Applications After (2)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CN 01120849 Expired - Lifetime CN1250223C (en) | 1996-07-24 | 2001-05-30 | Pyrrolo-triazine and pyrimidine compounds |
| CN 02118589 Pending CN1388126A (en) | 1996-07-24 | 2002-04-25 | Pyrrolotriazine and pyrimidine compound |
Country Status (15)
| Country | Link |
|---|---|
| JP (2) | JP4704521B2 (en) |
| CN (3) | CN1104432C (en) |
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| CA (1) | CA2259583C (en) |
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| HR (1) | HRP970413A2 (en) |
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| SI (1) | SI9720045B (en) |
| SK (1) | SK286461B6 (en) |
Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN103694242A (en) * | 2013-12-10 | 2014-04-02 | 中国科学院昆明植物研究所 | Pyrazolopyrimidine compound and pharmaceutical composition thereof as well as pharmaceutical application of pyrazolopyrimidine compound |
Families Citing this family (8)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| MXPA03008185A (en) * | 2001-03-13 | 2004-01-29 | Bristol Myers Squibb Pharma Co | 4-(2-butylamino)-2,7-dimethyl-8-(2-methyl-6-methoxypyrid-3-yl) pyrazolo-[1,5-a]-1,3, 5-triazine, its enantiomers and pharmaceutically acceptable salts as corticotropin releasing factor receptor ligands. |
| WO2004110454A1 (en) * | 2003-06-13 | 2004-12-23 | Ishihara Sangyo Kaisha, Ltd. | COMPOSITION FOR TREATMENT FOR OR PREVENTION OF DISEASE NECESSITATING ADMINISTRATION OF ADENOSINE A2a RECEPTOR AGONIST |
| US7329662B2 (en) * | 2003-10-03 | 2008-02-12 | Hoffmann-La Roche Inc. | Pyrazolo-pyridine |
| GB0519957D0 (en) * | 2005-09-30 | 2005-11-09 | Sb Pharmco Inc | Chemical compound |
| KR101088239B1 (en) * | 2006-09-20 | 2011-11-30 | 일라이 릴리 앤드 캄파니 | Thiazole pyrazolopyrimidines as crf1 receptor antagonists |
| CN112028891B (en) * | 2019-07-30 | 2022-07-05 | 厦门宝太生物科技股份有限公司 | Adenosine receptor antagonists |
| KR20230043222A (en) | 2020-08-12 | 2023-03-30 | 스프루스 바이오사이언시스 인코포레이티드 | Methods and compositions for treating polycystic ovary syndrome |
| US11708372B2 (en) | 2021-11-19 | 2023-07-25 | Spruce Biosciences, Inc. | Crystalline composition of tildacerfont and methods of use and preparation thereof |
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| Publication number | Priority date | Publication date | Assignee | Title |
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| US3995039A (en) * | 1975-05-27 | 1976-11-30 | Merck & Co., Inc. | Pyrazolo [1,5-a] [1,3,5] triazines |
| US4824834A (en) * | 1986-10-31 | 1989-04-25 | Otsuka Pharmaceutical Company, Limited | Pyrazolotriazine compounds |
| EP0414200A2 (en) * | 1989-08-25 | 1991-02-27 | Otsuka Pharmaceutical Factory, Inc. | Salts of optically active 4-hydroxy-8-(3-lower alkoxy-4-phenylsulfinylphenyl)pyrazolo [1,5-a]-1,3,5-triazines and a process for production thereof |
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| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JPS6157587A (en) * | 1984-08-29 | 1986-03-24 | Shionogi & Co Ltd | Condensed heterocyclic derivative and antiulcerative |
| US5420128A (en) * | 1990-10-09 | 1995-05-30 | Otsuka Pharmaceutical Co., Ltd. | Pyrimidine derivatives, method of manufacturing the same, and androgen inhibitor |
| DE69130683T2 (en) * | 1991-04-22 | 1999-05-06 | Otsuka Pharma Co Ltd | PYRAZOLO [1,5-a] PYRIMIDINE DERIVATIVES AND ANTI-INFLAMMATORY CONTAINERS THEREOF |
| US5356897A (en) * | 1991-09-09 | 1994-10-18 | Fujisawa Pharmaceutical Co., Ltd. | 3-(heteroaryl)-pyrazololi[1,5-a]pyrimidines |
-
1997
- 1997-07-23 NZ NZ333777A patent/NZ333777A/en not_active IP Right Cessation
- 1997-07-23 CN CN97196525A patent/CN1104432C/en not_active Expired - Lifetime
- 1997-07-23 SK SK97-99A patent/SK286461B6/en not_active IP Right Cessation
- 1997-07-23 BR BR9710544A patent/BR9710544A/en not_active IP Right Cessation
- 1997-07-23 PL PL97331523A patent/PL195762B1/en unknown
- 1997-07-23 IL IL12787197A patent/IL127871A0/en unknown
- 1997-07-23 CZ CZ0018499A patent/CZ299451B6/en not_active IP Right Cessation
- 1997-07-23 EE EEP199900019A patent/EE04316B1/en unknown
- 1997-07-23 CA CA002259583A patent/CA2259583C/en not_active Expired - Lifetime
- 1997-07-23 EA EA199900158A patent/EA004403B1/en not_active IP Right Cessation
- 1997-07-23 JP JP50723398A patent/JP4704521B2/en not_active Expired - Fee Related
- 1997-07-23 SI SI9720045A patent/SI9720045B/en active Search and Examination
- 1997-07-24 HR HRP970413 patent/HRP970413A2/en not_active Application Discontinuation
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1998
- 1998-12-30 IL IL127871A patent/IL127871A/en not_active IP Right Cessation
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1999
- 1999-01-21 NO NO19990264A patent/NO315610B3/en not_active IP Right Cessation
-
2001
- 2001-05-30 CN CN 01120849 patent/CN1250223C/en not_active Expired - Lifetime
-
2002
- 2002-04-25 CN CN 02118589 patent/CN1388126A/en active Pending
- 2002-06-11 IL IL150163A patent/IL150163A/en not_active IP Right Cessation
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2004
- 2004-07-23 JP JP2004216483A patent/JP4194539B2/en not_active Expired - Fee Related
- 2004-10-12 IL IL164513A patent/IL164513A/en not_active IP Right Cessation
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2005
- 2005-07-11 AR ARP050102868A patent/AR049583A2/en not_active Application Discontinuation
Patent Citations (3)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US3995039A (en) * | 1975-05-27 | 1976-11-30 | Merck & Co., Inc. | Pyrazolo [1,5-a] [1,3,5] triazines |
| US4824834A (en) * | 1986-10-31 | 1989-04-25 | Otsuka Pharmaceutical Company, Limited | Pyrazolotriazine compounds |
| EP0414200A2 (en) * | 1989-08-25 | 1991-02-27 | Otsuka Pharmaceutical Factory, Inc. | Salts of optically active 4-hydroxy-8-(3-lower alkoxy-4-phenylsulfinylphenyl)pyrazolo [1,5-a]-1,3,5-triazines and a process for production thereof |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN103694242A (en) * | 2013-12-10 | 2014-04-02 | 中国科学院昆明植物研究所 | Pyrazolopyrimidine compound and pharmaceutical composition thereof as well as pharmaceutical application of pyrazolopyrimidine compound |
| CN103694242B (en) * | 2013-12-10 | 2016-01-06 | 昆明翔昊科技有限公司 | Pyrazolopyrimidines and pharmaceutical composition thereof and its application in pharmacy |
Also Published As
| Publication number | Publication date |
|---|---|
| EE9900019A (en) | 1999-08-16 |
| CN1225637A (en) | 1999-08-11 |
| CA2259583A1 (en) | 1998-01-29 |
| NZ333777A (en) | 2000-07-28 |
| CN1250223C (en) | 2006-04-12 |
| SI9720045A (en) | 1999-10-31 |
| EA199900158A1 (en) | 1999-10-28 |
| IL164513A (en) | 2010-04-29 |
| IL150163A (en) | 2010-12-30 |
| NO990264D0 (en) | 1999-01-21 |
| EA004403B1 (en) | 2004-04-29 |
| IL164513A0 (en) | 2005-12-18 |
| NO315610B1 (en) | 2003-09-29 |
| NO315610B3 (en) | 2003-09-29 |
| JP2002513382A (en) | 2002-05-08 |
| IL127871A0 (en) | 1999-10-28 |
| CN1327793A (en) | 2001-12-26 |
| AR049583A2 (en) | 2006-08-16 |
| NO990264L (en) | 1999-03-10 |
| SK286461B6 (en) | 2008-10-07 |
| CN1388126A (en) | 2003-01-01 |
| PL195762B1 (en) | 2007-10-31 |
| JP4704521B2 (en) | 2011-06-15 |
| CZ299451B6 (en) | 2008-07-30 |
| IL127871A (en) | 2010-04-29 |
| CA2259583C (en) | 2009-11-17 |
| JP2005097257A (en) | 2005-04-14 |
| PL331523A1 (en) | 1999-07-19 |
| EE04316B1 (en) | 2004-06-15 |
| SK9799A3 (en) | 2005-04-01 |
| CZ18499A3 (en) | 1999-11-17 |
| BR9710544A (en) | 1999-08-17 |
| SI9720045B (en) | 2008-02-29 |
| JP4194539B2 (en) | 2008-12-10 |
| HRP970413A2 (en) | 1998-10-31 |
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