CN101516369A - Pyridinone diketo acids: inhibitors of HIV replication in combination therapy - Google Patents
Pyridinone diketo acids: inhibitors of HIV replication in combination therapy Download PDFInfo
- Publication number
- CN101516369A CN101516369A CNA2007800346972A CN200780034697A CN101516369A CN 101516369 A CN101516369 A CN 101516369A CN A2007800346972 A CNA2007800346972 A CN A2007800346972A CN 200780034697 A CN200780034697 A CN 200780034697A CN 101516369 A CN101516369 A CN 101516369A
- Authority
- CN
- China
- Prior art keywords
- azido
- dideoxy
- alkyl
- methyl
- hiv
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Pending
Links
Abstract
A new class of diketo acids constructed on pyridinone scaffolds, designed as inhibitors of HTV replication through inhibition of HIV integrase, is described. These compounds are useful in the prevention or treatment of infection by HIV and in the treatment of AIDS and ARC, either as the compounds, or as pharmaceutically acceptable salts, with pharmaceutically acceptable carriers, used alone or in combination with antivirals, immunomodulators, antibiotics, vaccines, and other therapeutic agents, especially other anti- HIV compounds (including other anti-HIV integrase agents), which can be used to create combination anti-HIV cocktails. Methods of treating AIDS and ARC and methods of treating or preventing infection by HIV are also described. Compounds of the present application include those of formula I and include tautomers, regioisomers, geometric isomers, and pharmaceutically acceptable salts thereof, wherein the pyridinone scaffold and R groups are as otherwise defined in the specification. These are combined, with any number of typical other anti-HIV agents (including other integrase-based anti-HIV agents) and other combination therapeutic agents described herein, to provide an effective treatment modality for HIV infections, including AIDS and ARC.
Description
Invention field
The present invention relates to the antiviral therapy field, especially treat people HIV and infect, the preferred compositions treatment.
Related application and financial support
The provisional application US60/831 that submit to the 19 days July in 2006 that the application requires title to be " pyridinone diketo acids: HIV replication inhibitors ", 990, the provisional application US60/920 that submitted to March 27 in 2007,196, with the provisional application 60/920 of title for 27 submissions March in 2007 of " pyridinone diketo acids: the HIV replication inhibitors that is used for combined therapy ", 197 priority, described application is complete to be incorporated herein by reference.
The working portion of present patent application has obtained from the National Institutes of Health bonus number support for the fund of A143181.Therefore, U.S. government keeps certain right to this invention.
Background of invention
The human immunodeficiency virus is HIV, and the viral enzyme by three keys of its pol gene code and these enzymes are for duplicating of this virus very important [Fauci, Science, 239,617-622 (1988); Katz ﹠amp; Skalka, Annu.Rev.Biochem., 63,133-173 (1994); Frankel, Annu.Rev.Biochem., 67,1-25 (1998)].Therefore, in the exploitation HIV antiviral chemotherapeutics, these enzymes of pol gene are as the possible target spot [De Clercq, J.Med.Chem.38, the 2491-2517 (1995) that attack; Clin.Microbiol.Rev., 10,674-693 (1997); De Clercq, Nature Reviews:DrugDiscovery, 11,13-25 (2002); De Clercq, J.Med.Chem.48,1297-1313 (2005)].Relate to this two kinds of enzymes, the drug development of hiv reverse transcriptase (RT) and hiv protease (PR), and some the therapeutic agent combined therapies in these therapeutic agents are used for the follow-up clinical application of the treatment of the relevant complex with AIDS of acquired immune deficiency syndrome (AIDS) (AIDS) (complex) HAART (treatment of high activity retrovirus) (ARC), have illustrated that these class methods of targeting key enzyme have shown useful approach [the Johnson ﹠amp that is used for the antiviral chemotherapy; Gerber, " Advances in Internal Medicine, " vol.44.Mosby:St.Louis, 1-40 (2000); De Clercq, Nature Reviews:Drug Discovery, 11,13-25 (2002); Miller ﹠amp; Hazuda, Current Opinion in Microbiology, 4,535-539 (2001); Asante-Appiah ﹠amp; Skalka, Adv.Virus Res., 52,351-369 (1999); Nair, " RecentAdvances in Nucleosides:Chemistry and chemotherapy, " Elsevier Science:Netherlands, 149-166 (2002); DeClercq, Intl.J.Biochem.Cell Biol.36,1800-1822 (2004)].And for treatment, HIV RT and HIV PR have been widely studied, the 3rd enzyme of pol gene, hiv integrase (integrase), the much less of research [Miller ﹠amp; Hazuda, Current Opinion in Microbiology, 4,535-539 (2001); Nair, Rev.Med.Virol., 12,179-193 (2002); Nair, Current Pharmaceutical Design, 9,2553-2565 (2003); People such as Pommier, Nature Rev.Drug Discovery 4,236-248 (2005); Nair, Frontiersin Med.Chem.2,3-20 (2005)].
Mechanism of action is the HIV/AIDS of inhibition hiv integrase not have at present medicine to be used for wherein clinically.The HIV-1 intergrase be pol gene 3 '-albumen [the Asante-Appiah ﹠amp of the 32kDa of terminal coding; Skalka, Adv.Virus Res., 52,351-369 (1999); Esposito ﹠amp; Craigie, Adv.Virus Res., 52,319-333 (1999)].It relates to the integration (integration) of HIV DNA to host cell chromosome.Because intergrase nobody homologue (counterpart), and in finishing HIV intrusion people cell, play an important role, it is the attack target spot of the inhibitor of exploitation treatment effect.
HIV DNA be incorporated into host cell nuclear staining body DNA obviously by by specific sequence 3 '-processing or shear and be connected enzyme catalysis [the Asante-Appiah ﹠amp that (strand) conversion/integrating remark produces; Skalka, Adv.Virus Res., 52,351-369 (1999); Esposito ﹠amp; Craigie Adv.Virus Res., 52,319-333 (1999)].Before the beginning integration process, the viral DNA that assembling produces through reverse transcription in advance on intergrase.Distinguished sequence among the LTRs of hiv integrase identification viral DNA.Behind assembling viral DNA on the intergrase, wherein has the processing of the active place's generation of locus specificity endonuclease viral DNA, and two nucleotidases from the Double helix viral DNA each 3 '-end is cut out producing specific viral DNA, described specific viral DNA embeds and has a terminal CAOH-3 ' through two nucleotidases.For initial 3 '-procedure of processing, intergrase has obviously activated the phosphodiester bond for cutting.So the viral DNA of the embedding that produces is connected to host cell nuclear DNA through trans-esterification in next step.In this step, intergrase be positioned at 3 of viral DNA '-the OH end, be used for the phosphodiester bond of nucleophillic attack host DNA.In subsequent step, in host DNA, produce the cutting of 4-6bp, and this coupling relates to after the processing
CAOH-3 ' viral DNA end to 5 of host DNA '-connection of phosphate terminal.At last, repair resulting intermediate through host cell enzymes (although intergrase also may have this effect) mediation jaggy.
A large amount of chemical compounds are hiv integrase inhibitor, but some chemical compounds in these chemical compounds are non--specific inhibitors of enzyme, evidence show that then other chemical compound can have specificity.The different classes of nucleotidase that comprises, the oligonucleotide enzyme, dinucleotide enzyme and various micromolecule (comprise heterocyclic system, natural product, two keto acids, sulfone and other [Nair, Rev.Med.Virol., 12,179-193 (2002); Nair, Current Pharmaceutical Design, 9,2553-2565 (2003); Chi and and Nair, Bioorg.Med.Chem.Lett.14,4815-4817 (2004); Nair and coworkers, J.Am.Chem.Soc., 122,5671-5677 (2000)].
This compounds the most directly related with this patent of previous research is for having the substituent diketone of aryl or heteroaryl.Some these compounds are hiv integrase inhibitor, but the most common only be chain transfer step (strand transfer step).Intergrase suppresses data report [Wai in some scientific publication things, Deng the people, " 4-Aryl-2,4-dioxobutanoic acid inhibitors of HIV-1 integrase and viralreplication in cells; " J.Med.Chem.43,4923-4926 (2000); Pais, G.C.G. waits the people, " Structure activity of 3-aryl-1,3-diketo-containing compounds as HIV-1 integraseinhibitors, " J.Med.Chem.45,3184-3194 (2002); Marchand, C. waits the people, " Structural determinants for HIV-1 integrase inhibition by β-diketo acids, " J.Biol.Chem.277,12596-12603 (2002); Sechi, M. waits the people, " Design and synthesisof novel indole beta-diketo acid derivatives as HIV-1 integrase inhibitors, " J.Med.Chem.47,5298-5310 (2004); Zhang, Deng the people, " Azido-containing aryl β-ketoacid HIV-1 integrase inhibitors; " Bioorg.Med.Chem.Lett.13,1215-1219 (2003), Nair, Deng the people, " HIV integrase inhibitors with nucleobase scaffolds:discovery of ahighly potent anti-HIV agent, " J.Med.Chem.49,445-447 (2006); Nair waits the people, " Conceptually novel HIV integrase inhibitors with nucleobase scaffolds:discovery of a highly potent anti-HIV agent, " Antiviral Res.70, A26 (2006); Sato waits the people, " Novel HIV-1 integrase inhibitors derived from quinolone antibiotics, " J.Med.Chem.49,1506-1508 (2006); People such as Nair, " Beta-diketo acids with purinenucleobase scaffolds:novel selective inhibitors of the strand transfer step of HIVintegrase; " Bioorg.Med.Chem.Lett.16,1920-1923 (2006), people such as Chi, " A noveldiketo phosphonic acid that exhibits specific; strand-transfer inhibition of HIVintegrase and anti-HIV activity; " Bioorg.Med.Chem.Lett.17,1266-1269 (2007)].The publication in other this field is a surround relationship for the application.
The mechanism of action of hiv integrase inhibitor by diketone may be the results of interaction of the avtive spot metal ion of functional group on these chemical compounds and intergrase, caused the functionality of these crucial metal common factors to isolate (functional sequestration) [Grobler, J.A., Deng the people, Proc.Natl.Acad.Sci.U.S.A.99,6661-6666 (2002)].
The patent relevant with the application is: Selnick, people such as H.G., (Merck ﹠amp; Co.Inc.), and " Preparation of nitrogen-containing 4-heteroaryl-2,4-dioxobutyric acids useful asHIV integrase inhibitors, " WO 9962513; Young, S.D. waits the people, (Merck ﹠amp; Co.Inc.), and " Preparation of aromatic and heteroaromatic 4-aryl-2,4-dioxobutyric acidderivatives useful as HIV integrase inhibitors, " WO 9962897; Fujishita, T. waits the people, Yoshinaga, T. waits people (Shionogi ﹠amp; Co.Ltd.), " Preparation of aromatic heterocyclecompounds having HIV integrase inhibiting activities, " WO 0039086; Akihiko, S., (Shionogi ﹠amp; Co.Ltd.), " Medicinal compositions containing propenonederivatives, " WO 0196329; Payne, L.S. waits the people, (Merck ﹠amp; Co.Inc.; Tularik, Inc.), " Preparation of 1,3-diaryl-1,3-propanediones as HIV integrase inhibitors, " WO0100578; Egbertson, M. waits the people, (Merck ﹠amp; Co.Ltd.), " HIV integrase inhibitors, " WO 9962520.Above-mentioned some patents of quoting are closely related.Yet these patents or publication are not all described this compounds of the present invention.With the application other patent of surround relationship: Anthony is arranged, wait the people, (Merck ﹠amp; Co.Inc.), " Aza and polyaza-napthalenyl-carboxamides useful asHIV integrase inhibitors, " WO 02/30426; Sato waits the people, (Japan Tobacco Inc.), " Preparation of 4-oxoquinoline derivatives as HIV integrase inhibitors, " WO2004046115; Sato waits the people, (Japan Tobacco Inc.), " Novel 4-oxoquinolinecompounds and use thereof as HIV integrase inhibitors, " WO 2005113509; Crescenzi, Deng the people, (Instituto Di Richerche Di Biologia Molecolare P.AngelettiSPA) " Preparation of N-substituted hydroxypyrimidinone carboxamide inhibitorsof HIV integrase, " WO 2003035077; Belyk waits the people, (Merck ﹠amp; Co.Inc., InstitutoDi Richerche Di Biologia Molecolare P.Angeletti SPA), " Preparation ofN-(4-fluorobenzyl)-5-hydroxy-1-methyl-2-(1-methyl-1-{[(5-methyl-1; 3; 4-oxadiazol-2-yl) carbonyl] amino}ethyl)-6-oxo-1; 6-dihydropyrimidine-4-carboxamidepotassium salts as HIV integrase inhibitors, " WO 2006060712; Sato waits the people, (Japan Tobacco Inc.), " Preparation of quinolizinone compounds as HIV integraseinhibitors, " WO 2006033422; Yoshida, H. waits the people, (Shionogi ﹠amp; Co.Ltd.), " Preparation of carbamoyl-pyridinone derivative having HIV integrase inhibitoryactivity, " WO 2006030807; Dress waits the people, (Pfizer, Inc.), " Preparation ofN-hydroxy pyrrolopyridinecarboxamides as inhibitors of HIV integrase, " WO2006027694; Naidu waits the people, (Bristol-Myers Squibb Co.), " HIV integraseinhibitors, " US 2005/0261322; Naidu waits the people, (Bristol-Myers Squibb Co.), " Bicyclic heterocycles as HIV integrase inhibitors, " US 2005/0267105; Naidu waits the people, (Bristol-Myers Squibb Co.), " Bicyclic heterocycles as HIV integraseinhibitors, " US 2006/0199956.Above-mentioned some patents of quoting are more relevant than other patent, but described patent or publication are not all described this compounds of the present invention.
This compounds that we describe in the present invention is the HIV-1 integrase inhibitor, and also has external anti-HIV activity.Be used for clinical isolating PBMC, HIV
NL4-3In the example (in PBMC our chemical compound 4-(1,5-dibenzyl-1,2-dihydro-2-oxo-pyridin-3-yl)-2-hydroxyl-4-oxo fourth-2 olefin(e) acid (8) of research and in same research, studying AZT) of anti-HIV data as follows.
Chemical compound 8 EC
950.61 μ M, CC
95>200 μ M, therapeutic index (TI)>330
AZT EC
959.42nM, CC
95>1 μ M, therapeutic index (TI)>106
PH 7.4,8 half-life of chemical compound (t
1/2) be>41 hours.The t of chemical compound 8 in people's hepatomicrosome of collecting
1/2Be>6 hours.
Summary of the invention
The present invention put down in writing a class novelty with the pyridone framework construction and by suppressing two keto acids of hiv integrase as the HIV replication inhibitors.These chemical compounds can be expressed as general formula I and (and comprise its tautomer, regional isomer (regioisomers) and geometric isomer, and the acceptable salt of pharmacy, when applicable), wherein the part in the block diagram (moiety) is the molecular skeleton that constitutes with Pyridione derivatives.These chemical compounds are used for prevention or treatment HIV infects and treatment AIDS and ARC, with chemical compound or the acceptable salt of its pharmacy, with pharmaceutically acceptable carrier, use separately or be used in combination with antiviral agent, immunomodulator, antibiotic, vaccine and other therapeutic agent especially other anti-HIV chemical compound (comprising other anti-HIV intergrase medicine) (they can be used for producing the combination of combination anti-HIV HAART).The method of treatment AIDS and ARC and the method for treatment or prevention HIV infection are also disclosed.
The preferred aspect of the purposes of other anti-hiv agent combination that also relates at least a above-claimed cpd and at least a this paper and put down in writing of the present invention.
Detailed Description Of The Invention
In whole description, use following term description the present invention.Except as otherwise noted, being used for term of the present invention explains by the meaning of those skilled in the art's common sense.
Term herein " chemical compound " except as otherwise noted, is meant any concrete chemical compound disclosed herein, comprises its tautomer, regional isomer, geometric isomer and if desired, optical isomer, with and the acceptable salt of pharmacy.In the context of this article, the term chemical compound is often referred to individualized compound, but also can comprise other chemical compound for example stereoisomer, regional isomer and/or the optical isomer (comprising racemic mixture) of disclosed chemical compound and the mixture of special enantiomer or enantiomer enrichment.Term " chemical compound " scope should be used for explaining according to this term making in context.
Term " patient " or " experimenter " of running through description are meant animal, and normally mammal people preferably uses compositions provided by the invention that they are treated and comprises prophylactic treatment.For the treatment of those infection, disease or morbid state, its for concrete animal for example people patient be specific, the term patient is meant the animal that this is concrete.
Term herein " effectively ", except as otherwise noted, a certain amount of chemical compound or compositions or composition are described, it is used for producing or influencing desired result in context, if this result relates in particular to virus, microorganism or other morbid state, disease or the disease relevant with HIV, ARC or AIDS; Perhaps be used to prepare other chemical compound, medicine or compositions.This term comprises all other effective doses or valid density term, and it is described in this application in addition.
The term " skeleton (scaffold) " that runs through description is meant the pyridone chemical constitution, can contain at least 4 substituent groups in substituted position at this skeleton at 5, and one of them is the keto acid (ketoacid) that defines in addition herein, other 4, and R
1, R
2, R
3And R
4As definition herein.
Term " heteroaryl " is meant 5 or 6-unit hetero-aromatic ring, and it contains 1~2 hetero atom that is selected from oxygen, nitrogen and sulfur, and this hetero-aromatic ring is optional to be replaced by 1~3 substituent group, and described substituent group is halogen, hydroxyl, C for example
1-3Alkyl, C
1-3Alkoxyl and CF
3Term heteroaryl and " hetero-aromatic ring " can exchange use in this article.
Term " human immunodeficiency virus " or " HIV " can be used for describing human immunodeficiency virus 1 and 2 (HIV-1 and HIV-2).
Term " ARC " and " AIDS " are meant the immune system syndrome that the human immunodeficiency virus causes, and it is characterized in that the susceptibility to some disease, and compare the decline of T cell counting with normal counting.HIV from 1 class (asymptomatic HIV disease) be developed to 2 classes (ARC), to 3 classes (AIDS), severity of disease increases.
1 class HIV infection characteristic is that patient or experimenter are the HIV positives, and is asymptomatic but also do not have and be less than 500 cd4 cell.If the patient has the disease that the listed AIDS-to 2 classes (ARC) or 3 classes (AIDS) of any following table defines, then the patient does not belong to such.Be lower than 500 if patient's t-cell counting has dropped to, then the patient is considered to 2 classes (ARC) or 3 classes (AIDS).
2 classes (ARC) infection characteristic is following standard: patient's T-cell has dropped to and has been lower than 500, but also is not lower than 200, and the patient does not also have 3 class diseases (as follows) but the disease of at least a following qualification has been arranged--
The ο BA
The ο candidiasis, (thrush) of oropharynx
The ο candidiasis, vulvoaginal; Lasting to treating, often or seldom reply
ο cervical atypical hyperplasia (moderate or serious)/carcinoma in situs of cervix
ο General Symptoms, for example heating (38.5C) or lasting above 1 month diarrhoea
The ο hairy leukoplakia, the oral cavity
ο herpes zoster (shingles) relates at least two kinds of different outbreaks or more than a kind of dermatotome
The ο idiopathic thrombocytopenic purpura
The ο listeriosis
If the ο inflammatory pelvic disease is concurrent especially tubo-ovarian abscess
The ο peripheral neuropathy
According to U.S. government, in 2 class ARC, immune system has shown the signal of damage but has not been life-threatening.
3 classes (AIDS) infection characteristic is following standard:
The T-cell dropped to be lower than 200 or
The disease that has had at least a following qualification--
The candidiasis of ο bronchus, trachea or lung
The candidiasis of ο esophagus
ο invasive cervical cancer
*
Outside the ο coccidioidomycosis, dispersivity or lung
Outside the ο cryptococcosis, lung
The ο cryptosporidiosis, (being longer than one month persistent period) of chronic enteral
ο cytomegalovirus disease (not comprising liver, spleen or lymph node)
ο cytomegalovirus retinitis (with visual deprivation)
The ο encephalopathy, HIV-is correlated with
ο herpes simplex: chronic ulcer (being longer than one month persistent period); Or bronchitis, pneumonia, or esophagitis
Outside the ο histoplasmosis, dispersivity or lung
The ο isosporiasis, (being longer than one month persistent period) of chronic enteral
The ο Kaposi sarcoma
ο Burkitt lymphomas (or suitable term)
ο lymphoblast lymphoma (or suitable term)
ο lymphoma former, brain
Outside ο bird-mycobacteria compound bacteria group (Mycobacterium avium complex) or the Kansasiin (M.kansasii), dispersivity or lung
The ο Mycobacterium tuberculosis, any site be (lung
*Or outside the lung)
The ο mycobacteria, other class or unidentified classification, outside dispersivity or the lung
The ο pneumocystis carinii pneumonia
The ο pneumonia, recurrence
*
The ο progressive multifocal leukoencephalopathy
The ο salmonella septicemia, recurrence
ο cerebral toxoplasmosis disease
The exhaustion syndrome that ο HIV brings out
Term " altogether administration (coadministration) " or " combined therapy " be meant simultaneously to two kinds of chemical compounds of patient's administration or compositions at least, so that each in two or more chemical compounds of given time point visible effective dose or valid density in patient's body.Although chemical compound of the present invention can be simultaneously to patient's administration altogether, this term comprises simultaneously or at two or more medicines of different time administrations, condition is chemical compound or the compositions in all the common administrations of visible valid density in subject of given time.More of the present invention preferred aspect, above-mentioned one or more diketone acid compounds, with herein in addition at least a other the inverase form of record be used for the treatment of HIV and infect with HAART (cocktail) combination administration altogether.The present invention especially preferred aspect, the common administration of chemical compound produces collaborative anti-HIV therapeutic activity.
Term herein " independently " is meant this variable (it uses independently), changes independently between using.
The present invention relates to chemical compound, its combination or the acceptable salt of its pharmacy of general formula I, be used to suppress hiv integrase, the treatment of prevention or treatment HIV infection and AIDS and ARC.Formula I chemical compound is as giving a definition:
Comprise its tautomer, regional isomer, and the acceptable salt of pharmacy, wherein two representative pyridone skeletons and R base as give a definition:
Two keto acids with following two pyridone skeletons;
R
1And R
2Be independently:
a)H,
B) C
1-6Alkyl,
C) C
1-6Fluoro-alkyl,
D) C
1-6Alkyl S (O)
nR, wherein n is selected from 0-2, and R is selected from C
1-3The phenyl of alkyl, phenyl and replacement, substituent group is selected from:
1) halogen,
2) hydroxyl,
3) C
1-3Alkyl,
4) C
1-3Alkoxyl,
5)CF
3,
E) have and be selected from 1~3 following substituent C
5-6Cycloalkyl:
1) halogen,
2) hydroxyl,
3) C
1-3Alkyl,
4) C
1-3Alkoxyl,
5)CF
3,
F) C
2-6Thiazolinyl,
G) C
1-6Alkyl CO
nR
a, wherein n is selected from 1 and 2, R
aBe selected from:
1) C
1-6Alkyl,
2)H,
H) phenyl,
I) be selected from the phenyl that following substituent group replaces by 1~3:
1) halogen,
2) hydroxyl,
3) C
1-3Alkyl,
4) C
1-3Alkoxyl,
5)CF
3,
J) benzyl,
K) have 1~3 and be selected from following substituent substituted benzyl:
1) halogen,
2) hydroxyl,
3) C
1-3Alkyl,
4) C
1-3Alkoxyl,
5)CF
3,
L) C that is replaced by phenyl
2-6Alkyl,
M) C that is replaced by phenyl
2-6Alkyl, this phenyl can be selected from following substituent group by 1~3 and replace:
1) halogen,
2) hydroxyl,
3) C
1-3Alkyl,
4) C
1-3Alkoxyl,
5)CF
3,
n)R
b,
O) by R
bThe C that replaces
1-6Alkyl,
Each R wherein
bBe 5 or 6 yuan of hetero-aromatic rings, it contains 1~2 hetero atom that is selected from oxygen, nitrogen and sulfur, and this ring can be selected from following substituent group replacement by 1~3 or not be substituted on carbon or nitrogen:
1) halogen,
2) hydroxyl,
3) C
1-3Alkyl,
4) C
1-3Alkoxyl,
5)CF
3,
R
3And R
4Be independently selected from:
a)H,
B) C
1-6Alkyl,
C) halogen,
D) hydroxyl,
E) thiophenyl (phenylthio),
F) have 1~3 and be selected from following substituent substituted thiophenyl:
1) halogen,
2) hydroxyl,
3) C
1-3Alkyl,
4) C
1-3Alkoxyl,
5)CF
3,
G) benzyl,
H) be selected from the substituted benzyl that following substituent group replaces by 1-3:
1) halogen,
2) hydroxyl,
3) C
1-3Alkyl,
4) C
1-3Alkoxyl,
5)CF
3, 。
R
5Be selected from:
A) CO
2R
c, R wherein
cBe selected from:
1) C
1-6Alkyl,
2)H,
3) sodium salt or the acceptable salt of other pharmacy,
B) P (O) (OR
d) (OR
e), R wherein
dAnd R
eCan be identical or different, and be selected from:
1) C
1-6Alkyl,
2)H,
3) sodium salt or the acceptable salt of other pharmacy.
Some embodiment preferred comprise following chemical compound: it is based on 2-pyridone (pyridin-2-ones) skeleton, and wherein said diketone acid moieties is in the 3-position of pyridone ring:
R wherein
1And R
2Be benzyl independently or on phenyl ring, be selected from fluorine, chlorine, C by 1~3
1-4Alkyl, C
2-4The benzyl that the substituent group of thiazolinyl, methoxyl group independently replaces;
R wherein
3Be H, C
1-3Alkyl, C
2-3Thiazolinyl, fluorine, chlorine, methoxyl group;
R wherein
4Be H, F, Cl, OH
R wherein
5Be CO
2H or P (O) are (OH)
2Or the acceptable salt of its pharmacy.
The present invention also comprises the pharmaceutical composition that is preferred for suppressing hiv integrase, and it comprises chemical compound of the present invention and pharmaceutically acceptable carrier, additive or the excipient of effective dose.Being used for the treatment of the pharmaceutical composition that infects HIV for example or treatment AIDS or ARC is also included among the present invention.The present invention also comprises and is used to suppress viral enzyme, the method for hiv integrase, and suppress the HIV growth or duplicate or treat the method that HIV infects or treat AIDS or ARC.In addition, the present invention relates to pharmaceutical composition, with combining form, comprise chemical compound of the present invention for the treatment of effective dose and the combination that is selected from the following medicine that is used for the treatment of AIDS for the treatment of effective dose: (i) AIDS or HIV antiviral agent, (ii) anti-infective, (iii) immunomodulator, (iv) other useful therapeutic agent comprises antibiotic and other antiviral agent.
For described pyridone skeleton and R
1, R
2, R
3And R
4, chemical compound of the present invention can have regional isomer, and these regional isomerism forms comprise in the present invention.Chemical compound can have geometric isomer, and these forms comprise in the present invention.
Also can there be tautomer in chemical compound of the present invention.Therefore, term " and tautomer " tautomer for example Ia and the Ib (as follows) that are used to describe formula I chemical compound.Chemical compound and tautomer thereof by the representative of name general formula I are appreciated that also to comprise tautomer Ia and Ib with regard to purpose of the present invention.Similarly,, be appreciated that with regard to purpose of the present invention, also comprise tautomer (I) and (Ib) for chemical compound (Ia).This is equally applicable to tautomer (Ib).
When relating to R
1, R
2, R
3, R
4And R
5Variable when in any formula I, occurring more than one time, the definition the when definition when at every turn occurring is independent of each other situation.Determine that except those structures the present invention also comprises the pyridone of regional isomerism.As long as in context, pyridone and variable be combined to form stable chemical compound, this makes up permission.
Chemical compound of the present invention is used to suppress hiv integrase, and prevention or treatment HIV infection and treatment are called the disease of AIDS.Treatment AIDS or inhibition or treatment HIV infect to be defined as and comprise that treating widely HIV infects disease: AIDS, ARC with actual or contact HIV potentially (for example by blood transfusion, body fluid exchange, pin puncture, the blood samples of patients of contact infection during medicine (medical) or dental operation, and alternate manner).
The present invention also comprises other application.For example, chemical compound of the present invention is used to prepare and finish the screening experiment of antiviral compound, comprises isolated viral enzyme mutant body and further understands this enzyme, hiv integrase.
The present invention also provides the chemical compound of structural formula (I) to be used for suppressing hiv integrase and to be used for the treatment of AIDS or the purposes of ARC pharmaceutical composition in preparation.
Can be with " known pharmacy is acceptable " salt form administration chemical compound of the present invention.Described " known pharmacy is acceptable " salt form is meant and comprises for example acetate of the acceptable salt of all pharmacy; lactobionate; benzene sulfonate; laruate; benzoate; malate; bicarbonate; maleate; disulfate; mandelate; biatrate; mesylate; borate; MB; bromide; methyl nitrate (methylnitrate); Ca-EDTA; camsilate; mucate; carbonate; naphthalene sulfonate; chloride; nitrate; Clavulanate; N-methyl glucoside amine; citrate; ammonium salt; dihydrochloride; oleate; edetate; oxalates; ethanedisulphonate; pamoate; propionic ester dodecyl sulphate (estolate); palmitate; esilate; fumarate; phosphate; hydrophosphate; gluceptate; Polygalacturonate; gluconate; Salicylate; glutamate, Glu; stearate; glycolyl arsanilic acid salt (glycollylarsanilate); sulfate; hexylresorcin salt (hexylresorcinate); basic acetate; breathe out amine salt (hydrabamine); succinate; hydrobromate; tannate; hydrochloride; tartrate; Hydroxynaphthoate; teoclate (teoclate); iodide; toluene fulfonate; different thiosulfate; triethiodide; lactate; panoate; valerate and other can change that dissolubility or hydrolysising characteristic maybe can be used for continuing discharging or the salt of prodrug formulation as dosage form.The acceptable salt of pharmacy of the present invention comprises having for example those of sodium, potassium, calcium, lithium, magnesium, zinc of counter ion counterionsl gegenions, and from alkali for example ammonium, ethylenediamine, N-methyl-glutamine, lysine, arginine, ornithine, choline, N, N '-dibenzyl-ethylenediamin, chloroprocaine (chloroprocaine), diethanolamine, procaine, N-benzyl-1-phenylethylamine, diethylamine, piperazine, three (hydroxymethyl) aminomethane, and those of Tetramethylammonium hydroxide.
Similarly, exist carboxylic acid (COOH) or under the situation of alcohol groups, can use the acceptable ester of pharmacy, acetate for example, maleate, pivaloyl oxygen methyl ester (pivaloyloxymethyl) and other, more preferably C
1-C
20Become known for improving dissolubility or hydrolysis properties in ester and this area as those esters that continue release or prodrug formulation.The acceptable ester of pharmacy also can comprise and wherein has phosphonate group [PO (OH)
2] situation.Two one phosphonic acids that are connected on the pyridone skeleton are also included among the present invention.
The chemical compound of the present invention of treatment effective dose can be oral to the patient, parenteral, suction spraying or rectum be with the dosage unit preparations form administration, and described dosage unit preparations contains pharmaceutically acceptable carrier, adjuvant and solvent (comprising the nano-particle drug release mode).Term " pharmacy is acceptable " is meant that carrier, diluent or other additive must be compatible with other composition in the preparation, and harmless for patient or receiver.Pharmaceutical composition can be oral administration suspensoid or tablet, nasal spray and injectable formulation (injection aqueous or oil-based suspension or suppository).This Therapeutic Method comprises in the present invention.Used administering mode (, quick-release tablet oral with solution or suspension, nose aerosol or inhalant, injection or suspension or with the suppository rectally) relates in the known technology of field of pharmaceutical preparations.
Chemical compound of the present invention can with preferred dosage form (for example tablet) and preferably with the divided dose of about 0.1~200mg/kg body weight to the human oral administration.Concrete dosage level and administration frequency for any concrete patient can change, and this depends on following various factors, comprise: the duration of compound activity, chemical compound metabolism and effect, patient age, body weight, health status, sex, diet, administering mode and time, excretion rate, drug regimen, concrete disease serious degree, and patient's situation of receiving treatment.
The present invention also comprise hiv integrase inhibitor formula I chemical compound and one or more other therapeutic agents for example AIDS antiviral agent, other antiviral agent, immunomodulator, anti-infective, antibiotic, vaccine or as the treatment of other therapeutic agent combination of describing in addition herein effectively make up.Some examples are as follows:
Antiviral agent, anti-infective, immunomodulator, opportunistic infection medicine, be used for its of AIDS
Its related drugs
Medicine name
Manufacturer
Therapeutic use
097 Hoechst/Bayer HIV infects, AIDS,
(NNRT suppresses ARC
Agent)
Amprenivir Glaxo Wellcome HIV infects, AIDS,
141W94, (protease suppresses GW141 ARC
Agent)
Abacavir Glaxo Wellcome HIV infects, AIDS,
(1592U89) ARC (RT inhibitor)
GW?1592
Acemannan Carrington Labs ARC
(Irving,TX)
Aciclovir Burroughs Wellcome HIV infects, AIDS,
ARC makes up with AZT
AD-439 Tanox Biosystems HIV infects, AIDS,
ARC
AD-519 Tanox Biosystems HIV infects, AIDS,
ARC
Two volts of adefovirdipivoxil Gilead Sciences HIV infects
Ester Ethigen (Los ARC, PGL HIV sun
AL-721 Angeles, CA) property, AIDS
Interferon-alpha Glaxo Wellcome Kaposi sarcoma, HIV,
Make up with the w/ azidothymidine AZT
Ansamycin Adria Laboratories ARC
LM?427 (Dublin,OH)
Erbamont(Stamford,
CT)
In and the unsettled Advanced Biotherapy of pH AIDS, ARC
The anti-Concepts of the unusual interferon of α (Rockville,
Body MD)
AR 177 Aronex Pharm HIV infect, AIDS,
ARC
β-fluoro-ddA National Cancer AIDS-relevant disease
Institute
BMS-232623 Bristol-Myers HIV infects, AIDS,
(CGP-73547) (protease suppresses Squibb/Novartis ARC
Agent)
BMS-234475 Bristol-Myers HIV infects, AIDS,
(CGP-61755) (protease suppresses Squibb/Novartis ARC
Agent)
CI-1012 Warner-Lambert HIV-1 infects
Cidofovir Gilead Science CMV retinitis, bleb
Rash, human papillomavirus
Sulfogel Polysaccharide A JI Pharma USA HIV infects
(Curdlan?sulfate)
Cytomegalovirus M edImmune CMV retinitis
Immunoglobulin
Cymevene Syntex vision threatens (Sight
Ganciclovir threatening) CMV
Periphery CMV
Retinitis
DdI Bristol-Myers Squibb HIV infects, AIDS,
Didanosine ARC; With AZT/d4T
Combination
DMP-450 AVID (Camden, NJ) HIV infects, AIDS,
(protease suppresses ARC
Agent)
Efavirenz DuPont Merck HIV infects, AIDS,
(DMP-266) (non-nucleoside RT presses down ARC
Preparation
EL10 Elan Corp, PLC HIV infects
(Gainesville,GA)
Famciclovir Smith Kline herpes zoster, herpes simplex
FTC Emory University HIV infects, AIDS,
(reverse transcriptase suppresses ARC
Agent)
GS 840 Gilead HIV infect, AIDS,
(reverse transcriptase suppresses ARC
Agent)
HBY097 Hoechst Marion HIV infects, AIDS,
(non-nucleoside reverses Roussel ARC
Transcriptase inhibitors)
Hypericin VIMRxPharm. HIV infects, AIDS,
ARC
Recombined human interferon-Triton Biosciences AIDS, KaposiShi meat
(Almeda, CA) tumor, ARC
Alferon N Interferon Scienes ARC, AIDS
Indinavir Merck HIV infects, AIDS,
ARC, asymptomatic HIV
Positive; With
The AZT/ddI/ddC combination
ISIS-2922 ISIS Pharmaceuticals CMV retinitis
KNI-272 Natl.Cancer Institute HIV-relevant disease
Lamivudine, 3TC Glaxo Wellcome HIV infects, AIDS,
(reverse transcriptase suppresses ARC
Agent); Also has AZT
Lobucavir Bristol-Myers Squibb cmv infection
Nelfinavir Agouron HIV infects, AIDS,
(protease suppresses Pharmaceuticals ARC
Agent)
Nevirapine Boeheringer HIV infects, AIDS,
Ingleheim ARC (RT inhibitor)
Novapren Novaferon Labs, the Inc. hiv inhibitor
(Akron,OH)
Peptide T Peninsula Labs AIDS
The octapeptide sequence (Belmont, CA)
Phosphonoformic acid trisodium Astra Pharm. CVV retinitis, HIV
Products, Inc. infects, other CMV
PNU-140690 Pharmacia Upjohn HIV infects, AIDS,
(protease suppresses ARC
Agent)
Probucol Vyrex HIV infects, AIDS
RBC-CD4 Sheffield Med.Tech HIV infects, AIDS,
(Houston,TX) ARC
Ritonavir Abbott HIV infects, AIDS,
(protease suppresses ARC
Agent)
Saquinavir Hoffmann-LaRoche HIV infects, AIDS,
(protease suppresses ARC
Agent)
Stavudine; D4T Bristol-Myers Squibb HIV infects, AIDS,
Two dehydrogenation deoxyribosylthymine ARC
Valaciclovir Glaxo Wellcome Genital HSV and
Cmv infection
Ribavirin Viratek/ICN (the asymptomatic HIV sun of Costa
Mesa, CA) property, LAS, ARC
VX-478 Vertex HIV infects, AIDS,
ARC
Zalcitabine Hoffmann-LaRoche uses the HIV sense of AZT
Dye AIDS, ARC
Zidovudine; AZT Glaxo Wellcome HIV infects, AIDS,
ARC, the Kaposi sarcoma,
With other therapeutic combination
Tenofovir diisoproxil Gilead HIV infects, AIDS,
Fumarate
(RT inhibitor)
Combivir
GSK HIV infects, AIDS,
(RT inhibitor)
Abacavir succinate (or GSK HIV infection, AIDS,
Match is advanced
(reverse transcriptase inhibitors)
Viral fusion inhibitor
AS-101 Wyeth-Ayerst AIDS
Bropirimine Pharmacia Upjohn AIDS in late period
Acemannan Carrington Labs, Inc. AIDS, ARC
(Irving,TX)
CL246,738 American Cyanamid AIDS, KaposiShi meat
Lederle Labs tumor
EL10 Elan Corp, PLC HIV infects
(Gainesville,GA)
FP-21399 Fuki Immuno CD4+ cell fusion
The Blocks HIV of PHARM
IFN-Genentech ARC organizes with w/TNF
Close
Granulocyte Genetics Institute AIDS
Macrophage colony stimulates because of Sandoz
Son
Granulocyte Hoeschst-Roussel AIDS
Macrophage colony stimulates because of Immunex
Son
Granulocyte Schering-Plough AIDS organizes with w/AZT
Macrophage colony stimulates because of closing
Son
HIV core granule immunity Rorer seropositivity HIV
Promoter
IL-2 Cetus AIDS organizes with w/AZT
Interleukin-2 closes
IL-2 Hoffman-LaRoche AIDS,ARC,HIV,
Interleukin-2 Immunex and w/AZT combination
IL-2 Chiron AIDS, the cd4 cell meter
The interleukin-2 number increases
(aldeslukin)
The intravenous Cutter Biological of immunoglobulin infant acquired immunity
(Immune Globulin (Berkeley, CA) deficit syndrome (Pediatric
Intravenous) AIDS), organize with w/AZT
(people) closes
IMREG-1 Imreg (New Orleans, AIDS, KaposiShi meat
LA) tumor, ARC, PGL
IMREG-2 Imreg (New Orleans, AIDS, KaposiShi meat
The LA tumor, ARC, PGL
Imuthiol diethyl dimercapto Merieux Institute AIDS, ARC
Carbaminate (Imuthiol
Diethyl Dithio
Carbamate)
α-2 interferon Schering Plough Kaposi sarcoma
w/AZT,AIDS
Met-enkephalin TNI Pharmaceutical AIDS, ARC
(Chicago,IL)
MTP-PE Ciba-Geigy Corp. Kaposi sarcoma
Muramyl-tripeptide
Granulocyte Amgen AIDS organizes with w/AZT
Colony stimulating factor closes
Remune Immune Response immunization therapy
Corp.
rCD4 Genentech AIDS,ARC
Solvable people recombinates
CD4-IgG
rCD4-IgG?Hybrids AIDS,ARC
The solvable people CD4 Biogen AIDS that recombinates, ARC
Interferon-ALPHA 2a Hoffman-LaRoche Kaposi sarcoma,
AIDS, AR, with
The w/AZT combination
SK﹠amp; F1-6528 Smith Kline HIV infects
Solvable T4
Thymopentin Immunobiology HIV infects
Research Institute
(Annandale,NJ)
Tumor necrosis factor (TNF) Genentech ARC is with the w/ IFN-
Combination
AK602 Kumamoto University HIV infects and (to enter and merge
The Japan inhibitor)
Alovudine Medivir, UK Ltd. HIV infects (nucleoside
The RT inhibitor)
Amdoxovir RFS Pharma, LLC HIV and HBV infect
Treatment (nucleoside RT inhibitor)
AMD070 AnorMED, Inc. HIV infect and (to enter and melt
Close (entry and fusion)
Inhibitor)
(protease presses down in Atazanavir (Reyataz) Bristol-Myers Squibb HIV infection
Preparation)
AVX754 (apricitabine) Avexa Ltd. HIV infects (nucleoside
The RT inhibitor
Bevirimat Panacos HIV infects (the ripe inhibition
The Pharmaceuticals agent)
BI-201 BioInvent HIV infection (gene therapy,
Blocking-up HIV tat gene).
BMS-378806 Bristol-Myers Squibb HIV infects (input inhibition
Agent)
BMS-488043 Bristol-Myers Squibb HIV infects and (to enter and melt
Close inhibitor)
(intergrase presses down in BMS-707035 Bristol-Myers Squibb HIV infection
Preparation)
C31G Cellegy HIV infects and other property biography
Pharmaceuticals, Inc broadcast disease (STDs)
Carbopol ReProtect, LLC HIV spreads through sex intercourse
(Carbopol)974P
Calanolide A Sarawak MediChem HIV infects (non-nucleoside RT
Pharmaceuticals, the Inc. inhibitor)
Carrageenin (Carrageenan) FMC Biopolymer HIV microbicide
Sulfate cellulose Polydex prevention HIV infects and it
Pharmaceuticals, its sexually transmitted disease (STD) of Ltd.
The property biography that blue algae antiviral protein-N Cellegy prevention HIV infects
(Cyanovirin-N) Pharmaceuticals, Inc. broadcasts disease
Darunavir Tibotec HIV infects (with Li Tuona
Wei administration altogether)
Delavirdine Pfizer HIV infects (non-nucleoside RT
Inhibitor)
Dextran sulfate Ueno Fine Chemicals prevention HIV infects
Industry,Ltd.
(Videx Bristol-Myers Squibb HIV infects (nucleoside RT to didanosine
(Videx), inhibitor Videx EC))
Efavirenz Bristol-Myers Squibb HIV infects (non-nucleoside RT
Inhibitor)
Elvucitabine Achillion HIV infects (nucleoside RT
The Pharmaceuticals inhibitor)
Emtricitabine Gilead Sciences HIV infects (nucleoside RT
Inhibitor)
(protease presses down in fosamprenavir (Lexiva) GlaxoSmithKline HIV infection
Preparation)
Fozivudine tidoxil Heidelberg Pharma HIV infects and (to enter and melt
Close inhibitor)
(intergrase presses down in GS 9137 Gilead Sciences HIV infection
Preparation)
GSK-873,140 GlaxoSmithKline HIV infect and (to enter and melt
(aplaviroc) close inhibitor)
(intergrase presses down in GSK-364735 GlaxoSmithKline HIV infection
Preparation)
(protease presses down in GW640385 GlaxoSmithKline HIV infection
(brecanavir) preparation)
HG0004 Human Genome HIV infects and (to enter and melt
Sciences closes inhibitor)
HGTV43 Enzo Therapeutics HIV infects (antisense drug)
Hydroxy ethyl cellulose Union Carbide prevention HIV spreads through sex intercourse
INCB9471 Incyte Corporation HIV infects and (to enter and melt
Close inhibitor)
KP-1461 Koronis HIV infects (nucleoside RT
The Pharmaceuticals inhibitor)
(protease presses down in Lopinavir Abbott Laboratories HIV infection
Preparation)
Mifepristone Viral Genomix HIV infection (gene therapy,
(VGX410 intervenes with vpr)
RU486)
(intergrase presses down in MK-0518 Merck HIV infection
Preparation)
The treatment of PA-457 (bevirimat) Panacos HIV
Pharmaceuticals, Inc. (ripe inhibitor)
Poly (I)-Poly (C12U) Hemispherx biological response modifier
(polyinosini) Biopharma, Inc.
(protease presses down in PPL-100 Merck HIV infection
Preparation)
PRO 140 Progenics HIV infect and (to enter and melt
Pharmaceuticals, Inc. closes inhibitor)
PRO 542 Progenics HIV infect and (to enter and melt
Pharmaceuticals, Inc. closes inhibitor)
PRO 2000 Indevus microbicide
Pharmaceuticals,Inc.
Racivir Pharmasset, Inc. HIV infects (nucleoside RT
Inhibitor)
SCH-D (vicriviroc) Schering-Plough Corp HIV infects and (to enter and melt
Close inhibitor)
SP01A Samaritan HIV infects and (to enter and melt
Pharmaceuticals closes inhibitor)
SPL7013 Starpharma microbicide
TAK-652 Takeda HIV infects and (to enter and melt
Close inhibitor)
(protease presses down in tipranavir (Aptivus) Boehringer Ingelheim HIV infection
The Pharmaceuticals preparation)
TNX-355 Tanox, Inc. HIV infect and (to enter and melt
Close inhibitor)
TMC125 (etravirine) Tibotec HIV infects (non-nucleoside RT
Inhibitor)
UC-781 Cellegy microbicide
Pharmaceuticals,Inc
UK-427,857 Pfizer HIV infect and (to enter and melt
(Maraviroc) close inhibitor)
Sending out during valproic acid Abbott treatment HIV infects
Do
VRX496 VIRxSYS gene therapy
Zalcitabine (Hivid) Roche HIV infects (nucleoside RT
Inhibitor)
Valganciclovir (Valcyte) Roche antiviral (among the AIDS
The CMV retinitis)
Clindamycin and primaquine Pharmacia Upjohn PCP
Fluconazol Pfizer cryptococcal meningitis is read
Pearl bacterium disease
Lozenge Squibb Corp. prevents oral candidiasis
Nystatin lozenge
Eflornithine hydrochloride injection Merrell Dow PCP
Agent (Ornidyl)
Eflornithine
(Eflornithine)
Hydroxyethylsulfonic acid. pentamidine LyphoMed PCP treatment
(IM?&?IV) (Rosemont,IL)
The trimethoprim antibacterial
Trimethoprim/sulfanilamide antibacterial
Piritrexim Burroughs Wellcome PCP treatment
Hydroxyethylsulfonic acid. pentamidine Fisons Corporation PCP prevention
Spiramycin Rhone-Poulenc conceals the spore protozoal diarrhea
Intraconazole-R51211 Janssen Pharm histoplasmosis; Latent ball
Bacterium property meningitis
Trimetrexate Warner-Lambert PCP
Daunorubicin NeXstar, Sequus Karposi sarcoma
It is relevant with the w/AZT treatment that recombinant, human red blood cell are given birth to Ortho Pharm.Corp.
The serious anemia of Cheng Su
Recombinant, human growth hormone Serono AIDS-is relevant becomes thin,
Cachexia
Megestrol acetate Bristol-Myers Squibb is relevant with w/AIDS
The treatment of loss of appetite
Testosterone Alza, what Smith Kline AIDS-was relevant becomes thin
Diarrhoea and suction among the nutrition Norwich Eaton AIDS in the intestines and stomach fully
Pharmaceuticals receives bad
Aldesleukin Chiron Corp biological response modifier
(Aldesleukin) (A Dibai
Plain (Proleukin) is situated between)
Amphotericin B (Abelecet, Pfizer, Bristol-Myers antifungal agent
AM Bison (two Squibb
The property mycin B liposome injection
Agent (AmBisome)),
Amphocin, amphotericin B
Injectable powder (Amphotec),
Fungizone)
Azithromycin (Zithromax) Pfizer antibacterial, antibiotic
Calcium hydroxyapatite Bioform Medical, Inc.Dermal filler
(Radiesse
Doxorubicin (liposome) (salt Ortho Biotech, Alza antineoplastic agent
Acid Mycocet Corporation
(Doxil))
Dronabinol (Marinol) Unimed Antiemetics
Pharmaceuticals,Inc.
Entecavir (Baraclude) Bristol-Myers Squibb antiviral
(erythrocyte is given birth to Ortho Biotech anemia to Epoetin Alfa
Become hormone injection (Epogen),
Procrit)
Etoposide (Etopophos (phosphorus Pfizer, Bristol-Myers antineoplastic agent
Hydrochlorate), Toposar, all complete Squibb
The scholar)
Fluconazol (Fluconazole) Pfizer antifungal agent
Interferon (Recombinant Interferon Roche, Schering biological response modifier
(2b), Rodferon-A (2a)-Plough
Isoniazid (Isoniazid) Sandoz, Hoffmann La-is antimycobacterial
(Nydrazid) Roche
Itraconazole (Sporanox) Ortho Biotech, the Janssen antifungal agent
Pharmaceutica
(Megace, Bristol-Myers Squibb is anticachectic for megestrol
Megace?ES)
Paclitaxel (Onxol, taxol) Bristol-Myers Squibb, antineoplastic agent
IVAX?Pharmaceuticals
Peg interferon Roche, the Schering antiviral
(Peginterferon?α-2)?-Plough
(PEG-Intron(2b),
Pegasys(2a))
Pentamidine (pentamidine aerosol American antiprotozoal drug
Agent (Nebupent)) Pharmaceutical
Partners,Fujisawa
Health?Care,Inc.
Poly--L-lactic acid (Sculptra) Dermik Laboratories Dermal Filler
Rifabutin (Mycobutin) Pharmacia Corporation is antimycobacterial
(Rifadin, Aventis is antimycobacterial for rifampicin
Rimactane) Pharmaceuticals
The synthetic human growth hormone of growth hormone (Somatropin) Pharmacia
Corporation,Serono?Inc
Sulfamethoxazole/methoxy benzyl Alpha care Inc, the Women antibacterial
Pyridine (bactrim First Health Care, King
(Bactrim),Septra) Pharmaceuticals
(Serostim)
Testosterone (Androderm, Pfizer Inc, Unimed androgens
Androgel, the Depo-testosterone) Pharmaceuticals, Inc.,
Alza Corporation,
Watson?Laboratories
Trimetrexate (Neutrexin) United States antiprotozoal drug
Bioscience Inc,
Medimmune,Inc.
The combination of chemical compound of the present invention and AIDS antiviral agent (comprising the antiviral agent based on the anti-HIV intergrase), other antiviral agent, immunomodulator, anti-infective, antibiotic, vaccine or other therapeutic agent is not limited to listed those of table, but comprise, basically with any combination that is used for the treatment of HIV infection or treatment AIDS or any pharmaceutical composition of ARC.Preferably be combined as chemical compound of the present invention and protease inhibitor (indinavir for example, nelfinavir, ritonavir, Saquinavir and other), reverse transcriptase inhibitors [nucleoside (AZT for example, 3TC, ddC, ddI, d4T, Abacavir and other and/or non-nucleoside (efavirenz for example, nevirapine and other), or the combination of two or more these inhibitor (seeing the above table) is simultaneously or alternating treatment.Quote combination the related application of several typical example be: EPO 0,484,071, U.S.5,413,999, WO 9962513.
In this combination, chemical compound of the present invention and other activating agent can individually dosed or administrations (concurrently administered) simultaneously.In addition, a kind of administration of component can be before other component, simultaneously or administration in succession.
Chemical compound of the present invention and AIDS antiviral agent (as mentioned above, other addresses as described below to some extent), it is listed that the combination of other antiviral agent, immunomodulator, anti-infective, antibiotic, vaccine, other therapeutic agent is not limited to table, but comprise, basically with any combination that is used for the treatment of HIV infection or treatment AIDS or any pharmaceutical composition of ARC.Preferably be combined as chemical compound of the present invention and protease inhibitor (indinavir especially for example, nelfinavir, ritonavir, Saquinavir), reverse transcriptase inhibitors [nucleoside (AZT for example, 3TC, ddC, ddI, d4T, Abacavir and other and/or non-nucleoside (efavirenz for example, nevirapine and other), or the combination of two or more these inhibitor (seeing the above table) is simultaneously or alternating treatment.Quote combination the related application of several typical example be: EPO 0,484,071, U.S.5,413,999, WO 9962513.
In this combination of chemical compound of the present invention and other activating agent, for example as described below, can individually dosed or administration simultaneously with effective dose.In addition, a kind of administration of component can be before other component, simultaneously or administration in succession.
Be effective to HIV or for the indication/disease of treatment HIV or HIV secondary (comprising the disease of AIDS/ARC and secondary or morbid state for example Kaposi sarcoma, hepatitis B virus infection etc.) the favourable medicine or the following example of bioactivator, its can with chemical compound combination of the present invention treatment HIV to be provided to infect or the pharmaceutical composition and the method for other secondary disease or morbid state.In the time of in being included in pharmaceutical composition or Therapeutic Method, these medicines or bioactivator exist to alleviate the disease of this chemical compound of administration or the effective dose of morbid state.
(-) beta-dioxolane (Dioxolane)-G; DXG;
(-) β-arctigenin; Arctigenin (Arctigenin);
(-)-Carbovir; (-)-C-D4G; (-)-Carbovir;
(-)-β-D-2,6-diaminopurine dioxolanes; Amdoxovir; DAPD; APD
(+)-2 '-deoxidation-3 '-oxa--4 '-the sulfo-cytidine; DOTC (+)
(+)-2 '-deoxidation-3 '-oxa--4 '-sulfo--5-fluorine cytidine; DOTFC (+)
(+/-)-Cyclobut-G; A-69992; (+/-)-Lobucavir; C-Oxt-G; Cyclobut-G; C-Oxetanocin-G
·(R)-2QuinCOAsnPhe[CHOHCH2]PipCONHtBu
(R)-3,6-diamino-N-(amino methyl) caproamide; Bellenamine
(R)-PMPA; (R)-9-(2-phosphonium mesitoyl methoxy propyl group) adenine; PMPA-(R); Tenofovir
·(R)-PMPDAP;PMPDAP-(R)
(S)-PMPA; (S)-9-(2-phosphonium mesitoyl methoxy propyl group) adenine; PMPA (S)
(S)-9-(2-phosphonium mesitoyl methoxy propyl group) adenine; (S)-PMPA
α-APA; R89439; Loviride
α-APA derivant; R87232
α-APA derivant; R88703
α-APA enantiomer; R90385
·α-L-AZT;AZT-α-L
α-L-DXC; α-L-dioxolanes-C; DXC-α-L-
·α-L-FTC;FTC-α-L-
α-single methyl fluoride dehydrogenation ornithine methyl ester; MFMOME
1,1 '-Celogen Az; ADA; Azodicarboamide
1-(11-octyl group amino-10-hydroxyl undecyl)-3, the 7-dimethyl xanthine; CT-2576
1-(2 ', 3 '-dideoxy-2 '-fluoro-beta-D-threo form-penta furyl glycosyl) cytosine; Ro 31-6840
1-(2 '-fluoro-2 ', 3 '-dideoxy-B-B-erythro-penta furyl glycosyl) thymus pyrimidine; 2 ' FddT
1-(2OHPr)-4-is substituted (Substit)-piperazine, the thienyl carbamate derivatives
1-(2OHPr)-4-is substituted-piperazine, the thienyl carbamate derivatives
1-(2OHPr)-4-is substituted-piperazine, the thienyl carbamate derivatives
1-(2OHPr)-4-is substituted-piperazine, the thienyl carbamate derivatives
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(3-aminomethyl phenyl) sulfenyl) thymus pyrimidine; HEPT-M
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(thiophenyl)-2-thio-thymine; HEPT-S
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(thiophenyl) thymus pyrimidine; HEPT
1-deoxidation nojirimycin; Deoxidation nojirimycin (Deoxynojirimycin)
141W94; VX-478; Amprenavir;
Approval
The 1592U89 succinate; Abacavir succinate;
Approval
1-amino oxygen base ethamine; AEA
1-methoxyl group oxalyl group-3, the 5-dicaffeoylquinic acid; 1-MO-3,5-DCQA; The dicaffeoylquinic acid derivant
1OH-2 (Cbz-Tle) 3PhPr[14] adjacent formic acid (paracyclophane) derivant of two Parylenes
1OH-2 (Cbz-ValNH) 3PhPr[13] metacyclophane (metacyclophane) derivant
1OH-2 (Cbz-ValNH) 3PhPr[13] the adjacent formic acid derivates of two Parylenes
1OH-2 (Cbz-ValNH) 3PhPr[14] the adjacent formic acid derivates of two Parylenes
1OH-2 (Cbz-ValNH) 3PhPr[17] the adjacent formic acid derivates of two Parylenes
12-deoxidation phorbol-13-(3E, 5E-decadinene acid esters (decadienoate)); The phorbol derivant
16. α-bromine epiandrosterone (Bromoepiandrosterone); Epi-Br; Inactivin; HE 2000; HE2000; PPB2; The DHEA derivant
1-β-D-arabinofuranosyl adenin glycosyl (arabinofuranosyl)-5-(2-bromo vinyl) uracil; BV-ara-U; BVaraU; BV ara-U; Sorivudine; SQ-32756; Bravavir; Brovavir; Usevir; YN-72; Bromo vinyl araU; BVAU
2 ', 3 '-two dehydrogenations-3 '-deoxycytidine; D4C
2 ', 3 '-dideoxy two dehydrogenation guanosines; D4G
2 ', 3 '-two dehydrogenations-3 '-deoxyribosylthymine; D4T; Stavudine;
Approval
2 ', 3 '-dideoxy-3 '-fluoro-4-sulfo-breast glycosides; 3 '-F-4-Thio-ddT
2 ', 3 '-dideoxy-3 '-fluoro-5-broxuridine; FddBrU
2 ', 3 '-dideoxy-3 '-fluoro-5-5-chloro-5-deoxyarabinosylcytosine; 3 '-F-5-Cl-ddC
2 ', 3 '-dideoxy-3 '-fluoro-5-chloriduria glycosides; 935U83; 5-chloro-2 ', 3 '-dideoxy-3 '-floxuridine; FddClU; Raluridine,
2 ', 3 '-dideoxy-5-ethyl cytidine; 5-Et-ddC
2 ', 3 '-DIDEOXYADENOSINE; D2A; DdAdo; DdA
2 ', 3 '-dideoxy two dehydrogenation adenosines; D4A
2 ', 3 '-the dideoxy guanosine; D2G; DdG
2 ', 3 '-dideoxy-3 '-hydroxymethyl cytidine; 3 '-hydroxymethyl-ddC; BEA-005
2,5 '-dehydration-3 '-azido-2 ', 3 '-di-deoxyuridine; AZU-2,5 '-dehydration
2,5 '-dehydration-3 '-azido-3 '-deoxyribosylthymine; AZT-2,5 '-dehydration
·2′,5′diSilySpiroT;TSAO-T
·2′,5′diSilySpiroT;TSAO-me^3T
2,6-diaminourea-2 ', 3 '-dideoxy purine-9-ribofuranoside (ribofuranoside); DdDAPR; DAPDDR; 2,6-diaminourea-ddP
2,6-diaminopurine-2 ', 3 '-dideoxy two dehydrogenation nucleoside; DdeDAPR
2,6-diaminopurine-3 '-fluoro-2 ', 3 '-di-deoxynucleoside; 3 '-F-ddDAPR
2-aminobenzyl statine (statine) valyl Cbz derivant; The statine derivant
2-glycine amide-5-chlorphenyl 2-pyrrolyl ketone; GCPK
·[2-PyridCH2NCH3CO-Val-NHCH(Bz)]CHOHCHOH;A-77003
2 '-azido-2 ', 3 '-DIDEOXYADENOSINE; 9-(2 '-azido-2 ', 3 '-dideoxy-β-D-erythro penta furyl glycosyl (pentofuranosyl)) adenine; 2 '-N3ddA
2 '-FddA (B-D-threo form); F-ddA; '-F-dd-ara-A; 9-(2 '-fluoro-2 ', 3 '-dideoxy-B-D-threo form penta furyl glycosyl) adenine; Lodensine
2 '-N3ddA (B-D-threo form); 9-(2 '-azido-2 ', 3 '-dideoxy-β-threo form penta furyl glycosyl) adenine
·2-NaphCOAsnPhe[CHOHCH2]Pro-OtBu
2-nitrobenzophenone phenylsulfone; NPPS
3-(3-oxo-1-acrylic)-3 '-azido-3 '-deoxyribosylthymine; 3-(3-oxo-1-acrylic) AZT
3-(phenyl sulfonyl)-indole derivatives; L-737,126
3,5-DCQA; 3, the 5-dicaffeoylquinic acid; Dicaffeoylquinic acid
3 '-azido-2 ', 3 '-dideoxy-5-[(cyano methyl) the oxygen base] uridnine; 3 '-N3-5-cyano methyl oxygen base-ddU
3 '-azido-2 ', 3 '-dideoxy-5-aminouridine; 3 '-N3-5-NH2-ddU
3 '-azido-2 ', 3 '-assorted (deaza) uridnine of dideoxy-5-azepine-6-denitrification, 3 '-the C-analog of N3-ddU
3 '-azido-2 ', 3 '-dideoxy-5-broxuridine; 3 '-N3-5-Br-ddU; AZddBrU
3 '-azido-2 ', 3 '-dideoxy-5-5-chloro-5-deoxyarabinosylcytosine; 3 '-Az-5-Cl-ddC
3 '-azido-2 ', 3 '-dideoxy-5-dimethylamino uridnine; 3 '-N3-5-NMe2-ddU
3 '-azido-2 ', 3 '-dideoxy-5-ethyl uridnine; 3 '-N3-5-EtddU; CS-85; AZddEtU
3 '-azido-2 ', 3 '-dideoxy-5-fluorine cytidine; 3 '-N3-5-F-ddC
3 '-azido-2 ', 3 '-dideoxy-5-floxuridine; AZddFU
3 '-azido-2 ', 3 '-dideoxy-5-hydroxyuridine; 3 '-N3-5-OH-ddU
3 '-azido-2 ', 3 '-dideoxy-5-iodo uridnine; 3 '-N3-5-I-ddU; AZddIU
3 '-azido-2 ', 3 '-dideoxy-5-methylamino uridnine; 3 '-N3-5-NHMe-ddU
3 '-azido-2 ', 3 '-dideoxy-5-methylcytidine; CS-92; 3 '-N3-5-Me-ddC
3 '-azido-2 ', 3 '-dideoxy-5-thiocyano uridnine; 3 '-N3-5-SCN-ddU
3 '-azido-2 ', 3 '-dideoxy-5-trifluoromethyl uridnine; 3 '-N3-5-CF3-ddU
3 '-azido-2 ', 3 '-zalcitabine; CS-91; 3 '-N3-ddC
3 '-azido-2 ', 3 '-the dideoxy guanosine; AZG; 3 '-N3ddG
3 '-azido-2 ', 3 '-dideoxy-N4--5-dimethyl cytidine; 3 '-N3-N4-5-diMe-ddC
3 '-azido-2 ', 3 '-dideoxy-N4-OH-5-methylcytidine; 3 '-N3-N4-OH-5-Me-ddC
3 '-azido-2 ', 3 '-di-deoxyuridine; CS-87; 3 '-N3ddU; AZdU; Uravidine
3 '-azido-3 '-deoxidation-6-azathymidine; 3 ' AZ-6AzaT
3-azido-3 '-deoxyribosylthymine base (thymidilyl)-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-adenylic acid;
AZT-P-ddA
3 '-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-adenylic acid, 2-cyano ethyl ester;
AZT-P(CyE)-ddA
3 '-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-inosinic acid; AZT-P-ddI
3 '-azido-3 '-deoxyribosylthymine-5 '-(butyl methoxyl group valine (valinyl)) phosphate ester;
5′MeOValPO3(Bu)AZT
3 '-azido-5-chloro-2 ', 3 '-di-deoxyuridine; AzddClUrd; AzddClU
3 '-deoxyribosylthymine; DdT
3 '-FddA (B-D-erythro); 9-(3 '-fluoro-2 ', 3 '-dideoxy-B-D-erythro penta furyl glycosyl) adenine
3 '-FddC; 3 '-fluoro-2 ', 3 '-zalcitabine
3 '-FddG; 3 '-fluoro-2 ', 3 '-the dideoxy guanosine
3 '-FddT; Alovudine; FddT; FddThD; 3 '-FLT; FLT
3 '-FddU; 3 '-fluoro-2 ', 3 '-di-deoxyuridine,
3 '-fluoro-2 ', 3 '-dideoxy-5-iodo uridnine; FddIU
3 '-N3-ddA; 9-(3 '-azido-2 ', 3 '-dideoxy-B-B-erythro penta furyl glycosyl) adenine
3TC; Lamivudine;
Approval;
Lamivudine and zidovudine;
3TC ﹠amp; AZT; Approval
4 '-acetylamino phenyl 4-guanidine benzoate (guadinobenzoate); AGB
4 '-Az-3 '-dT; 4 '-azido-3 '-deoxyribosylthymine
4 '-Az-5CldU; 4 '-azido-5-chloro-2 '-BrdU,
4 '-AzdA; 4 '-azido-2 '-deoxyadenosine
4 '-AzdC; 4 '-azido-2 '-deoxycytidine
4 '-AzdG; 4 '-azido-2 '-deoxyguanosine
4 '-AzdI; 4 '-azido-2 '-deoxyinosine
4 '-AzdU; 4 '-azido-2 '-BrdU,
4 '-azido-2 '-deoxidation-β-D-erythro-penta furyl glycosyl-5-methyl-2,4-dioxo pyrimidine; 4 '-the azido thymidine
4 '-cyano group breast glycosides; 4 '-CN-T
4-methyl-5-(pyrazinyl)-3H-1,2-dithiole (dithiole)-3-thioketone; Oltipraz
5 '-[(1,4-dihydro-1-methyl-3-pyridine radicals carbonyl) oxygen base]-3 '-azido-2 ', 3 '-deoxyribosylthymine; DP-AZT; HP-AZT; The AZT prodrug; AZT-DHP
5 '-[[(Z)-and 4-amino-crotyl] methylamino]-5 '-deoxyadenosine; MDL 73811
5 '-alkyl polyglucoside carbonic ester of 3 '-azido-3 '-deoxyribosylthymine; AcNHGlc-hexyl-CO3 AZT
5Cl3PhS-2 indole CONH2
5-fluoro-2 ', 3 '-zalcitabine; 5-F-ddC
5-methyl-3 '-azido-2 ', 3 '-the different cytidine of dideoxy; MeAZddIsoC
6-O-bytyry Castanospermine; BuCast; MDL 28,574; Celgosivir
6-chloro-9-(2,3-dideoxy-β-D-glycerol penta furyl glycosyl)-9H-purine; D2ClP; 6-chloro-ddP; CPDDR; 6Cl-ddP
6-dimethylaminopurine-2 ', 3 '-di-deoxynucleoside; N-6-dimethyl ddA; DMAPDDR
7-chloro-N-methyl-5-(1H-pyrroles-2-yl)-3H-1, the 4-benzodiazepine
(benzodiazepin)-2-amine; Ro 24-7429
7-chloro-5-(2-pyrrole radicals)-3H-1, the 4-benzodiazepine
-2 (H)-ketone; Ro 5-3335
8-chloro-TIBO; Tivirapine; R86183
9-(2,3-dideoxy-β-D-ribofuranosyl (ribofuranosyl))-6-(methyl mercapto) purine; D2SMeP
Two (OHMe) cBu of 9-[] A; A-69463; Cyclobutyl-A; Cyclobut-A; C-Europe tower mycin (oxetanocin) A
·A-76890
·A-77212
A-80987; The ritonavir derivant
A-81525; The ritonavir derivant
A-83962; The ritonavir derivant
A-98881; Azacyclo-urea (Azacyclic urea) derivant
AA; The L-ascorbic acid; Calcium ascorbate
·AAP-BHAP;U-104489;PNU-104489
A Bakawei ﹠amp; Lamivudine and zidovudine; Three associations only
ABC ﹠amp; (-)-3TC ﹠amp; AZT
ABT-378; Lopinavir; The composition of Kaletra;
ABT-378 ﹠amp; ABT-538;
Lopinavir and ritonavir;
With
ABT-538;
Ritonavir; The composition of Kaletra; Approval
Acemannan
Adefovirdipivoxil; PMEA; GS-0393
Adefovir dipivoxil; BisPom PMEA; GS-840;
AG-1343;
Nelfinavir; Approval
AG1350; LY316957; The similar thing of nelfinavir-octahydro-thienopyridine
The AHPBA analog; R-87366
Alpha-lipoic acid; Alpha-lipoic acid; Thioctic acid (Thioctic acid)
·ALX40-4C
·AMD3100;JM3100
The phosphoric acid amprenavir; VX-175; GW433908; GW433908A (
*Sodium salt
*); GW433908G (
*Calcium salt
*); Fosamprenavir
·Ancer?20;Z-100
Antisense 25-aggressiveness phosphorothioate (phosphorothioate); GEM91
·Atazanavir;CGP-73547;BMS-232632;BMS?232632;Zrivada;Latazanavir;
Ah 's dimension is fixed; U-87201E; The BHAP derivant
Aurintricarboxylic acid (Aurintricarboxylic acid); Dupont ATA; Dupont DA639; SD-095345; ATA
AY 9944; Anti-form-1, two (2-dichloro benzyl amino-ethyl) the cyclohexane extraction dihydrochlorides of 4-
AZT; Zidovudine; Azido breast glycosides;
AZT-PO3 (CH3)-AZT; O, O '-two (3 '-azido-3 '-methyl phosphonate of deoxyribosylthymine-5 '-yl)
Baicalin; TJN-151
Belulinic acid Betulinic acid (Betulinic acid); Mairin
Belulinic acid Betulinic acid, 3-O-(3 ', 3 '-the dimethyl succinate ester)
The BHAP derivant
The BHAP derivant
The BHAP derivant
The BHAP derivant
The BHAP derivant
The BHAP derivant;
Delavirdine; U-90152
The BHAP derivant; U-88204E
BI-RG-587; Nevirapine;
Approval
·BILA?1906?BS
BILA 2011 BS; Palinavir
·BILA?2185?BS
Two (2-nitrobenzophenone) sulfone; Two (2NO2Ph) SO2; NSC633001
Two-ValHOEt-N2aza-peptide isostere; CGP 53820
Two-ValHOEt-N2aza-peptide isostere; CGP 53820 analog
·BMS-186318
·BocPhe[CHOH(CH2)3CH=CHPhCO]IleAMBI;L-687,908
·BzOCValPhe[diCHOH(RR)]PheValBzOC
·BzOCValPhe[diCHOH(SS)]PheValBzOC
C2-Sym phosphine (Phosphinic) amide derivatives (HOECHST AG)
·Calanolide?A;NSC675451
·Calanolide?B
Capravirine; S-1153
Castanospermine
·CbzAF(CHOHCH2)AVVOMe
·Cbz-Asn-Apns-Pro-NH-tBu;KNI-102
CGP 61755; LASINAVIR BMS-234475 Lasinavir [INN
·CGP?64222
·CNI-H0294
Coactinon; I-EBU; The HEPT derivant; MKC-442; Emivirine
·Conocurvone;NSC650891
Coviracil; (-) FTC; (-)-2 ', 3 '-dideoxy-5-fluoro-3 '-thia cytidine (thiacytidine); Emtricitabine; Emtriva
C-Europe tower mycin-G; A-69992; (+-) Lobucavir; C-Oxt-G; Cyclobut-G; (+-) Cyclobut-G
The sulfogel polysaccharide
·CV-N;Cyanovirin-N
Ring urea amide; SD146
Cyclosporin A;
[Me-Ile-4] cyclosporin A; SDZ NIM 811
D4A (L); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-DIDEOXYADENOSINE
D4FC; D-D4FC; 2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy-5-fluorine cytidine; DPC 817
D4FC (L); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy-5-fluorine cytidine
D4G (L); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-the dideoxy guanosine
D4I (L); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-didanosine
·DABO
DdC; Zalcitabine; Zalcitabine;
DdI; Didanosine; Didanosine;
Dehydroepiandrosterone; DHEA; Astenile (Prasterone); Dehydroepiandrosterone
(Dehydroisoandrosterone);EL-10
Dextran sulfate
Two caffeic acid esters; L-chicoric acid (Chicoric acid)
DMP-266;
Efavirenz; Approval
·DMP-323;XM-323
·DMP-450
Docosanol; Just-docosanol
DOTC (-); (-)-2 '-deoxidation-3 '-oxa--4 '-sulfo-cytidine (thiocytidine)
DOTFC (-); (-)-2 '-deoxidation-3 '-oxa--4 '-sulfo--5-flurocytosine
DP-178; Pentafuside; T-20; GP41 127-162 AA; Enfuvirtide;
E-BPTU; The HEPT derivant; NSC 648400
E-EBU; The HEPT derivant; The MKC-442 derivant
E-EBU-dM; The HEPT derivant; The MKC-442 derivant
E-EPSeU; The HEPT derivant; The MKC-442 derivant
E-EPU; The HEPT derivant; The MKC-442 derivant
Ebselen
Etoposide
The epoxy steroid derivatives; (4 α, 5 α, 17 β)-17-hydroxyl-3-oxo-4,5-epoxy androstane-2-Methanamide
Eulicin
Fenalamide A1 (fenalamide A1); Phenalamide A1; Stipiamide
·Fleephilone
Fluoro quinolone derivative; K-12
Fortovase
Saquinavir; Ro31-8959; Approval
Foscarnet; Phosphine formic acid; Foscarnet sodium (Foscavir);
·FPMDAP;
·FPMPA
·FPMPG
GPGRAF eight aggressiveness; SPC3
Hammerhead shape (Hammerhead) is anti--and gag RNA constitutes enzyme, B
·Harziphilone
HBY 097; Quinoxaline derivant
The HEPT derivant; The MKC-442 derivant
The HEPT derivant; The MKC-442 derivant
The HOCH2CH2 isostere; Thienopyridine (Thienopyrid) CON thienyl urea alkane (urethane) derivant
The HOCH2CH2 isostere; Thienopyridine CON thienyl urethane derivant
The HOCH2CH2 isostere; Thienopyridine CON thienyl urethane derivant
The HOCH2CH2 isostere; Thienopyridine CON thienyl urethane derivant
The HOCH2CH2 isostere; Thienopyridine CON thienyl urethane derivant
The HOCH2CH2 isostere; Thienopyridine CON thienyl urethane derivant; LY326188
·HPMPA
·HPMPDAP
HU; Hydroxyurea; Hydrea
Hydroxocobalamine
Hypericin
Ingenol 3,5, the 20-triacetate; ITA; RD3-2118
The ingenol derivant; RD4-2138
Calophylloide (Inophyllum) B
Calophylloide P
·iQoa-Mta-Apns-Thz-NH-tBu;KNI-272
IsoquinCON furyl urea alkane analog
IsoquinCON thienyl urea alkane analog
IsoquinCON thienyl urea alkane analog
·KNI-154;Noa-Asn-Apns-Thz-NH-tBu
·KNI-174;Noa-Asn-Apns-Dmt-NH-tBu
·KNI-227;Qoa-Mta-Apns-Thz-NH-tBu
·L-685,434
L-685, the 434-6-hydroxy derivatives
L-685, the 434-OEtMorph derivant; L-689,502
·L-685,434-OEtNMe2
L-685, the 434-OPrMorph derivant
L-697,593; The 2-Pyridione derivatives
L-697,639; The 2-Pyridione derivatives
L-697,661; The 2-Pyridione derivatives
·L-FddC;β-L-5F-ddC
Lamivudine and zidovudine;
3TC ﹠amp; AZT; Approval
·LY289612
The LY289612 analog
The LY289612 analog
LY-300046-HCl; The PETT derivant; Trovirdine
LY314163; Saquinavir/nelfinavir derivant.
LY-73497; N-(2-phenethyl)-N '-(2-thiazolyl) thiourea; PETT
MAP; The allylene putrescine
·Michellamine?A;NSC650898
·Michellamine?B;NSC649324
·Michellamine?F
N-6-Et-ddA; N-ethyl-2 ', 3 '-DIDEOXYADENOSINE
N-6-methyl ddA; N6-methyl-2 ', 3 '-DIDEOXYADENOSINE
Naphthalene 2-sulphonic acid ester polymer (Naphthalene 2-sulphonate polymer); PRO 2000
The similar thing of nelfinavir-octahydro-thienopyridine
Nonoxynolum (Nonoxynol) 9
NSC625487; Thiazole and benzimidazole; TBZ
Oxathiin (Oxathiin) derivant; UC-38
The oxathiin derivant; UC-84
·P9941
Penicillin Et (NH) 2Sym dimer
Benzylpenicillin, ET (NH) 2 derivants
Penicillin, the 2Isoquin-OHPrNH2 analog
Penicillin, the 2Isoquin-OHPrNH2 analog
The sulphuric acid pentosan; Elmiron; SP54; Sulphuric acid xylan (Xylan Sulfate);
PETT Cl, the F derivant
The PETT derivant
The PETT derivant
The PETT derivant
The PETT derivant
·Phenoxan
The phorbol derivant; Prostratin
·Platanic?acid
·PMEDAP
·PMEG
·PMEHx;PMEI
·PMEMAP
·PMET
PNU-140690; U-140690; Tipranavir
Pyridione derivatives
Pyridione derivatives
Quinoxaline 2 40 thione derivatives; S-2720
R14458; The TIBO derivant.
R82150; The TIBO derivant.
R82913; The TIBO derivant
·Resobene
Ribavirin; Virazole
Ro 31-8959-bis-thf derivant
Saquinavir/nelfinavir derivant
Saquinavir/nelfinavir derivant
SB-205569; Val-Phe-Phe-HOCH2CH2 isostere analog
SC-52151; Compound E
·SDZ?PRI?053
Naganol
·T22
Thalidomide
·Thiangazole;(-)-Thiangazole
Thiazole and iso-indoles (Thiazoloisoindol)-5-ketone
Thiazole and iso-indoles-5-ketone, derivant
Tle-Val-Sta, the 5PhBuCOOH derivant; The statine derivant
Tle-Val-Sta, the 5PhBuCOOH derivant; The statine derivant
·UC-781
Val-Val-Sta, the 5PhBuCOOH derivant; The statine derivant
Val-Val-Sta, the 5PhBuCOOH derivant; The statine derivant
Val-Val-Sta, the 5PhBuCOOH derivant; The statine derivant
Val-Val-Sta, the 5PhBuCOOH derivant; The statine derivant
Val-Val-Sta, the 5PhBuCOOH derivant; The statine derivant
·VB-11,328
Be used for the treatment of HIV and infect, or be secondary to the medicine of disease that HIV infects or morbid state and/or bioactivator another be listed as follows described.In these medicines one or more can comprise AIDS/ARC, Kaposi sarcoma, hepatitis B virus infection, other infected by microbes (for example tuberculosis etc.) with treatment HIV or a kind of secondary disease or morbid state with at least a as in addition disclosed two keto acid anti-hiv agents combination (administration altogether) herein.These chemical compounds also use with effective dose.
These chemical compounds comprise: ACV; AK602; AMD070; APV; ATV; ATZ; AVX754 (apricitabine); AZT; Abacavir; Abacavir/lamivudine/zidovudine; Abacavir sulfate; Abacavir sulfate/lamivudine; Abacavir/lamivudine; Abelecet; Aciclovir; Adefovir dipivoxil; Amycin; Agenerase; Aldesleukin; Alovudine; Aluvia; Ambisome; Amdoxovir; Amphocin; Amphotec; Amphotericin B; Polyinosini; Amprenavir; Androderm; Androgel; Apricitabine; Aptivus; Atazanavir; Atripla; Azithromycin; BMS-378806; BMS-488043; Bactrim; Baraclude; Bevirimat; Biaxin; Brecanavir; BufferGel; C31G; CD4-IgG2; CS; CV-N; Calanolide A; Calcium hydroxyapatite; Carbopol 974P; Carrageenan; Carraguard; Sulfate cellulose; Clarithromycin; Combivir; Copegus; Sulfamethoxazole (Cotrimoxazole); Crixivan; Cyanovirin-N; Cymevene; DAPD; DLV; DS; Darunavir; Delavirdine; The Depo-testosterone; Dextran sulfate; Didanosine; Fluconazole; Doxil; Doxorubicin (liposome); Dronabinol; EFV; Efavirenz; Elvucitabine; Emtricitabine; The tenofovir disoproxil fumarate; Emtriva; Enfufirtide; Entecavir; Lamivudine; Epoetin Alfa; Epogen; Epzicom; Etopophos (phosphate); Etoposide; Etravirine; FTC; Fluconazol; Fortovase; Fosamprenavir; Foxivudinetidoxil; Fungizone; Fuzeon; GS 9137; GSK-873,140 (aplaviroc); GW433908; GW640385 (brecanavir); Ganciclovir; Immunoglobulin (Globulin, Immune); Growth hormone (people); Hepsera; Hivid; The human growth hormone; IL-2; INH; Immunoglobulin intravenous (people); Indinavir; Interferon; Interleukin-2, recombinant, people; Recombinant Interferon (2b); Invirase; Isoniazid; Itraconazole; KP-1461; Lamivudine/zidovudine; Lexiva; Lopinavir/ritonavir; MK-0518; Nebupent; Nelfinavir; Neutrexin; Nevirapine; Nuo Wei; Nydrazid; Peptide T; PMPA prodrug (Viread) ' Prezista (Darunavir); PRO 140; PRO2000; PRO 542 (CD4 IGg2); Procrit (Epoetin); Aldesleukin; Racivir; Radiesse; Rrebetol; Delavirdine; Zidovudine; Reyataz; Ribavirin; Rifabutin; Rifadin; Rifampicin; Rimactane; Ritonavir; Rodferon-A (2a); Saquinavir; SCH-D (vicriviroc); Growth hormone; Stavudinie; Sulfamethoxazole/trimethoprim; Testosterone (Sustanon); Sustiva; TNX-355; Taxol; Tenofovir; The tenofovir disoproxil fumarate; Testosterone; Tipranavir; Toposar; Trimetrexate; Three associations only; Truvada (Emtriva and Viread combination); U-90152S (Delaviridine); UC-781; UK-427,857 (maraviroc); Valcyte; Valganciclovir; Valproic acid; Fan Bishi; Vicriviroc; Videx; Viracept see nelfinaivr (Tennofovir DF); The happy life of dimension; Virazole; Viread; Vitrasert; Zalcitabine; Sai Ruite; Match is advanced; Zidovudine; Zithromax; Zovirax.
Be used for the treatment of HIV and infect, or be secondary to disease that HIV infects or morbid state medicine and/another of bioactivator is listed as follows described.In these medicines one or more can comprise AIDS/ARC, Kaposi sarcoma, hepatitis B virus infection, other infected by microbes (for example tuberculosis etc.) with treatment HIV or a kind of secondary disease or morbid state with at least a as in addition disclosed two keto acid anti-hiv agents combination (administration altogether) herein.These chemical compounds also use with effective dose.
These chemical compounds comprise: ACV; AK602; AMD070; APV; ATV; ATZ; AVX754 (apricitabine); AZT; Abacavir; Abacavir/lamivudine/zidovudine; Abacavir sulfate; Abacavir sulfate/lamivudine; Abacavir/lamivudine; Abelecet; Aciclovir; Adefovir dipivoxil; Amycin; Agenerase; Aldesleukin; Alovudine; Aluvia; Ambisome; Amdoxovir; Amphocin; Amphotec; Amphotericin B; Polyinosini; Amprenavir; Androderm; Androgel; Apricitabine; Aptivus; Atazanavir; Atripla; Azithromycin; BMS-378806; BMS-488043; Bactrim; Baraclude; Bevirimat; Biaxin; Brecanavir; BufferGel; C31G; CD4-IgG2; CS; CV-N; Calanolide A; Calcium hydroxyapatite; Carbopol 974P; Carrageenan; Carraguard; Sulfate cellulose; Clarithromycin; Combivir; Copegus; Sulfamethoxazole; Crixivan; Cyanovirin-N; Cymevene; DAPD; DLV; DS; Darunavir; Delavirdine; The Depo-testosterone; Dextran sulfate; Didanosine; Fluconazole; Doxil; Doxorubicin (liposome); Dronabinol; EFV; Efavirenz; Elvucitabine; Emtricitabine; Emtricitabine; The tenofovir disoproxil fumarate; Emtriva; Enfufirtide; Entecavir; Lamivudine; Epoetin Alfa; Epogen; Epzicom; Etopophos (phosphate); Etoposide; Etravirine; FTC; Fluconazol; Fortovase; Fosamprenavir; Foxivudinetidoxil; Fungizone; Fuzeon; GS 9137; GSK-873,140 (aplaviroc); GW433908; GW640385 (brecanavir); Ganciclovir; Immunoglobulin; Growth hormone (people); Hepsera; Hivid; The human growth hormone; IL-2; INH; Immunoglobulin, intravenous (people); Indinavir; Interferon; Interleukin-2, recombinant, people; Recombinant Interferon (2b); Invirase; Isoniazid; Itraconazole; KP-1461; Lamivudine/zidovudine; Lexiva; Lopinavir/ritonavir; MK-0518; Nebupent; Nelfinavir; Neutrexin; Nevirapine; Nuo Wei; Nydrazid; Peptide T; PMPA prodrug (Viread) ' Prezista (Darunavir); PRO 140; PRO 2000; PRO 542 (CD4IGg2); Procrit (Epoetin); Aldesleukin; Racivir; Radiesse; Rrebetol; Delavirdine; Zidovudine; Reyataz; Ribavirin; Rifabutin; Rifadin; Rifampicin; Rimactane; Ritonavir; Rodferon-A (2a); Saquinavir; SCH-D (vicriviroc); Growth hormone; Stavudinie; Sulfamethoxazole/trimethoprim; Testosterone; Sustiva; TNX-355; Taxol; Tenofovir; The tenofovir disoproxil fumarate; Testosterone; Tipranavir; Toposar; Trimetrexate; Three associations only; Truvada (Emtriva and Viread combination); U-90152S (Delaviridine); UC-781; UK-427,857 (maraviroc); Valcyte; Valganciclovir; Valproic acid; Fan Bishi; Vicriviroc; Videx; Viracept see nelfinaivr (Tennofovir DF); The happy life of dimension; Virazole; Viread; Vitrasert; Zalcitabine; Sai Ruite; Match is advanced; Zidovudine; Zithromax; Zovirax.
Provide following representative embodiment to describe the preparation of chemical compound of the present invention in detail.Embodiment is not in order to limit scope of the present invention, and should not be interpreted as restriction.And the chemical compound that following embodiment describes only should not regarded as and forms as the sort of chemical compound that the present invention thought, any combination itself of the composition of described chemical compound or their part (moieties) can form other chemical compound.This writes exactly in this patent documentation in advance.Those skilled in the art will understand easily, can prepare these other chemical compounds to change and the synthetic conversion that following preparation method is carried out known reaction condition.
Provide following representative embodiment to describe the preparation of chemical compound of the present invention in detail.Embodiment does not limit scope of the present invention, should not be interpreted as restriction.And the chemical compound that following embodiment describes only should not regarded as and forms as the sort of chemical compound that the present invention thought, any combination itself of the composition of described chemical compound or their part (moieties) can form other chemical compound.This writes exactly in this patent documentation in advance.Those skilled in the art will understand easily, can prepare these other chemical compounds to change and the synthetic conversion that following preparation method is carried out known reaction condition.
Chemosynthesis
Represent embodiment 1
4-(1,5-dibenzyl-1,2-dihydro-2-oxo-pyridin-3-yl)-2-hydroxyl-4-oxo fourth-2 olefin(e) acid (8).
Related procedure (1) is as follows.
Flow process 1
Step 1:5-benzyl pyridine-2-amine (2).
With pyridine-2-amine 1 (14.1g, 149.8mmol) and benzyl chloride (36.0g, mixture heated to 180 284.6mmol) ℃ is until mixture boiling [Kowalski, J.Heterocycl.Chem.28,875-879 (1991)].Temperature progressively rose to 250 ℃ and kept 24 hours in 3 hours then.After the cooling, reactant mixture is washed out from flask with MeOH (60mL), and with 10% NH
4OH aqueous solution (40mL) is handled.After adding entry (200mL), use CHCl
3(grease of 2 * 200mL) extraction gained is used anhydrous Na
2SO
4Drying, and distill out CHCl
3Residue separates by distilling under reduced pressure.The fraction of collecting at 130-135 ℃/1mm Hg is further purified on silica gel (EtOAc: hexane, 7: 3) by flash chromatography.Output 9.2g (34%), white solid, mp 79-80 ℃.
1H NMR (CDCl
3, 500MHz): δ 3.87 (s, 2H, CH
2), 4.43 (bs, 2H, NH
2), 6.48 (d, 1H, CH J=8.5Hz), 7.19-7.33 (m, 6H, Ar-H and CH), 7.99 (d, 1H, CH, J=1.5Hz).
13C NMR (CDCl
3, 125MHz): δ 38.2,108.7, and 126.1,126.4,128.5,128.7,128.9,128.9,138.6,140.9,147.7,156.8.
Step 2:5-benzyl-3-bromopyridine-2-amine (3).
(6.0g is 32.3mmol) at CH to 0 ℃ the 5-benzyl pyridine-2-amine 2 of being cooled to that stirs
2Cl
2Dripping bromine in the solution (100mL) (5.1g, 32.3mmol) [Kelly waits the people, J.Am.Chem.Soc.112,8024-8034 (1990)].Bromine decolours immediately, and described mixture was stirred 30 minutes.With the saturated NaHCO of this mixture
3Solution (100mL) jolting is then with the organic layer anhydrous Na
2SO
4Drying, and distillation obtains yellow residue, and it is further purified on silica gel (EtOAc: hexane, 3: 7) with flash chromatography.Output 7.3g (86%), white solid, mp 110-111 ℃.
1H NMR (CDCl
3, 500MHz): δ 3.86 (s, 2H, CH
2), 4.88 (bs, 2H, NH
2), 7.19-7.35 (m, 5H, Ar-H), 7.50 (d, 1H, CH, J=1.5Hz), 7.94 (d, 1H, CH, J=1.0Hz).
13CNMR (CDCl
3, 125MHz): δ 37.7,104.6, and 126.4,126.4,128.1,128.6,128.6,128.7,140.2,140.8,146.7,154.0; HRMS (M+H)
+Value of calculation C
12H
13BrN
2263.0184, measured value 263.0184.
Step 3:5-benzyl-3-bromopyridine-2 (1H)-ketone (4).
(0.2g adds entry (2) in DMF 0.7mmol) (4mL) solution, (0.378g 3.6mmol) and with reactant mixture at room temperature stirred 30 minutes to add nitrite tert-butyl then to the 5-benzyl-3-bromopyridine-2-amine 3 that stirs.Distill out DMF and excessive reagent, residue is further purified on silica gel (EtOAc: hexane, 1: 1) by flash chromatography.Output 7.3g (86%), white solid, mp 151-152 ℃.
1H NMR (CDCl
3, 500MHz): δ 3.77 (s, 2H, CH
2), 7.17-7.36 (m, 6H, Ar-H and CH), 7.76 (d, 1H, CH, J=1.5Hz) 13.25 (bs, 1H, NH).
13CNMR (CDCl
3, 125MHz): δ 37.3,115.4, and 121.0,126.9,128.8,128.8,128.9,128.9,132.4,138.5,145.3,161.0; HRMS (M+H)
+Value of calculation C
12H
11BrNO264.0024, measured value 264.0014.
Step 4:1,5-dibenzyl-3-bromopyridine-2 (1H)-ketone (5).
To 5-benzyl-3-bromopyridine-2 (1H)-ketone 4 (3.5g, 13.5mmol) add NaH (60% mineral oil suspension) (0.5g in the suspension in dry DMF (100mL), 16.2mmol) and stirred 30 minutes, add then benzyl bromide a-bromotoluene (0.1.36g, 7.9mmol) and with mixture room temperature restir 1 hour.DMF is distilled out, and residue is dissolved among the EtOAc (250mL) again, (anhydrous Na is used in 2 * 100mL) washings with saline solution
2SO
4Drying also distills out EtOAc, obtains yellow slurry, and it is further purified on silica gel (EtOAc: hexane, 4: 6) by column chromatography and obtains 5.Output 3.8g (83%), yellow solid, mp 89-90 ℃.
1H NMR (CDCl
3, 500MHz): δ 3.69 (s, 2H, CH
2), 5.18 (s, 2H, CH
2), 7.11 (d, 1H, CH, J=2Hz), 7.12-7.39 (m, 10H, Ar-H), 7.60 (d, 1H, CH, J=2Hz),
13C NMR (CDCl
3, 125MHz): δ 37.4,53.5,117.1,119.1,126.9,128.2,128.2,128.3,128.3,128.6,128.8,128.8,128.9,128.9,134.6,135.8,138.7,143.0,158.3.HRMS (M+H)
+Value of calculation C
19H
17BrNO354.0494, measured value 354.0455.
Step 5:3-acetyl group-1,5-dibenzyl-3-pyridine-2 (1H)-ketone (6).
At N
2In at 70 ℃, with 1, and 5-dibenzyl-3-bromopyridine-2 (1H)-ketone 5 (1.0g, 2.8mmol), two (triphenylphosphine) Palladous chloride. (II) (0.19g, 0.28mmol) and ethoxy vinyl (tributyl) stannum (2.03g, 5.6mmol) mixture heated in dry DMF (50mL) is 1 hour.DMF is distilled out, and residue is dissolved among the EtOAc (50mL) and through Celite pad again filters.HCl (30mL) with 1N stirred 15 minutes with the EtOAc fraction, and (anhydrous Na is used in 2 * 30mL) washings to water
2SO
4Drying, distillation obtains yellow residue, and it is further purified on silica gel (EtOAc: hexane, 2: 8) by flash chromatography.Output 0.86g (97%), yellow oil.
1H NMR (CDCl
3, 500MHz): δ 2.73 (s, 3H, CH
3), 3.75 (s, 2H, CH
2), 5.19 (s, 2H, CH
2), 7.14-7.40 (m, 11H, Ar-H and CH), 8.04 (d, 1H, CH, J=3Hz).
13C NMR (CDCl
3, 125MHz): δ 31.1,37.5, and 52.5,118.6,126.8,127.8,127.8,127.9,128.2,128.2,128.6,128.6,128.8,128.8,129.0,135.8,138.8,140.7,144.8,160.4,198.0; HRMS (M+H)
+Value of calculation C
21H
20NO
2318.1494, measured value 318.1461.
Step 6:4-(1,5-dibenzyl-1,2-dihydro-2-oxo-pyridin-3-yl)-2-hydroxyl-4-oxo but-2-ene acid methyl ester (7).
To the 3-acetyl group-1 that stirs, (0.1g, (0.30g 3.1mmol), and stirs reactant mixture 15 minutes 5-dibenzyl-3-pyridine-2 (1H)-ketone 6 to add sodium tert-butoxide in THF 0.31mmol) (5mL) solution.Add dimethyl oxalate. (0.37g, THF 3.1mmol) (5mL) solution, and stirring 2 hours under the room temperature.Distill out THF, the HCl (1mL) that adds 1N, with EtOAc (2 * 10mL) extractions, with saturated brine solution (4 * 20mL) washings, use anhydrous sodium sulfate drying, distill out EtOAc and obtain the brown residue, it is at first by ion exchange chromatography (diethylamino cross-linking dextran anion exchange resin (CH
3CN: H
2O, 1: 1) purification, and then by flash chromatography at silica gel (CHCl
3: MeOH, 9.9: 0.1) last purification.Output 0.054g (44%), yellow oil.
1H NMR (CDCl
3, 500MHz): δ 3.79 (s, 2H, CH
2), 3.91 (s, 3H, CH
3), 5.21 (s, 2H, CH
2), 7.15-7.42 (m, 11H, Ar-H and CH), 7.98 (s, 1H, alkene CH), 8.24 (d, 1H, CH, J=2.5Hz),
13C NMR (CDCl
3, 100MHz): δ 37.5,52.7, and 53.0,101.8,119.0,123.4,126.9,128.0,128.0,128.3,128.6,128.6,128.9,129.0,129.0,129.1,135.6,138.6,141.4,145.0,159.5,162.6,172.2,185.5; HRMS (M+H)
+Value of calculation C
24H
22NO
5404.1498, measured value 404.1411.
Step 7:4-(1,5-dibenzyl-1,2-dihydro-2-oxo-pyridin-3-yl)-2-hydroxyl-4-oxo fourth-2 olefin(e) acid (8).
At 0 ℃, to 4-(1,5-dibenzyl-1,2-dihydro-2-oxo-the pyridin-3-yl)-2-hydroxyl that stirs-4-oxo but-2-ene acid methyl ester 7 (0.069g, 0.17mmol) MeOH (5mL) solution in add NaOH (0.5mL) solution of 1N, reactant mixture stirred 30 minutes at 0 ℃.Then, will be reflected at ambient temperature stirred 1 hour.With of the HCl neutralization of this reactant mixture, with isolating solid filtering and vacuum drying with 1N.Obtain yellow solid with EtOAc/ hexane recrystallization.Output 0.034g (52%), yellow solid, mp 158-159 ℃.
1H NMR (CDCl
3, 500MHz): δ 3.82 (s, 2H, CH
2), 5.26 (s, 2H, CH
2), 7.16-7.39 (m, 10H, Ar-H), 7.45 (d, 1H, CH, J=2Hz), 7.98 (s, 1H, alkene CH), 8.26 (d, 1H, CH, J=2Hz),
13C NMR (CDCl
3, 125MHz): δ 37.5,53.3, and 100.8,119.8,123.1,127.0,128.2,128.5,128.5,128.6,128.6,128.9,128.9,129.0,129.1,129.1,135.2,138.4,141.3,145.1,159.5,162.3,173.7; HRMS (M+H)
+Value of calculation C
23H
20NO
5390.1341, measured value 390.1342.
Represent embodiment 2
4-(1,5-dibenzyl-1,4-dihydro-4-oxo pyridine-3-yl)-2-hydroxyl-4-oxo fourth-2 olefin(e) acid (16).
Related procedure (2) is as follows.
Flow process 2
Step 1:3,5-two bromo-pyridine-4-ketone (10)
Through the ice-cold pyridine-4-ketone 9 of 30 fens clockwise (6.98g, 73.4mmol) and KOH (9.52g, dripping bromine in water 146.8mmol) (140mL) solution (7.58mL, 147.5mmol) [Spivey waits the people, J.Org.Chem.65,3154-3159 (2000)].Added back 30 minutes, filtering-depositing, with a large amount of water washings, and vacuum drying.Output 16.17g (87%), yellow solid, 320 ℃ of mp (distillation).
1H?NMR(DMSO-d
6,500MHz):δ12.3(s,1H),8.26(s,2H).
13C?NMR(DMSO-d
6,125MHz):δ167.5,138.2,138.2,111.8,111.8。
Step 2:3-bromo-5-(hydroxyl-phenyl-methyl)-pyridine-4-ketone (11)
At-78 ℃, under blanket of nitrogen, to 3, (0.313g 1.24mmol) adds phenyl-magnesium-bromide solution (1.36mL, the THF solution of 1M to 5-two bromo-pyridine-4-ketone 10 in the heterogeneous mixture of anhydrous THF (4mL), 1.36mmol) [people such as Borzilleri, United States Patent (USP) 20050245530].Stir after 15 minutes, add n-BuLi solution (0.68mL, the 2M cyclohexane solution, 1.36mmol), and-78 ℃ under blanket of nitrogen, reactant mixture was stirred 15 minutes.(0.26mL 2.6mmol) and with this mixture stirred 2 hours at-78 ℃ to add benzaldehyde in this mixture.The cancellation of this reactant mixture by adding HOAc (0.38mL) and TFA (0.38mL), vacuum concentration, residue is gone up purification by flash column chromatography at silica gel (dichloromethane: methanol, 95: 5).Output 0.125g (36%), white solid, 123-124 ℃.
1H?NMR(MeOH-d
4,500MHz):δ8.09(s,1H),7.81(s,1H),7.38-7.17(m,5H),5.92(s,1H),3.83(s,2H).
13C?NMR(MeOH-d
4,125MHz):δ174.3,144.4,139.7,135.8,133.6,129.4,129.3,128.6,128.0,128.0,114.8,70.8。
Step 3:3-benzyl-5-bromopyridine-4-ketone (12)
3-bromo-5-(hydroxyl-phenyl-methyl) pyridine-4-ketone 11 (0.125g, 91mmol), TFA (16mL) and Et
3The mixture of SiH in anhydrous methylene chloride (30mL) is in stirring at room 10 hours [Borzilleri waits the people, United States Patent (USP) 20050245530].With the reactant mixture vacuum concentration, residue is gone up purification by flash column chromatography at silica gel (dichloromethane: methanol, 98: 2).Output 0.081g (69%), white solid.
1H?NMR?(MeOH-d
4,500MHz):δ8.12(s,1H),7.47(s,1H),7.29-7.17(m,5H),3.83(s,2H).
13C?NMR(MeOH-d
4,125MHz):δ175.2,140.7,139.5,136.9,130.8,130.0,130.0,129.5,129.5,127.3,114.1,34.9。
Step 4:1,3-dibenzyl-5-bromo-1H-pyridine-4-ketone (13)
Under blanket of nitrogen, with 3-benzyl-5-bromopyridine-4-ketone 12 (0.57g, 2.16mmol) and NaOEt (0.89mL, 2.37mmol) (0.30mL 2.59mmol) refluxed 1 hour for mixture in dehydrated alcohol (20mL) and benzyl chloride.Solvent distilled away obtain yellow residue, it goes up purification by flash column chromatography at silica gel (dichloromethane: methanol, 98: 2).Output 1.31g (96.7%), yellow solid, mp 120-121 ℃.
1H NMR (CDCl
3, 500MHz): δ 7.67 (d, 1H, J=2.4), 7.32-7.07 (m, 10H), 4.83 (s, 1H), 3.78 (s, 2H).
13C NMR (CDCl
3, 125MHz): δ 172.2,139.6,139.1,137.6,134.7,129.9,129.9,129.3,129.3,129.2,129.0,128.6,128.6,127.5,127.6,126.4,114.1,60.3,34.4.HRMS (M+H)
+Value of calculation C
19H
16BrNO 354.0494, measured value 354.0499.
Step 5:3-acetyl group-1,5-dibenzyl-1H-pyridine-4-ketone (14)
1,3-dibenzyl-5-bromo-1H-pyridine-4-ketone 13 (1.31g, 2.70mmol), tributyl-(1-ethoxy ethylene base) stannum (1.80mL, 5.18mmol) and two (the triphenylphosphine)-palladiums (II) of dichloro (0.26g, 0.37mmol) mixture in dry DMF (20mL) stirred 8 hours at 95 ℃ under blanket of nitrogen.(3 * 50mL) extractive reaction mixture are with HCl (3 * 50mL) washings, and distilling off solvent of 1N with ethyl acetate.Residue is gone up purification by flash column chromatography at silica gel (dichloromethane: methanol, 98: 2).Output 1.06g (90%), yellow oil.
1H NMR (CDCl
3, 500MHz): δ 8.19 (d, 1H, J=2.6), 7.39-7.10 (m, 10H), 6.90 (d, 1H, J=2.5), 4.89 (s, 2H), 3.81 (s, 2H), 2.74 (s, 3H) .HRMS (M+H)
+Value of calculation C
21H
19NO
2318.1494, measured value 318.1493.
Step 6:4-(1,5-dibenzyl-4-oxo-1,4-dihydro-pyridin-3-yl)-2-hydroxyl-4-oxo-but-2-ene acid methyl ester (15).
At the sodium tert-butoxide (0.52g of room temperature to stirring; 5.23mmol) anhydrous THF (13mL) solution in drip dimethyl oxalate. (0.42g; 3.48mmol) THF (6mL) solution; add 3-acetyl group-1 then; 5-dibenzyl-1H-pyridine-4-ketone 14 (0.55g, THF 1.74mmol) (8mL) solution.With the mixture of gained in stirring at room 4 hours, acidify then (pH=6).Crude product is with ethyl acetate (100mL) extraction, water (2 * 100mL) and saline (2 * 100mL) wash, and use anhydrous sodium sulfate drying, and distilling off solvent.Residue is by ion exchange chromatography (diethylamino cross-linking dextran anion exchange resin (CH
3CN: H
2O, 1: 1) purification, go up purification by flash chromatography at silica gel (chloroform, 100%) then.Output 0.44g (63%), mp 148-150 ℃.
1H NMR (CDCl
3, 500MHz): δ 8.34 (d, J=2.5,1H), 8.12 (s, 1H), 7.40-7.12 (m, 10H), 6.91 (d, J=2.3,1H), 4.94 (s, 2H), 3.88 (s, 3H), 3.82 (s, 2H).
13C NMR (CDCl
3, 125MHz): δ 187.2,175.2, and 170.3,162.7,143.9,138.4,136.9,136.1,133.8,129.4,129.5,129.3,129.1,129.1,128.7,128.6,127.5,127.4,126.5,120.2,102.4,61.2,53.0,33.5.HRMS (M+H)
+Value of calculation C
24H
22NO
5404.1498, measured value 404.1497.
Step 7:4-(1,5-dibenzyl-1,4-dihydro-4-oxo pyridine-3-yl)-2-hydroxyl-4-oxo fourth-2 olefin(e) acid (16).
At 0 ℃, with 4-(1,5-dibenzyl-1,4-dihydro-4-oxo pyridine-3-yl)-2-hydroxyl-4-oxo but-2-ene acid methyl ester 15, (0.080g, 0.19mmol) mixture of NaOH (4mL) in THF (12mL) with 1N stirred 4 hours.THF is distilled away, and (2 * 25mL) extractions, (anhydrous Na is used in 1 * 25mL) washing to residue with saline solution with the HCl acidify of 1N and with EtOAc
2SO
4Drying is distilled away EtOAc and is obtained yellow solid.Thick solid grinds with ether, filters and vacuum drying.Last solid grinds with chloroform, filtration and vacuum drying 24 hours. output 0.065g (84%), yellow solid, mp 140-142 ℃.
1H NMR (CDCl
3+ MeOH-d
4, 500MHz): δ 3.80 (s, 2H, CH
2), 4.97 (s, 2H, CH
2), 6.95 (t, 1H, CH, J=1Hz), 7.13-7.40 (m, 11H, Ar-H and alkene CH), 8.36 (d, 1H, CH, J=2.5Hz).
13C NMR (CDCl
3, 125MHz): δ 33.4,61.2,120.5,126.5,127.5,127.6,128.6,128.7,128.7,129.1,129.1,129.2,129.2,129.2,129.4,133.8,135.9,137.2,138.2,143.8,163.8,175.4.HRMS (M+H)
+Value of calculation C
23H
20NO
5390.1341, measured value 390.1343.
Claims (56)
1. the chemical compound of general formula I or the acceptable salt of its pharmacy:
2-and 4-pyridone and regional isomer thereof that wherein said skeleton limits for this paper independently;
R
1And R
2Be H independently of one another; C
1-6Alkyl; C
1-6Fluoro-alkyl; Unsubstituted or substituted C
5-6Cycloalkyl; C
1-6Thiazolinyl; Unsubstituted or substituted phenyl; Unsubstituted or substituted benzyl; C
2-6Alkyl phenyl, described phenyl can be chosen wantonly and be substituted; Unsubstituted or substituted heteroaryl; The C that is replaced by heteroaryl
1-6Alkyl, described heteroaryl is optional to be substituted; C
1-6Alkyl S (O) R or alkyl (SO
2) R, wherein R is alkyl, phenyl or substituted phenyl; C
1-6Alkyl CO
2R
a, R wherein
aBe C
1-6Alkyl or H; C
1-6Alkyl COR
a', R wherein
a' be C
1-6Alkyl;
R
3And R
4Be independently selected from H, C
1-6Alkyl, halogen, hydroxyl, the unsubstituted or substituted thiophenyl of unsubstituted or substituted benzyl;
R
5Be CO
2R
cOr P (O) (OR
c) (OR
c), each R wherein
cBe independently selected from H and C
1-6Alkyl.
2. the chemical compound of claim 1 or the acceptable salt of its pharmacy, described chemical compound has following structure:
R wherein
1And R
2Be benzyl or the benzyl that replaced by 1~3 substituent group on aromatic ring independently of one another, described substituent group is selected from halogen, hydroxyl, methoxyl group, methyl, ethyl, propyl group, CF
3, or-CH
2R
bBase, wherein R
bBe 5-or 6-unit heteroaryl;
R
3And R
4Be H, C independently
1-6Alkyl, halogen, benzyl, substituted benzyl, thiophenyl or the thiophenyl that is replaced by 1~3 substituent group on phenyl ring, described substituent group is selected from halogen, hydroxyl, methoxyl group, methyl, ethyl, propyl group, CF
3
R wherein
5Be CO
2R, wherein R is selected from H and C
1-6Alkyl.
3. the chemical compound of claim 1 or the acceptable salt of its pharmacy, described chemical compound has following structure:
R wherein
1And R
2Be benzyl or the benzyl that replaced by 1~3 substituent group on aromatic ring independently of one another, described substituent group is selected from halogen, hydroxyl, methoxyl group, methyl, ethyl, propyl group, CF
3, or R wherein
1And R
2Be independently-CH
2R
b, R wherein
bIt is 5-or 6-unit hetero-aromatic ring;
R wherein
3And R
4Be H, C independently
1-6Alkyl, halogen, benzyl, substituted benzyl, thiophenyl or the thiophenyl that is replaced by 1~3 substituent group on phenyl ring, described substituent group is selected from halogen, methoxyl group, methyl, ethyl, propyl group, CF
3
R wherein
5Be P (O) (OR) (OR) that wherein said R base is identical or different, and is selected from H or C
1-6Alkyl.
4. the chemical compound of claim 1 or the acceptable salt of its pharmacy, described chemical compound has following structure:
R wherein
1And R
2Be the benzyl that is replaced by 1~3 substituent group on benzyl or the aromatic ring independently of one another, described substituent group is selected from halogen, hydroxyl, methoxyl group, methyl, ethyl, propyl group, CF
3, or-CH
2R
bBase, wherein R
bBe 5-or 6-unit heteroaryl;
R
3And R
4Be H, C independently
1-6Alkyl, halogen, benzyl, substituted benzyl, thiophenyl or have 1~3 substituent substituted thiophenyl on phenyl ring, described substituent group is selected from halogen, hydroxyl, methoxyl group, methyl, ethyl, propyl group, CF
3
R wherein
5Be CO
2R, wherein R is selected from H and C
1-6Alkyl.
5. the chemical compound of claim 1 or the acceptable salt of its pharmacy, described chemical compound has following structure:
R wherein
1And R
2Be the benzyl that is replaced by 1~3 substituent group on benzyl or the aromatic ring independently of one another, described substituent group is selected from halogen, hydroxyl, methoxyl group, methyl, ethyl, propyl group, CF
3, or R wherein
1And R
2Be independently-CH
2R
b, R wherein
bBe 5-or 6-unit hetero-aromatic ring;
R wherein
3And R
4Be H, C independently
1-6Alkyl, halogen, benzyl, substituted benzyl, thiophenyl or the thiophenyl that is replaced by 1~3 substituent group on phenyl ring, described substituent group is selected from halogen, methoxyl group, methyl, ethyl, propyl group, CF
3
R wherein
5Be P (O) (OR) (OR) that wherein R is identical or different, and is selected from H or C
1-6Alkyl.
6. the chemical compound of claim 1, it is selected from
4-(1,5-dibenzyl-1,2-dihydro-2-oxo-pyridin-3-yl)-2-hydroxyl-4-oxo but-2-ene acid;
4-(1,5-dibenzyl-1,4-dihydro-4-oxo pyridine-3-yl)-2-hydroxyl-4-oxo but-2-ene acid;
3-acetyl group-1,5-dibenzyl-3-pyridine-2 (1H)-ketone;
3-acetyl group-1,5-dibenzyl-1H-pyridine-4-ketone;
4-(1,5-dibenzyl-1,2-dihydro-2-oxo-pyridin-3-yl)-2-hydroxyl-4-oxo but-2-ene acid methyl ester; With
4-(1,5-dibenzyl-4-oxo-1,4-dihydro-pyridin-3-yl)-2-hydroxyl-4-oxo-but-2-ene acid methyl ester, or the acceptable salt of their pharmacy.
7. the chemical compound of claim 1, it is selected from
4-(1,5-dibenzyl-1,2-dihydro-2-oxo-pyridin-3-yl)-2-hydroxyl-4-oxo but-2-ene acid; With
4-(1,5-dibenzyl-1,4-dihydro-4-oxo pyridine-3-yl)-2-hydroxyl-4-oxo but-2-ene acid, or
The acceptable salt of their pharmacy.
8. the chemical compound of claim 1 or the acceptable salt of its pharmacy, described chemical compound has following structure:
R wherein
1And R
2Be benzyl or the benzyl that replaced by 1~3 substituent group on phenyl ring independently, described substituent group is selected from fluorine, chlorine, C
1-4Alkyl, C
2-4Thiazolinyl and methoxyl group;
R
3Be H, C
1-3Alkyl, C
2-3Thiazolinyl, fluorine, chlorine or methoxyl group;
R
4Be H, F, Cl or OH; With
R
5Be CO
2H or P (O) are (OH)
2
9. the chemical compound of claim 1, wherein R
1And R
2In at least one is a benzyl.
10. the chemical compound of claim 1, wherein R
1And R
2Be benzyl.
11. the chemical compound of claim 8, wherein R
1And R
2Be benzyl.
12. each chemical compound, wherein R among claim 1-5 and the 8-11
3And R
4Be H, methyl, fluorine or chlorine independently.
13. each chemical compound, wherein R among claim 1-5 and the 8-12
3And R
4Be H, fluorine or chlorine independently.
14. each chemical compound, wherein R among claim 1-5 and the 8-13
3And R
4H respectively does for oneself.
15. each chemical compound, wherein R among claim 1-5 and the 8-14
5Be CO
2H, or the acceptable salt of its pharmacy.
16. pharmaceutical composition comprises among the claim 1-15 that treats effective dose each chemical compound and pharmaceutically acceptable carrier, additive or excipient.
17. the property rights profit requires 16 pharmaceutical composition, wherein said compositions suppresses the hiv integrase among the human host, and described hiv integrase is wild type and mutant.
18. pharmaceutical composition, first chemical compound that comprises among the claim 1-15 that treats effective dose each, at least a other combination of compounds with the treatment effective dose, and pharmaceutically acceptable carrier, additive or excipient, described other chemical compound is selected from i) other anti-hiv agent, the ii) anti-infective except anti-hiv agent, iii) immunomodulator, iv) other is selected from the composition of medicine in the table shown in the description 17-28 page or leaf.
19. the compositions of claim 18, wherein said anti-infective are antiviral agent, it is selected from protease inhibitor, reverse transcriptase inhibitors, other integrase inhibitor or its combination.
20. the compositions of claim 19, wherein said reverse transcriptase inhibitors are nucleoside compound.
21. the compositions of claim 19, wherein said reverse transcriptase inhibitors are the non-nucleoside chemical compound.
22. the compositions of claim 19, wherein said other integrase inhibitor are the chemical compound of non-pyrimidinone compound.
23. each compositions among the claim 16-22, it is oral or parenteral dosage form.
24. each compositions among the claim 16-22, it is mixed with the suction spraying or rectal suppository is used for administration.
25. the method for a pharmaceutical compositions, described method comprise with among the claim 1-15 each chemical compound and pharmaceutically acceptable carrier, additive or excipient composition with the preparation mixture, and prepare oral or parenteral dosage form from described mixture.
26. treat the method that patient HIV infects for one kind, described method comprises in the claim 16-24 of described patient's effective dosage each compositions.
27. a minimizing has the patient's of HIV infection risk the method for HIV infection potential, described method comprises in the claim 16-24 of described patient's effective dosage each compositions.
28. a treatment has the patient's of AIDS or ARC method, comprises in the claim 16-24 of described patient's drug treatment effective dose each compositions.
29. a method that suppresses experimenter's hiv integrase, described method comprise in the claim 16-24 of described experimenter's drug treatment effective dose each compositions.
30. each method among the claim 26-29, wherein said experimenter is the people.
31. each method among the claim 26-30, wherein said anti-HIV or other drug are listed chemical compound in the description 17-28 page or leaf invading the exterior.
32. treat the method that human host HIV infects, comprise compositions for one kind to described host's administration claim 27.
33. the method for claim 32, wherein said compositions comprises the chemical compound of effective dose
34. pharmaceutical composition, comprise among the claim 1-15 of effective dose each first chemical compound and at least a anti-HIV-1 compounds of effective dose or description 17-28 page or leaf invading the exterior in other listed combination of compounds, and with the combination of pharmaceutically acceptable carrier, additive or excipient.
35. claim 16,18 or 34 pharmaceutical composition, wherein said chemical compound is
36. the pharmaceutical composition of claim 16 also comprises at least a other chemical compound, described chemical compound is selected from (-) beta-dioxolane-G (DXG); (-) β-arctigenin (arctigenin); (-)-Carbovir (-)-C-D4G; (-)-2 ', 3 '-dideoxy-5-fluoro-3 '-thia cytidine (FTC); (-)-β-D-2,6-diaminopurine dioxolanes (DAPD); (+)-2 '-deoxidation-3 '-oxa--4 '-sulfo-cytidine (dOTC+); (+)-2 '-deoxidation-3 '-oxa--4 '-sulfo--5-fluorine cytidine (dOTFC+); (+/-)-Lobucavir;
(R)-and 2QuinCOAsnPhe[CHOHCH2] PipCONHtBu; (R)-3,6-diamino-N-(amino methyl) caproamide (Bellenamine); (R)-9-(2-phosphonium mesitoyl methoxy propyl group) adenine (tenofovir); (R)-PMPDAP; (S)-9-(2-phosphonium mesitoyl methoxy propyl group) adenine ((S)-PMPA); PMPA (S); α-APA (loviride); R87232; R88703; α-APA enantiomer (R90385);
α-L-AZT; α-L-dioxolanes-C (α-L-DXC); α-L-FTC;
α-single methyl fluoride dehydrogenation ornithine methyl ester (MFMOME); 1,1 '-Celogen Az (ADA); 1-(11-octyl group amino-10-hydroxyl undecyl)-3,7-dimethyl xanthine (CT-2576);
1-(2 ', 3 '-dideoxy-2 '-fluoro-beta-D-threo form-penta furyl glycosyl) cytosine (Ro 31-6840);
1-(2 '-fluoro-2 ', 3 '-dideoxy-β-D-erythro-penta furyl glycosyl) thymus pyrimidine (2 ' FddT);
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(3-aminomethyl phenyl) sulfenyl) thymus pyrimidine (HEPT-M);
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(thiophenyl)-2-thio-thymine (HEPT-S);
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(thiophenyl) thymus pyrimidine (HEPT);
Deoxidation nojirimycin (1-deoxidation nojirimycin); Amprenavir; Abacavir succinate (match is advanced); 1-amino oxygen base ethamine (AEA); 1-methoxyl group oxalyl group-3, and the 5-dicaffeoylquinic acid (1-MO-3,5-DCQA); 1OH-2 (Cbz-Tle) 3PhPr[14] the adjacent formic acid derivates of two Parylenes; 1OH-2 (Cbz-ValNH) 3PhPr[13] the adjacent formic acid derivates of dimerization meta-xylene; 1OH-2 (Cbz-ValNH) 3PhPr[13] the adjacent formic acid derivates of two Parylenes;
1OH-2 (Cbz-ValNH) 3PhPr[14] the adjacent formic acid derivates of two Parylenes; 1OH-2 (Cbz-ValNH) 3PhPr[17] the adjacent formic acid derivates of two Parylenes; 12-deoxidation phorbol-13-(3E, 5E-decadinene acid esters); 16. α-bromine epiandrosterone (Epi-Br) or (Inactivin); 1-β-D-arabinofuranosyl adenin glycosyl-5-(2-bromo vinyl) uracil (Sorivudine); 2 ', 3 '-two dehydrogenations-3 '-deoxycytidine (D4C);
2 ', 3 '-dideoxy two dehydrogenation guanosines (D4G); 2 ', 3 '-two dehydrogenations-3 '-deoxyribosylthymine (D4T) (stavudine); 2 ', 3 '-dideoxy-3 '-fluoro-4-sulfo-thymidine (3 '-F-4-Thio-ddT);
2 ', 3 '-dideoxy-3 '-fluoro-5-broxuridine (FddBrU); 2 ', 3 '-dideoxy-3 '-fluoro-5-5-chloro-5-deoxyarabinosylcytosine (3 '-F-5-Cl-ddC); 2 ', 3 '-dideoxy-3 '-fluoro-5-chloriduria glycosides (935U83) (raluridine); 2 ', 3 '-dideoxy-5-ethyl cytidine (5-Et-ddC); 2 ', 3 '-DIDEOXYADENOSINE (ddA);
2 ', 3 '-dideoxy two dehydrogenation adenosines (d4A); 2 ', 3 '-dideoxy guanosine (ddG);
2 ', 3 '-dideoxy-3 '-hydroxymethyl cytidine (3 '-hydroxymethyl-ddC); 2,5 '-dehydration-3 '-azido-2 ', 3 '-di-deoxyuridine (AZU-2,5 '-dehydration); 2,5 '-dehydration-3 '-azido-3 '-deoxyribosylthymine (AZT-2,5 '-dehydration); 2 ', 5 ' diSilySpiroT (TSAO-T); 2 ', 5 ' diSilySpiroT (TSAO-me^3T); 2,6-diaminourea-2 ', 3 '-dideoxy purine-9-ribofuranoside (ddDAPR) (2, the 6-diaminourea-ddP); 2,6-diaminopurine-2 ', 3 '-dideoxy two dehydrogenation nucleoside (ddeDAPR); 2,6-diaminopurine-3 '-fluoro-2 ', 3 '-di-deoxynucleoside (3 '-F-ddDAPR); 2-aminobenzyl statine valyl Cbz derivant; 2-glycine amide-5-chlorphenyl 2-pyrrolyl ketone (GCPK); [2-PyridCH2NCH3CO-Val-NHCH (Bz)] CHOHCHOH (A-77003); 2 '-azido-2 ', 3 '-DIDEOXYADENOSINE (2 '-N3ddA); 2 '-F-dd-ara-A (Lodensine); 2 '-FddT; 2 '-N3ddA; 2 '-N3ddA (β-D-threo form); 2-NaphCOAsnPhe[CHOHCH2] Pro-OtBu; 2-nitrobenzophenone phenylsulfone (NPPS); 3-(3-oxo-1-acrylic)-3 '-azido-3 '-deoxyribosylthymine (3-(3-oxo-1-acrylic) AZT); 3-(3-oxo-1-acrylic) AZT; L-737,126; 3, and the 5-dicaffeoylquinic acid (3,5-DCQA); 3 '-azido-3 '-deoxidation-6-azathymidine; 3 '-azido-2 ', 3 '-dideoxy-5-[(cyano methyl) the oxygen base] uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-aminouridine; 3 '-azido-2 ', 3 '-the assorted uridnine of dideoxy-5-azepine-6-denitrification; 3 '-azido-2 ', 3 '-dideoxy-5-broxuridine; 3 '-azido-2 ', 3 '-dideoxy-5-5-chloro-5-deoxyarabinosylcytosine (3 '-Az-5-Cl-ddC); 3 '-azido-2 ', 3 '-dideoxy-5-dimethylamino uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-ethyl uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-fluorine cytidine; 3 '-azido-2 ', 3 '-dideoxy-5-floxuridine; 3 '-azido-2 ', 3 '-dideoxy-5-hydroxyuridine; 3 '-azido-2 ', 3 '-dideoxy-5-iodo uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-methylamino uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-methylcytidine; 3 '-azido-2 ', 3 '-dideoxy-5-thiocyano uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-trifluoromethyl uridnine; 3 '-azido-2 ', 3 '-zalcitabine; 3 '-azido-2 ', 3 '-the dideoxy guanosine; 3 '-azido-2 ', 3 '-dideoxy-N4--5-dimethyl cytidine; 3 '-azido-2 ', 3 '-dideoxy-N4-OH-5-methylcytidine; 3 '-azido-2 ', 3 '-di-deoxyuridine (Uravidine); 3 '-azido-3 '-deoxidation-6-azathymidine; 3-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-adenylic acid; 3 '-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-adenylic acid, 2-cyano ethyl ester; 3 '-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-inosinic acid (AZT-P-ddI); 3 '-azido-3 '-deoxyribosylthymine-5 '-(butyl methoxyl group valine) phosphate ester; 3 '-azido-5-chloro-2 ', 3 '-di-deoxyuridine; 3 '-deoxyribosylthymine (ddT); 9-(3 '-fluoro-2 ', 3 '-dideoxy-β-D-erythro penta furyl glycosyl) adenine;
3 '-fluoro-2 ', 3 '-dideoxy-5-iodo uridnine (FddIU); 3 '-fluoro-2 ', 3 '-zalcitabine (3 '-FddC); 3 '-fluoro-2 ', 3 '-the dideoxy guanosine (3 '-FddG); 3 '-fluoro-2 ', 3 '-di-deoxyuridine (3 '-FddU); 9-(3 '-azido-2 ', 3 '-dideoxy-β-D-erythro penta furyl glycosyl) adenine; 3TC (lamivudine); 3TC﹠amp; AZT (Combivir); 4 '-acetylamino phenyl 4-guanidine benzoate; 4 '-azido-3 '-deoxyribosylthymine; 4 '-azido-5-chloro-2 '-BrdU; 4 '-azido-2 '-deoxyadenosine; 4 '-azido-2 '-deoxycytidine; 4 '-azido-2 '-deoxyguanosine; 4 '-azido-2 '-deoxyinosine; 4 '-azido-2 '-BrdU; 4 '-azido breast glycosides; 4 '-cyano group breast glycosides; 4-methyl-5-(pyrazinyl)-3H-1,2-dithia cyclopentenes-3-thioketone (oltipraz); 5 '-[(1,4-dihydro-1-methyl-3-pyridine radicals carbonyl) oxygen base]-3 '-azido-2 ', 3 '-deoxyribosylthymine (DP-AZT); 5 '-[[(Z)-and 4-amino-crotyl] methylamino]-5 '-deoxyadenosine (MDL 73811); 5 '-alkyl polyglucoside carbonic ester of 3 '-azido-3 '-deoxyribosylthymine; 5Cl3PhS-2 indole CONH2; 5-fluoro-2 ', 3 '-zalcitabine; 5-methyl-3 '-azido-2 ', 3 '-the different cytidine of dideoxy; Celgosivir; 6-chloro-9-(2,3-dideoxy-β-D-glycerol penta furyl glycosyl)-9H-purine; 6-dimethylaminopurine-2 ', 3 '-di-deoxynucleoside; Ro 24-7429; Ro 5-3335; Tivirapine; 9-(2,3-dideoxy-β-D-ribofuranosyl)-6-(methyl mercapto) purine; 9-(2 '-azido-2 ', 3 '-dideoxy-B-D-threo form penta furyl glycosyl) adenine; C-Europe tower mycin A; (+-) Lobucavir; A-76890; A-77003; A-77212; A-80987; A-81525; A-83962; A-98881; PNU-104489; Three associations only; Lopinavir; Kaletra; Lopinavir and ritonavir;
With the promise Wei; Azodicarboamide; Adefovirdipivoxil; Adefovir dipivoxil
Nelfinavir; AG1350 (LY316957); R-87366; Alpha-lipoic acid; Alovudine (3 '-FddT); ALX40-4C; AMD3100 (JM3100); Amdoxovir (APD); Phosphoric acid amprenavir (fosamprenavir); Ancer 20 (Z-100); Atazanavir (Latazanavir); Ah 's dimension is fixed; The aurintricarboxylic acid; AY 9944; 3 '-azido-5-chloro-2 ', 3 '-di-deoxyuridine; AZT; α-L-AZT; O, O '-two (3 '-azido-3 '-methyl phosphonate of deoxyribosylthymine-5 '-yl); Baicalin (TJN-151); Belulinic acid Betulinic acid (Mairin); Belulinic acid Betulinic acid, 3-O-(3 ', 3 '-the dimethyl succinate ester); Delavirdine (U-90152); U-g8204E; Nevirapine; BILA 1906 BS; BILA2011 BS (palinavir); BILA 2185 BS; NSC633001; CGP 53820; Two-ValHOEt-N2aza-peptide isostere (CGP 53820 analog); BMS-186318; L-687,908; Brovavir; BzOCValPhe[diCHOH (RR)] PheValBzOC; BzOCValPhe[diCHOH (SS)] PheValBzOC; C2-Sym phosphonic amide derivant (HOECHSTAG); NSC675451; Calanolide B; Capravirine (S-1153); Carbovir; Castanospermine; CGP 61755 (LASINAVIR BMS-234475 Lasinavir [INN); CGP 64222; CNI-H0294; Emivirine; Conocurvone (NSC650891); Emtricitabine; C-Oxetanocin-G; Indinavir; The sulfogel polysaccharide; Blue algae antiviral protein-N; SD146; Cyclosporin A; SDZ NIM 811; L-2 ', 3 '-two dehydrogenations-2 ', 3 '-DIDEOXYADENOSINE (L-D4A); 2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy-5-fluorine cytidine (DD4C); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy-5-fluorine cytidine (LD4C); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy guanosine (LD4G); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-didanosine (LD4I); DABO; DdI; DdC; DMP-323; DMP-450; (-)-2 '-deoxidation-3 '-oxa--4 '-the sulfo-cytidine; (-)-2 '-deoxidation-3 '-oxa--4 '-sulfo--5-flurocytosine; Pentafuside (Enfuvirtide); Etoposide; Efavirenz; Emtriva; K-12 (fluorine quinoline); Saquinavir; Foscarnet; Phosphine formic acid; Foscarnet sodium; FPMDAP; FPMPA; FPMPG; Gene Expression Modulator 91 (GEM91); Hammerhead shape resists-gagRNA formation enzyme B; Harziphilone; HBY 097 (quinoxaline derivant); E-EBU; E-EPSeU; E-EPU; NSC 648400; E-EBU-dM; Zalcitabine; LY326188; Ingenol 3,5,20-triacetate (ITA); Calophylloide B; KNI-272; RD3-2118; KNI-102; KNI-154; KNI-174; KNI-227; L-685,434; L-689,502; L-697,593; L-697,639; L-697,661; LY289612; Trovirdine; LY-73497; L-735,524; N-ethyl-2 ', 3 '-DIDEOXYADENOSINE; N6-methyl-2 ', 3 '-DIDEOXYADENOSINE; Noa-Asn-Apns-Thz-NH-tBu; Nonoxinol 9; Ritonavir; NSC625487; NSC649324; NSC650898; UC-38; UC-84; P9941; Palinavir; The sulphuric acid pentosan; Elmiron; SP54; PNU-140690 (tipranavir); S-2720; R14458; R82150; R82913; R86183; RD4-2138; Resobene; Reyataz; Ribavirin; 7-chloro-N-methyl-5-(1H-pyrroles-2-yl)-3H-1, the 4-benzodiazepine
-2-amine; 7-chloro-5-(2-pyrrole radicals)-3H-1, the 4-benzodiazepine
-2 (H)-ketone; LY314163; SB-205569; Compound E; SD-095345SD146; SDZ PRI 053; SPC3; Naganol; T22; Thalidomide; Thiangazole; Thiazole and iso-indoles-5-ketone; U-104489; U-140690; U-87201E; U-88204E; UC-781; VB-11,328; VX-478; 141W94; XM-323 and composition thereof.
37. the pharmaceutical composition of claim 16 also comprises other chemical compound, described other chemical compound is selected from ACV; AK602; AMD070; APV; ATV; ATZ; AVX754 (apricitabine); AZT; Abacavir; Abacavir/lamivudine/zidovudine; Abacavir sulfate; Abacavir sulfate/lamivudine; Abacavir/lamivudine; Abelecet; Aciclovir; Adefovir dipivoxil; Amycin; Agenerase; Aldesleukin; Alovudine; Aluvia; Ambisome; Amdoxovir; Amphocin; Amphotec; Amphotericin B; Polyinosini; Amprenavir; Androderm; Androgel; Apricitabine; Aptivus; Atazanavir; Atripla; Azithromycin; BMS-378806; BMS-488043; Bactrim; Baraclude; Bevirimat; Biaxin; Brecanavir; BufferGel; C31G; CD4-IgG2; CS; CV-N; Calanolide A; Calcium hydroxyapatite; Carbopol 974P; Carrageenan; Carraguard; Sulfate cellulose; Clarithromycin; Combivir; Copegus; Sulfamethoxazole; Crixivan; Blue algae antiviral protein-N; Cymevene; DAPD; DLV; DS; Darunavir; Delavirdine; The Depo-testosterone; Dextran sulfate; Didanosine; Fluconazole; Doxil; Doxorubicin (liposome); Dronabinol; EFV; Efavirenz; Elvucitabine; Emtricitabine; The tenofovir disoproxil fumarate; Emtriva; Enfufirtide; Entecavir; Lamivudine; Epoetin Alfa; Epogen; Epzicom; Etopophos (phosphate); Etoposide; Etravirine; FTC; Fluconazol; Fortovase; Fosamprenavir; Foxivudine tidoxil; Fungizone; Fuzeon; GS 9137; GSK-873,140 (aplaviroc); GW433908; GW640385 (brecanavir); Ganciclovir; Immunoglobulin; Growth hormone (people); Hepsera; Hivid; The human growth hormone; IL-2; INH; Immunoglobulin, intravenous (people); Indinavir; Interferon; Interleukin-2, recombinant, people; Recombinant Interferon (2b); Invirase; Isoniazid; Itraconazole; KP-1461; Lamivudine/zidovudine; Lexiva; Lopinavir/ritonavir; MK-0518; Nebupent; Nelfinavir; Neutrexin; Nevirapine; Nuo Wei; Nydrazid; Peptide T; PMPA prodrug (Viread) ' Prezista (Darunavir); PRO 140; PRO 2000; PRO 542 (CD4IGg2); Procrit (Epoetin); Aldesleukin; Racivir; Radiesse; Rrebetol; Delavirdine; Zidovudine; Reyataz; Ribavirin; Rifabutin; Rifadin; Rifampicin; Rimactane; Ritonavir; Rodferon-A (2a); Saquinavir; SCH-D (vicriviroc); Growth hormone; Stavudinie; Sulfamethoxazole/trimethoprim; Testosterone; Sustiva; TNX-355; Taxol; Tenofovir; The tenofovir disoproxil fumarate; Testosterone; Tipranavir; Toposar; Trimetrexate; Three associations only; Truvada (Emtriva and Viread combination); U-90152S (Delaviridine); UC-781; UK-427,857 (maraviroc); Valcyte; Valganciclovir; Valproic acid; Fan Bishi; Vicriviroc; Videx; Viracept see nelfinaivr (Tennofovir DF); The happy life of dimension; Virazole; Viread; Vitrasert; Zalcitabine; Sai Ruite; Match is advanced; Zidovudine; Zithromax; Shu Wei treats and composition thereof.
38. each compositions among the claim 34-37, wherein said compositions is treated human host's described HIV and is infected by suppressing hiv integrase at least, and described intergrase is wild type and mutant.
39. each compositions among the claim 34-38, it is oral or parenteral dosage form.
40. each compositions among the claim 34-38, it is mixed with the suction spraying or rectal suppository is used for administration.
41. treat the method that patient HIV infects for one kind, described method comprises in the claim 34-40 of described patient's effective dosage each compositions.
42. a minimizing has the patient's of HIV infection risk the method for HIV infection potential, described method comprises in the claim 34-40 of described patient's effective dosage each compositions.
43. a treatment has the patient's of AIDS or ARC method, comprises in the claim 34-40 of described patient's drug treatment effective dose each compositions.
44. a method that suppresses experimenter's hiv integrase, described method comprise in the claim 34-40 of described experimenter's drug treatment effective dose each compositions.
45. each method among the claim 41-44, wherein said experimenter is the people
46. each compositions is used for the treatment of purposes in patient's the medicine of HIV in preparation among claim 16-24 and the 34-40.
47. each compositions is used for reducing the purposes that the patient contacts the medicine of HIV possibility of infection in preparation among claim 16-24 and the 34-40.
48. each compositions is used for the treatment of purposes in the medicine of the patient with AIDS or ARC in preparation among claim 16-24 and the 34-30.
49. each compositions is used for suppressing the purposes of medicine of experimenter's hiv integrase among claim 16-24 and the 34-40 in preparation.
50. the purposes of claim 46-49, wherein said experimenter is people patient.
51. the method that treatment human host's HIV infects, comprise first chemical compound and the acceptable salt of pharmacy thereof to the following structure of described host's combination medicine-feeding effective dose, with the combination of at least a other chemical compound and composition thereof, also make up pharmaceutically acceptable carrier, additive or excipient:
2-and 4-pyridone and regional isomer thereof that skeleton described in the formula I limits for this paper independently;
R
1And R
2Be H independently of one another; C
1-6Alkyl; C
1-6Fluoro-alkyl; Unsubstituted or substituted C
5-6Cycloalkyl; C
1-6Thiazolinyl, unsubstituted or substituted phenyl; Unsubstituted or substituted benzyl; C
2-6Alkyl phenyl, described phenyl can be chosen wantonly and be substituted; Unsubstituted or substituted heteroaryl; The C that is replaced by heteroaryl
1-6Alkyl, described heteroaryl is optional to be substituted; C
1-6Alkyl S (O) R or alkyl (SO
2) R, wherein R is alkyl, phenyl or substituted phenyl; C
1-6Alkyl CO
2R
a, R wherein
aBe C
1-6Alkyl or H, C
1-6Alkyl COR
a', R wherein
a' be C
1-6Alkyl;
R
3And R
4Be independently selected from H, C
1-6Alkyl, halogen, hydroxyl, the unsubstituted or substituted thiophenyl of unsubstituted or substituted benzyl;
R
5Be CO
2R
cOr P (O) (OR
c) (OR
c), each R wherein
cBe independently selected from H and C
1-6Alkyl,
Described other chemical compound is selected from: (-) beta-dioxolane-G (DXG); (-) β-arctigenin (arctigenin); (-)-Carbovir (-)-C-D4G; (-)-2 ', 3 '-dideoxy-5-fluoro-3 '-thia cytidine (FTC); (-)-β-D-2,6-diaminopurine dioxolanes (DAPD); (+)-2 '-deoxidation-3 '-oxa--4 '-sulfo-cytidine (dOTC+); (+)-2 '-deoxidation-3 '-oxa--4 '-sulfo--5-fluorine cytidine (dOTFC+); (+/-)-Lobucavir; (R)-and 2QuinCOAsnPhe[CHOHCH2] PipCONHtBu; (R)-3,6-diamino-N-(amino methyl) caproamide (Bellenamine); (R)-9-(2-phosphonium mesitoyl methoxy propyl group) adenine (tenofovir); (R)-PMPDAP; (S)-9-(2-phosphonium mesitoyl methoxy propyl group) adenine ((S)-PMPA); PMPA (S); α-APA (loviride); R87232; R88703; α-APA enantiomer (R90385);
α-L-AZT; α-L-dioxolanes-C (α-L-DXC); α-L-FTC;
α-single methyl fluoride dehydrogenation ornithine methyl ester (MFMOME); 1,1 '-Celogen Az (ADA); 1-(11-octyl group amino-10-hydroxyl undecyl)-3,7-dimethyl xanthine (CT-2576);
1-(2 ', 3 '-dideoxy-2 '-fluoro-beta-D-threo form-penta furyl glycosyl) cytosine (Ro 31-6840);
1-(2 '-fluoro-2 ', 3 '-dideoxy-β-D-erythro-penta furyl glycosyl) thymus pyrimidine (2 ' FddT);
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(3-aminomethyl phenyl) sulfenyl) thymus pyrimidine (HEPT-M);
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(thiophenyl)-2-thio-thymine (HEPT-S);
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(thiophenyl) thymus pyrimidine (HEPT);
Deoxidation nojirimycin (1-deoxidation nojirimycin); Amprenavir; Abacavir succinate (match is advanced); 1-amino oxygen base ethamine (AEA); 1-methoxyl group oxalyl group-3, and the 5-dicaffeoylquinic acid (1-MO-3,5-DCQA); 1OH-2 (Cbz-Tle) 3PhPr[14] the adjacent formic acid derivates of two Parylenes; 1OH-2 (Cbz-ValNH) 3PhPr[13] the adjacent formic acid derivates of dimerization meta-xylene; 1OH-2 (Cbz-ValNH) 3PhPr[13] the adjacent formic acid derivates of two Parylenes;
1OH-2 (Cbz-ValNH) 3PhPr[14] the adjacent formic acid derivates of two Parylenes; 1OH-2 (Cbz-ValNH) 3PhPr[17] the adjacent formic acid derivates of two Parylenes; 12-deoxidation phorbol-13-(3E, 5E-decadinene acid esters); 16. α-bromine epiandrosterone (Epi-Br) or (Inactivin); 1-β-D-arabinofuranosyl adenin glycosyl-5-(2-bromo vinyl) uracil (Sorivudine); 2 ', 3 '-two dehydrogenations-3 '-deoxycytidine (D4C);
2 ', 3 '-dideoxy two dehydrogenation guanosines (D4G); 2 ', 3 '-two dehydrogenations-3 '-deoxyribosylthymine (D4T) (stavudine); 2 ', 3 '-dideoxy-3 '-fluoro-4-sulfo-thymidine (3 '-F-4-Thio-ddT);
2 ', 3 '-dideoxy-3 '-fluoro-5-broxuridine (FddBrU); 2 ', 3 '-dideoxy-3 '-fluoro-5-5-chloro-5-deoxyarabinosylcytosine (3 '-F-5-Cl-ddC); 2 ', 3 '-dideoxy-3 '-fluoro-5-chloriduria glycosides (935U83) (raluridine); 2 ', 3 '-dideoxy-5-ethyl cytidine (5-Et-ddC); 2 ', 3 '-DIDEOXYADENOSINE (ddA);
2 ', 3 '-dideoxy two dehydrogenation adenosines (d4A); 2 ', 3 '-dideoxy guanosine (ddG);
2 ', 3 '-dideoxy-3 '-hydroxymethyl cytidine (3 '-hydroxymethyl-ddC); 2,5 '-dehydration-3 '-azido-2 ', 3 '-di-deoxyuridine (AZU-2,5 '-dehydration); 2,5 '-dehydration-3 '-azido-3 '-deoxyribosylthymine (AZT-2,5 '-dehydration); 2 ', 5 ' diSilySpiroT (TSAO-T); 2 ', 5 ' diSilySpiroT (TSAO-me^3T); 2,6-diaminourea-2 ', 3 '-dideoxy purine-9-ribofuranoside (ddDAPR) (2, the 6-diaminourea-ddP); 2,6-diaminopurine-2 ', 3 '-dideoxy two dehydrogenation nucleoside (ddeDAPR); 2,6-diaminopurine-3 '-fluoro-2 ', 3 '-di-deoxynucleoside (3 '-F-ddDAPR); 2-aminobenzyl statine valyl Cbz derivant; 2-glycine amide-5-chlorphenyl 2-pyrrolyl ketone (GCPK); [2-PyridCH2NCH3CO-Val-NHCH (Bz)] CHOHCHOH (A-77003); 2 '-azido-2 ', 3 '-DIDEOXYADENOSINE (2 '-N3ddA); 2 '-F-dd-ara-A (Lodensine); 2 '-FddT; 2 '-N3ddA; 2 '-N3ddA (β-D-threo form); 2-NaphCOAsnPhe[CHOHCH2] Pro-OtBu; 2-nitrobenzophenone phenylsulfone (NPPS); 3-(3-oxo-1-acrylic)-3 '-azido-3 '-deoxyribosylthymine (3-(3-oxo-1-acrylic) AZT); 3-(3-oxo-1-acrylic) AZT; L-737,126; 3, and the 5-dicaffeoylquinic acid (3,5-DCQA); 3 '-azido-3 '-deoxidation-6-azathymidine; 3 '-azido-2 ', 3 '-dideoxy-5-[(cyano methyl) the oxygen base] uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-aminouridine; 3 '-azido-2 ', 3 '-the assorted uridnine of dideoxy-5-azepine-6-denitrification; 3 '-azido-2 ', 3 '-dideoxy-5-broxuridine; 3 '-azido-2 ', 3 '-dideoxy-5-5-chloro-5-deoxyarabinosylcytosine (3 '-Az-5-Cl-ddC); 3 '-azido-2 ', 3 '-dideoxy-5-dimethylamino uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-ethyl uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-fluorine cytidine; 3 '-azido-2 ', 3 '-dideoxy-5-floxuridine; 3 '-azido-2 ', 3 '-dideoxy-5-hydroxyuridine; 3 '-azido-2 ', 3 '-dideoxy-5-iodo uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-methylamino uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-methylcytidine; 3 '-azido-2 ', 3 '-dideoxy-5-thiocyano uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-trifluoromethyl uridnine; 3 '-azido-2 ', 3 '-zalcitabine; 3 '-azido-2 ', 3 '-the dideoxy guanosine; 3 '-azido-2 ', 3 '-dideoxy-N4--5-dimethyl cytidine; 3 '-azido-2 ', 3 '-dideoxy-N4-OH-5-methylcytidine; 3 '-azido-2 ', 3 '-di-deoxyuridine (Uravidine); 3 '-azido-3 '-deoxidation-6-azathymidine; 3-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-adenylic acid; 3 '-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-adenylic acid, 2-cyano ethyl ester; 3 '-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-inosinic acid (AZT-P-ddI); 3 '-azido-3 '-deoxyribosylthymine-5 '-(butyl methoxyl group valine) phosphate ester; 3 '-azido-5-chloro-2 ', 3 '-di-deoxyuridine; 3 '-deoxyribosylthymine (ddT); 9-(3 '-fluoro-2 ', 3 '-dideoxy-β-D-erythro penta furyl glycosyl) adenine;
3 '-fluoro-2 ', 3 '-dideoxy-5-iodo uridnine (FddIU); 3 '-fluoro-2 ', 3 '-zalcitabine (3 '-FddC); 3 '-fluoro-2 ', 3 '-the dideoxy guanosine (3 '-FddG); 3 '-fluoro-2 ', 3 '-di-deoxyuridine (3 '-FddU); 9-(3 '-azido-2 ', 3 '-dideoxy-β-D-erythro penta furyl glycosyl) adenine; 3TC (lamivudine); 3TC﹠amp; AZT (Combivir); 4 '-acetylamino phenyl 4-guanidine benzoate; 4 '-azido-3 '-deoxyribosylthymine; 4 '-azido-5-chloro-2 '-BrdU; 4 '-azido-2 '-deoxyadenosine; 4 '-azido-2 '-deoxycytidine; 4 '-azido-2 '-deoxyguanosine; 4 '-azido-2 '-deoxyinosine; 4 '-azido-2 '-BrdU; 4 '-azido breast glycosides; 4 '-cyano group breast glycosides; 4-methyl-5-(pyrazinyl)-3H-1,2-dithia cyclopentenes-3-thioketone (oltipraz); 5 '-[(1,4-dihydro-1-methyl-3-pyridine radicals carbonyl) oxygen base]-3 '-azido-2 ', 3 '-deoxyribosylthymine (DP-AZT); 5 '-[[(Z)-and 4-amino-crotyl] methylamino]-5 '-deoxyadenosine (MDL 73811); 5 '-alkyl polyglucoside carbonic ester of 3 '-azido-3 '-deoxyribosylthymine; 5Cl3PhS-2 indole CONH2; 5-fluoro-2 ', 3 '-zalcitabine; 5-methyl-3 '-azido-2 ', 3 '-the different cytidine of dideoxy; Celgosivir; 6-chloro-9-(2,3-dideoxy-β-D-glycerol penta furyl glycosyl)-9H-purine; 6-dimethylaminopurine-2 ', 3 '-di-deoxynucleoside; Ro 24-7429; Ro 5-3335; Tivirapine; 9-(2,3-dideoxy-β-D-ribofuranosyl)-6-(methyl mercapto) purine; 9-(2 '-azido-2 ', 3 '-dideoxy-B-D-threo form penta furyl glycosyl) adenine; C-Europe tower mycin A; (+-) Lobucavir; A-76890; A-77003; A-77212; A-80987; A-81525; A-83962; A-98881; PNU-104489; Three associations only; Lopinavir; Kaletra; Lopinavir and ritonavir;
With the promise Wei; Azodicarboamide; Adefovirdipivoxil; Adefovir dipivoxil
Nelfinavir; AG1350 (LY316957); R-87366; Alpha-lipoic acid; Alovudine (3 '-FddT); ALX40-4C; AMD3100 (JM3100); Amdoxovir (APD); Phosphoric acid amprenavir (fosamprenavir); Ancer 20 (Z-100); Atazanavir (Latazanavir); Ah 's dimension is fixed; The aurintricarboxylic acid; AY 9944; 3 '-azido-5-chloro-2 ', 3 '-di-deoxyuridine; AZT; α-L-AZT; O, O '-two (3 '-azido-3 '-methyl phosphonate of deoxyribosylthymine-5 '-yl); Baicalin (TJN-151); Belulinic acid Betulinic acid (Mairin); Belulinic acid Betulinic acid, 3-O-(3 ', 3 '-the dimethyl succinate ester); Delavirdine (U-90152); U-88204E; Nevirapine; BILA 1906 BS; BILA 2011BS (palinavir); BILA 2185BS; NSC633001; CGP 53820; Two-ValHOEt-N2aza-peptide isostere (CGP 53820 analog); BMS-186318; L-687,908; Brovavir; BzOCValPhe[diCHOH (RR)] PheValBzOC; BzOCValPhe[diCHOH (SS)] PheValBzOC; C2-Sym phosphonic amide derivant (HOECHSTAG); NSC675451; Calanolide B; Capravirine (S-1153); Carbovir; Castanospermine; CGP 61755 (LASINAVIR BMS-234475 Lasinavir [INN); CGP 64222; CNI-H0294; Emivirine; Conocurvone (NSC650891); Emtricitabine; C-Oxetanocin-G; Indinavir; The sulfogel polysaccharide; Blue algae antiviral protein-N; SD146; Cyclosporin A; SDZ NIM 811; L-2 ', 3 '-two dehydrogenations-2 ', 3 '-DIDEOXYADENOSINE (L-D4A); 2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy-5-fluorine cytidine (DD4C); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy-5-fluorine cytidine (LD4C); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy guanosine (LD4G); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-didanosine (LD4I); DABO; DdI; DdC; DMP-323; DMP-450; (-)-2 '-deoxidation-3 '-oxa--4 '-the sulfo-cytidine; (-)-2 '-deoxidation-3 '-oxa--4 '-sulfo--5-flurocytosine; Pentafuside (Enfuvirtide); Etoposide; Efavirenz; Emtriva; K-12 (fluorine quinoline); Saquinavir; Foscarnet; Phosphine formic acid; Foscarnet sodium; FPMDAP; FPMPA; FPMPG; Gene Expression Modulator 91 (GEM91); Hammerhead shape is anti--and gagRNA constitutes enzyme, B; Harziphilone; HBY 097 (quinoxaline derivant); E-EBU; E-EPSeU; E-EPU; NSC 648400; E-EBU-dM; Zalcitabine; LY326188; Ingenol 3,5,20-triacetate (ITA); Calophylloide B; KNI-272; RD3-2118; KNI-102; KNI-154; KNI-174; KNI-227; L-685,434; L-689,502; L-697,593; L-697,639; L-697,661; LY289612; Trovirdine; LY-73497; L-735,524; N-ethyl-2 ', 3 '-DIDEOXYADENOSINE; N6-methyl-2 ', 3 '-DIDEOXYADENOSINE; Noa-Asn-Apns-Thz-NH-tBu; Nonoxinol 9; Ritonavir; NSC625487; NSC649324; NSC650898; UC-38; UC-84; P9941; Palinavir; The sulphuric acid pentosan; Elmiron; SP54; PNU-140690 (tipranavir); S-2720; R14458; R82150; R82913; R86183; RD4-2138; Resobene; Reyataz; Ribavirin; 7-chloro-N-methyl-5-(1H-pyrroles-2-yl)-3H-1, the 4-benzodiazepine
-2-amine; 7-chloro-5-(2-pyrrole radicals)-3H-1, the 4-benzodiazepine
-2 (H)-ketone; LY314163; SB-205569; Compound E; SD-095345SD146; SDZ PRI 053; SPC3; Naganol; T22; Thalidomide; Thiangazole; Thiazole and iso-indoles-5-ketone; U-104489; U-140690; U-87201E; U-88204E; UC-781; VB-11,328; VX-478; 141W94; XM-323 and composition thereof.
52. the method for claim 51, wherein said first chemical compound is
53. treat the method that human host HIV infects for one kind, comprise first chemical compound and the acceptable salt of pharmacy thereof to the following formula of described host's combination medicine-feeding effective dose, with the combination of at least a other chemical compound and composition thereof, also combination has pharmaceutically acceptable carrier, additive or excipient:
2-and 4-pyridone and regional isomer thereof that skeleton described in the formula I limits for this paper independently;
R
1And R
2Be H independently of one another; C
1-6Alkyl; C
1-6Fluoro-alkyl; Unsubstituted or substituted C
5-6Cycloalkyl; C
1-6Thiazolinyl; Unsubstituted or substituted phenyl; Unsubstituted or substituted benzyl; C
2-6Alkyl phenyl, described phenyl can be chosen wantonly and be substituted; Unsubstituted or substituted heteroaryl; The C that is replaced by heteroaryl
1-6Alkyl, described heteroaryl is optional to be substituted; C
1-6Alkyl S (O) R or alkyl (SO
2) R, wherein R is alkyl, phenyl or substituted phenyl; C
1-6Alkyl CO
2R
a, R wherein
aBe C
1-6Alkyl or H; C
1-6Alkyl COR
a', R wherein
a' be C
1-6Alkyl;
R
3And R
4Be independently selected from H, C
1-6Alkyl, halogen, hydroxyl, unsubstituted or substituted benzyl, unsubstituted or substituted thiophenyl;
R
5Be CO
2R
cOr P (O) (OR
c) (OR
c), each R wherein
cBe independently selected from H and C
1-6Alkyl,
Described at least a other chemical compound is selected from: ACV; AK602; AMD070; APV; ATV; ATZ; AVX754 (apricitabine); AZT; Abacavir; Abacavir/lamivudine/zidovudine; Abacavir sulfate; Abacavir sulfate/lamivudine; Abacavir/lamivudine; Abelecet; Aciclovir; Adefovir dipivoxil; Amycin; Agenerase; Aldesleukin; Alovudine; Aluvia; AM Bison; Amdoxovir; Amphocin; Amphotec; Amphotericin B; Polyinosini; Amprenavir; Androderm; Androgel; Apricitabine; Aptivus; Atazanavir; Atripla; Azithromycin; BMS-378806; BMS-488043; Bactrim; Baraclude; Bevirimat; Biaxin; Brecanavir; BufferGel; C31G; CD4-IgG2; CS; CV-N; Calanolide A; Calcium hydroxyapatite; Carbopol 974P; Carrageenan; Carraguard; Sulfate cellulose; Clarithromycin; Combivir; Copegus; Sulfamethoxazole; Crixivan; Blue algae antiviral protein-N; Cymevene; DAPD; DLV; DS; Darunavir; Delavirdine; The Depo-testosterone; Dextran sulfate; Didanosine; Fluconazole; Doxil; Doxorubicin (liposome); Dronabinol; EFV; Efavirenz; Elvucitabine; Emtricitabine; The tenofovir disoproxil fumarate; Emtriva; Enfufirtide; Entecavir; Lamivudine; Epoetin Alfa; Epogen; Epzicom; Etopophos (phosphate); Etoposide; Etravirine; FTC; Fluconazol; Fortovase; Fosamprenavir; Foxivudine tidoxil; Fungizone; Fuzeon; GS 9137; GSK-873,140 (aplaviroc); GW433908; GW640385 (brecanavir); Ganciclovir; Immunoglobulin; Growth hormone (people); Hepsera; Hivid; The human growth hormone; IL-2; INH; Immunoglobulin, intravenous (people); Indinavir; Interferon; Interleukin-2, recombinant, people; Recombinant Interferon (2b); Invirase; Isoniazid; Itraconazole; KP-1461; Lamivudine/zidovudine; Lexiva; Lopinavir/ritonavir; MK-0518; Nebupent; Nelfinavir; Neutrexin; Nevirapine; Nuo Wei; Nydrazid; Peptide T; PMPA prodrug (Viread) ' Prezista (Darunavir); PRO 140; PRO 2000; PRO 542 (CD4 IGg2); Procrit (Epoetin); Aldesleukin; Racivir; Radiesse; Rrebetol; Delavirdine; Zidovudine; Reyataz; Ribavirin; Rifabutin; Rifadin; Rifampicin; Rimactane; Ritonavir; Rodferon-A (2a); Saquinavir; SCH-D (vicriviroc); Growth hormone; Stavudinie; Sulfamethoxazole/trimethoprim; Testosterone; Sustiva; TNX-355; Taxol; Tenofovir; The tenofovir disoproxil fumarate; Testosterone; Tipranavir; Toposar; Trimetrexate; Three associations only; Truvada (Emtriva and Viread combination); U-90152S (Delaviridine); UC-781; UK-427,857 (maraviroc); Valcyte; Valganciclovir; Valproic acid; Fan Bishi; Vicriviroc; Videx; Viracept see nelfinaivr (Tennofovir DF); The happy life of dimension; Virazole; Viread; Vitrasert; Zalcitabine; Sai Ruite; Match is advanced; Zidovudine; Zithromax; Zovirax and composition thereof.
54. the method for claim 53, wherein said first chemical compound is
55. pharmaceutical composition comprises the chemical compound of the following structure of effective dose:
With the combination of at least a other chemical compound of effective dose and composition thereof, also combination has pharmaceutically acceptable carrier, additive or excipient, and described other chemical compound is selected from
(-) beta-dioxolane-G (DXG); (-) β-arctigenin (arctigenin); (-)-Carbovir (-)-C-D4G; (-)-2 ', 3 '-dideoxy-5-fluoro-3 '-thia cytidine (FTC); (-)-β-D-2,6-diaminopurine dioxolanes (DAPD); (+)-2 '-deoxidation-3 '-oxa--4 '-sulfo-cytidine (dOTC+); (+)-2 '-deoxidation-3 '-oxa--4 '-sulfo--5-fluorine cytidine (dOTFC+); (+/-)-Lobucavir;
(R)-and 2QuinCOAsnPhe[CHOHCH2] PipCONHtBu; (R)-3,6-diamino-N-(amino methyl) caproamide (Bellenamine); (R)-9-(2-phosphonium mesitoyl methoxy propyl group) adenine (tenofovir); (R)-PMPDAP; (S)-9-(2-phosphonium mesitoyl methoxy propyl group) adenine ((S)-PMPA); PMPA (S); α-APA (loviride); R87232; R88703; α-APA enantiomer (R90385);
α-L-AZT; α-L-dioxolanes-C (α-L-DXC); α-L-FTC;
α-single methyl fluoride dehydrogenation ornithine methyl ester (MFMOME); 1,1 '-Celogen Az (ADA); 1-(11-octyl group amino-10-hydroxyl undecyl)-3,7-dimethyl xanthine (CT-2576);
1-(2 ', 3 '-dideoxy-2 '-fluoro-beta-D-threo form-penta furyl glycosyl) cytosine (Ro 31-6840);
1-(2 '-fluoro-2 ', 3 '-dideoxy-β-D-erythro-penta furyl glycosyl) thymus pyrimidine (2 ' FddT);
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(3-aminomethyl phenyl) sulfenyl) thymus pyrimidine (HEPT-M);
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(thiophenyl)-2-thio-thymine (HEPT-S);
The 1-[(2-hydroxyl-oxethyl) methyl]-6-(thiophenyl) thymus pyrimidine (HEPT);
Deoxidation nojirimycin (1-deoxidation nojirimycin); Amprenavir; Abacavir succinate (match is advanced); 1-amino oxygen base ethamine (AEA); 1-methoxyl group oxalyl group-3, and the 5-dicaffeoylquinic acid (1-MO-3,5-DCQA); 1OH-2 (Cbz-Tle) 3PhPr[14] the adjacent formic acid derivates of two Parylenes; 1OH-2 (Cbz-ValNH) 3PhPr[13] the adjacent formic acid derivates of dimerization meta-xylene; 1OH-2 (Cbz-ValNH) 3PhPr[13] the adjacent formic acid derivates of two Parylenes;
1OH-2 (Cbz-ValNH) 3PhPr[14] the adjacent formic acid derivates of two Parylenes; 1OH-2 (Cbz-ValNH) 3PhPr[17] the adjacent formic acid derivates of two Parylenes; 12-deoxidation phorbol-13-(3E, 5E-decadinene acid esters); 16. α-bromine epiandrosterone (Epi-Br) or (Inactivin); 1-β-D-arabinofuranosyl adenin glycosyl-5-(2-bromo vinyl) uracil (Sorivudine); 2 ', 3 '-two dehydrogenations-3 '-deoxycytidine (D4C);
2 ', 3 '-dideoxy two dehydrogenation guanosines (D4G); 2 ', 3 '-two dehydrogenations-3 '-deoxyribosylthymine (D4T) (stavudine); 2 ', 3 '-dideoxy-3 '-fluoro-4-sulfo-thymidine (3 '-F-4-Thio-ddT);
2 ', 3 '-dideoxy-3 '-fluoro-5-broxuridine (FddBrU); 2 ', 3 '-dideoxy-3 '-fluoro-5-5-chloro-5-deoxyarabinosylcytosine (3 '-F-5-Cl-ddC); 2 ', 3 '-dideoxy-3 '-fluoro-5-chloriduria glycosides (935U83) (raluridine); 2 ', 3 '-dideoxy-5-ethyl cytidine (5-Et-ddC); 2 ', 3 '-DIDEOXYADENOSINE (ddA);
2 ', 3 '-dideoxy two dehydrogenation adenosines (d4A); 2 ', 3 '-dideoxy guanosine (ddG);
2 ', 3 '-dideoxy-3 '-hydroxymethyl cytidine (3 '-hydroxymethyl-ddC); 2,5 '-dehydration-3 '-azido-2 ', 3 '-di-deoxyuridine (AZU-2,5 '-dehydration); 2,5 '-dehydration-3 '-azido-3 '-deoxyribosylthymine (AZT-2,5 '-dehydration); 2 ', 5 ' diSilySpiroT (TSAO-T); 2 ', 5 ' diSilySpiroT (TSAO-me^3T); 2,6-diaminourea-2 ', 3 '-dideoxy purine-9-ribofuranoside (ddDAPR) (2, the 6-diaminourea-ddP); 2,6-diaminopurine-2 ', 3 '-dideoxy two dehydrogenation nucleoside (ddeDAPR); 2,6-diaminopurine-3 '-fluoro-2 ', 3 '-di-deoxynucleoside (3 '-F-ddDAPR); 2-aminobenzyl statine valyl Cbz derivant; 2-glycine amide-5-chlorphenyl 2-pyrrolyl ketone (GCPK); [2-PyridCH2NCH3CO-Val-NHCH (Bz)] CHOHCHOH (A-77003); 2 '-azido-2 ', 3 '-DIDEOXYADENOSINE (2 '-N3ddA); 2 '-F-dd-ara-A (Lodensine); 2 '-FddT; 2 '-N3ddA; 2 '-N3ddA (β-D-threo form); 2-NaphCOAsnPhe[CHOHCH2] Pro-OtBu; 2-nitrobenzophenone phenylsulfone (NPPS); 3-(3-oxo-1-acrylic)-3 '-azido-3 '-deoxyribosylthymine (3-(3-oxo-1-acrylic) AZT); 3-(3-oxo-1-acrylic) AZT; L-737,126; 3, and the 5-dicaffeoylquinic acid (3,5-DCQA); 3 '-azido-3 '-deoxidation-6-azathymidine; 3 '-azido-2 ', 3 '-dideoxy-5-[(cyano methyl) the oxygen base] uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-aminouridine; 3 '-azido-2 ', 3 '-the assorted uridnine of dideoxy-5-azepine-6-denitrification; 3 '-azido-2 ', 3 '-dideoxy-5-broxuridine; 3 '-azido-2 ', 3 '-dideoxy-5-5-chloro-5-deoxyarabinosylcytosine (3 '-Az-5-Cl-ddC); 3 '-azido-2 ', 3 '-dideoxy-5-dimethylamino uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-ethyl uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-fluorine cytidine; 3 '-azido-2 ', 3 '-dideoxy-5-floxuridine; 3 '-azido-2 ', 3 '-dideoxy-5-hydroxyuridine; 3 '-azido-2 ', 3 '-dideoxy-5-iodo uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-methylamino uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-methylcytidine; 3 '-azido-2 ', 3 '-dideoxy-5-thiocyano uridnine; 3 '-azido-2 ', 3 '-dideoxy-5-trifluoromethyl uridnine; 3 '-azido-2 ', 3 '-zalcitabine; 3 '-azido-2 ', 3 '-the dideoxy guanosine; 3 '-azido-2 ', 3 '-dideoxy-N4--5-dimethyl cytidine; 3 '-azido-2 ', 3 '-dideoxy-N4-OH-5-methylcytidine; 3 '-azido-2 ', 3 '-di-deoxyuridine (Uravidine); 3 '-azido-3 '-deoxidation-6-azathymidine; 3-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-adenylic acid; 3 '-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-adenylic acid, 2-cyano ethyl ester; 3 '-azido-3 '-the deoxyribosylthymine base-(5 ', 5 ')-2 ', 3 '-dideoxy-5 '-inosinic acid (AZT-P-ddI); 3 '-azido-3 '-deoxyribosylthymine-5 '-(butyl methoxyl group valine) phosphate ester; 3 '-azido-5-chloro-2 ', 3 '-di-deoxyuridine; 3 '-deoxyribosylthymine (ddT); 9-(3 '-fluoro-2 ', 3 '-dideoxy-β-D-erythro penta furyl glycosyl) adenine;
3 '-fluoro-2 ', 3 '-dideoxy-5-iodo uridnine (FddIU); 3 '-fluoro-2 ', 3 '-zalcitabine (3 '-FddC); 3 '-fluoro-2 ', 3 '-the dideoxy guanosine (3 '-FddG); 3 '-fluoro-2 ', 3 '-di-deoxyuridine (3 '-FddU); 9-(3 '-azido-2 ', 3 '-dideoxy-β-D-erythro penta furyl glycosyl) adenine; 3TC (lamivudine); 3TC ﹠amp; AZT (Combivir); 4 '-acetylamino phenyl 4-guanidine benzoate; 4 '-azido-3 '-deoxyribosylthymine; 4 '-azido-5-chloro-2 '-BrdU; 4 '-azido-2 '-deoxyadenosine; 4 '-azido-2 '-deoxycytidine; 4 '-azido-2 '-deoxyguanosine; 4 '-azido-2 '-deoxyinosine; 4 '-azido-2 '-BrdU; 4 '-azido breast glycosides; 4 '-cyano group breast glycosides; 4-methyl-5-(pyrazinyl)-3H-1,2-dithia cyclopentenes-3-thioketone (oltipraz); 5 '-[(1,4-dihydro-1-methyl-3-pyridine radicals carbonyl) oxygen base]-3 '-azido-2 ', 3 '-deoxyribosylthymine (DP-AZT); 5 '-[[(Z)-and 4-amino-crotyl] methylamino]-5 '-deoxyadenosine (MDL 73811); 5 '-alkyl polyglucoside carbonic ester of 3 '-azido-3 '-deoxyribosylthymine; 5Cl3PhS-2 indole CONH2; 5-fluoro-2 ', 3 '-zalcitabine; 5-methyl-3 '-azido-2 ', 3 '-the different cytidine of dideoxy; Celgosivir; 6-chloro-9-(2,3-dideoxy-β-D-glycerol penta furyl glycosyl)-9H-purine; 6-dimethylaminopurine-2 ', 3 '-di-deoxynucleoside; Ro 24-7429; Ro 5-3335; Tivirapine; 9-(2,3-dideoxy-β-D-ribofuranosyl)-6-(methyl mercapto) purine; 9-(2 '-azido-2 ', 3 '-dideoxy-B-D-threo form penta furyl glycosyl) adenine; C-Europe tower mycin A; (+-) Lobucavir; A-76890; A-77003; A-77212; A-80987; A-81525; A-83962; A-98881; PNU-104489; Three associations only; Lopinavir; Kaletra; Lopinavir and ritonavir;
With the promise Wei; Azodicarboamide; Adefovirdipivoxil; Adefovir dipivoxil
Nelfinavir; AG1350 (LY316957); R-87366; Alpha-lipoic acid; Alovudine (3 '-FddT); ALX40-4C; AMD3100 (JM3100); Amdoxovir (APD); Phosphoric acid amprenavir (fosamprenavir); Ancer 20 (Z-100); Atazanavir (Latazanavir); Ah 's dimension is fixed; The aurintricarboxylic acid; AY 9944; 3 '-azido-5-chloro-2 ', 3 '-di-deoxyuridine; AZT; α-L-AZT; O, O '-two (3 '-azido-3 '-methyl phosphonate of deoxyribosylthymine-5 '-yl); Baicalin (TJN-151); Belulinic acid Betulinic acid (Mairin); Belulinic acid Betulinic acid, 3-O-(3 ', 3 '-the dimethyl succinate ester); Delavirdine (U-90152); U-88204E; Nevirapine; BILA 1906 BS; BILA2011BS (palinavir); BILA 2185 BS; NSC633001; CGP 53820; Two-ValHOEt-N2aza-peptide isostere (CGP 53820 analog); BMS-186318; L-687,908; Brovavir; BzOCValPhe[diCHOH (RR)] PheValBzOC; BzOCValPhe[diCHOH (SS)] PheValBzOC; C2-Sym phosphonic amide derivant (HOECHSTAG); NSC675451; Calanolide B; Capravirine (S-1153); Carbovir; Castanospermine; CGP 61755 (LASINAVIR BMS-234475 Lasinavir [INN); CGP 64222; CNI-H0294; Emivirine; Conocurvone (NSC650891); Emtricitabine; C-Oxetanocin-G; Indinavir; The sulfogel polysaccharide; Blue algae antiviral protein-N; SD146; Cyclosporin A; SDZ NIM 811; L-2 ', 3 '-two dehydrogenations-2 ', 3 '-DIDEOXYADENOSINE (L-D4A); 2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy-5-fluorine cytidine (DD4C); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy-5-fluorine cytidine (LD4C); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-dideoxy guanosine (LD4G); L-2 ', 3 '-two dehydrogenations-2 ', 3 '-didanosine (LD4I); DABO; DdI; DdC; DMP-323; DMP-450; (-)-2 '-deoxidation-3 '-oxa--4 '-the sulfo-cytidine; (-)-2 '-deoxidation-3 '-oxa--4 '-sulfo--5-flurocytosine; Pentafuside (Enfuvirtide); Etoposide; Efavirenz; Emtriva; K-12 (fluorine quinoline); Saquinavir; Foscarnet; Phosphine formic acid; Foscarnet sodium; FPMDAP; FPMPA; FPMPG; Gene Expression Modulator 91 (GEM91); Hammerhead shape resists-gagRNA formation enzyme B; Harziphilone; HBY 097 (quinoxaline derivant); E-EBU; E-EPSeU; E-EPU; NSC 648400; E-EBU-dM; Zalcitabine; LY326188; Ingenol 3,5,20-triacetate (ITA); Calophylloide B; KNI-272; RD3-2118; KNI-102; KNI-154; KNI-174; KNI-227; L-685,434; L-689,502; L-697,593; L-697,639; L-697,661; LY289612; Trovirdine; LY-73497; L-735,524; N-ethyl-2 ', 3 '-DIDEOXYADENOSINE; N6-methyl-2 ', 3 '-DIDEOXYADENOSINE; Noa-Asn-Apns-Thz-NH-tBu; Nonoxinol 9; Ritonavir; NSC625487; NSC649324; NSC650898; UC-38; UC-84; P9941; Palinavir; The sulphuric acid pentosan; Elmiron; SP54; PNU-140690 (tipranavir); S-2720; R14458; R82150; R82913; R86183; RD4-2138; Resobene; Reyataz; Ribavirin; 7-chloro-N-methyl-5-(1H-pyrroles-2-yl)-3H-1, the 4-benzodiazepine
-2-amine; 7-chloro-5-(2-pyrrole radicals)-3H-1, the 4-benzodiazepine
-2 (H)-ketone; LY314163; SB-205569; Compound E; SD-095345SD146; SDZ PRI 053; SPC3; Naganol; T22; Thalidomide; Thiangazole; Thiazole and iso-indoles-5-ketone; U-104489; U-140690; U-87201E; U-88204E; UC-781; VB-11,328; VX-478; 141W94; XM-323 and composition thereof.
56. pharmaceutical composition comprises the chemical compound of the following structure of effective dose:
Also made up pharmaceutically acceptable carrier, additive or excipient with the combination of at least a other chemical compound of effective dose and composition thereof,
Described other chemical compound is selected from ACV; AK602; AMD070; APV; ATV; ATZ; AVX754 (apricitabine); AZT; Abacavir; Abacavir/lamivudine/zidovudine; Abacavir sulfate; Abacavir sulfate/lamivudine; Abacavir/lamivudine; Abelecet; Aciclovir; Adefovir dipivoxil; Amycin; Agenerase; Aldesleukin; Alovudine; Aluvia; AM Bison; Amdoxovir; Amphocin; Amphotec; Amphotericin B; Polyinosini; Amprenavir; Androderm; Androgel; Apricitabine; Aptivus; Atazanavir; Atripla; Azithromycin; BMS-378806; BMS-488043; Bactrim; Baraclude; Bevirimat; Biaxin; Brecanavir; BufferGel; C31G; CD4-IgG2; CS; CV-N; Calanolide A; Calcium hydroxyapatite; Carbopol 974P; Carrageenan; Carraguard; Sulfate cellulose; Clarithromycin; Combivir; Copegus; Sulfamethoxazole; Crixivan; Blue algae antiviral protein-N; Cymevene; DAPD; DLV; DS; Darunavir; Delavirdine; The Depo-testosterone; Dextran sulfate; Didanosine; Fluconazole; Doxil; Doxorubicin (liposome); Dronabinol; EFV; Efavirenz; Elvucitabine; Emtricitabine; The tenofovir disoproxil fumarate; Emtriva; Enfufirtide; Entecavir; Lamivudine; Epoetin Alfa; Epogen; Epzicom; Etopophos (phosphate); Etoposide; Etravirine; FTC; Fluconazol; Fortovase; Fosamprenavir; Foxivudine tidoxil; Fungizone; Fuzeon; GS 9137; GSK-873,140 (aplaviroc); GW433908; GW640385 (brecanavir); Ganciclovir; Immunoglobulin; Growth hormone (people); Hepsera; Hivid; The human growth hormone; IL-2; INH; Immunoglobulin, intravenous (people); Indinavir; Interferon; Interleukin-2, recombinant, people; Recombinant Interferon (2b); Invirase; Isoniazid; Itraconazole; KP-1461; Lamivudine/zidovudine; Lexiva; Lopinavir/ritonavir; MK-0518; Nebupent; Nelfinavir; Neutrexin; Nevirapine; Nuo Wei; Nydrazid; Peptide T; PMPA prodrug (Viread) ' Prezista (Darunavir); PRO 140; PRO 2000; PRO 542 (CD4 IGg2); Procrit (Epoetin); Aldesleukin; Racivir; Radiesse; Rrebetol; Delavirdine; Zidovudine; Reyataz; Ribavirin; Rifabutin; Rifadin; Rifampicin; Rimactane; Ritonavir; Rodferon-A (2a); Saquinavir; SCH-D (vicriviroc); Growth hormone; Stavudinie; Sulfamethoxazole/trimethoprim; Testosterone; Sustiva; TNX-355; Taxol; Tenofovir; The tenofovir disoproxil fumarate; Testosterone; Tipranavir; Toposar; Trimetrexate; Three associations only; Truvada (Emtriva and Viread combination); U-90152S (Delaviridine); UC-781; UK-427,857 (maraviroc); Valcyte; Valganciclovir; Valproic acid; Fan Bishi; Vicriviroc; Videx; Viracept see nelfinaivr (Tennofovir DF); The happy life of dimension; Virazole; Viread; Vitrasert; Zalcitabine; Sai Ruite; Match is advanced; Zidovudine; Zithromax; Zovirax and composition thereof.
Applications Claiming Priority (4)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| US83199006P | 2006-07-19 | 2006-07-19 | |
| US60/831,990 | 2006-07-19 | ||
| US60/920,197 | 2007-03-27 | ||
| US60/920,196 | 2007-03-27 |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| CN101516369A true CN101516369A (en) | 2009-08-26 |
Family
ID=41040412
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CNA2007800346972A Pending CN101516369A (en) | 2006-07-19 | 2007-07-13 | Pyridinone diketo acids: inhibitors of HIV replication in combination therapy |
Country Status (1)
| Country | Link |
|---|---|
| CN (1) | CN101516369A (en) |
Cited By (6)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN102753526A (en) * | 2009-12-07 | 2012-10-24 | 佐治亚大学研究基金会 | Pyridinone hydroxycyclopentyl carboxamides: HIV integrase inhibitors with therapeutic applications |
| WO2016045115A1 (en) * | 2014-09-28 | 2016-03-31 | 姜凡 | Hiv-1 integrase inhibitor |
| CN111265499A (en) * | 2020-02-17 | 2020-06-12 | 江苏艾立康药业股份有限公司 | Lopinavir inhalation aerosol and preparation method thereof |
| CN112691094A (en) * | 2019-10-22 | 2021-04-23 | 中国科学院分子细胞科学卓越创新中心 | Novel compound for preventing and treating virus and application thereof |
| CN113577081A (en) * | 2014-07-11 | 2021-11-02 | 吉利德科学公司 | TOLL-like receptor modulators for the treatment of HIV |
| WO2022143985A1 (en) * | 2020-12-31 | 2022-07-07 | 清华大学 | Pyridine-2-amine derivative and pharmaceutical composition and use thereof |
-
2007
- 2007-07-13 CN CNA2007800346972A patent/CN101516369A/en active Pending
Cited By (8)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN102753526A (en) * | 2009-12-07 | 2012-10-24 | 佐治亚大学研究基金会 | Pyridinone hydroxycyclopentyl carboxamides: HIV integrase inhibitors with therapeutic applications |
| CN102753526B (en) * | 2009-12-07 | 2014-11-26 | 佐治亚大学研究基金会 | Pyridinone hydroxycyclopentyl carboxamides: HIV integrase inhibitors with therapeutic applications |
| CN113577081A (en) * | 2014-07-11 | 2021-11-02 | 吉利德科学公司 | TOLL-like receptor modulators for the treatment of HIV |
| WO2016045115A1 (en) * | 2014-09-28 | 2016-03-31 | 姜凡 | Hiv-1 integrase inhibitor |
| CN112691094A (en) * | 2019-10-22 | 2021-04-23 | 中国科学院分子细胞科学卓越创新中心 | Novel compound for preventing and treating virus and application thereof |
| CN112691094B (en) * | 2019-10-22 | 2022-09-23 | 中国科学院分子细胞科学卓越创新中心 | Novel compound for preventing and treating virus and application thereof |
| CN111265499A (en) * | 2020-02-17 | 2020-06-12 | 江苏艾立康药业股份有限公司 | Lopinavir inhalation aerosol and preparation method thereof |
| WO2022143985A1 (en) * | 2020-12-31 | 2022-07-07 | 清华大学 | Pyridine-2-amine derivative and pharmaceutical composition and use thereof |
Similar Documents
| Publication | Publication Date | Title |
|---|---|---|
| US20100092427A1 (en) | Pyridinone Diketo Acids: Inhibitors of HIV Replication in Combination Therapy | |
| EP2509949B1 (en) | Pyridinone hydroxycyclopentyl carboxamides: hiv integrase inhibitors with therapeutic applications | |
| CN101679266B (en) | PIM kinase inhibitors and methods of their use | |
| EP2296653B1 (en) | Compounds and methods for treating inflammatory and fibrotic disorders | |
| CN101516369A (en) | Pyridinone diketo acids: inhibitors of HIV replication in combination therapy | |
| US20140249135A1 (en) | Pim kinase inhibitors and methods of their use | |
| JP2013512957A5 (en) | ||
| WO2007106450A2 (en) | Diketo acids with nucleobase scaffolds: anti-hiv replication inhibitors targeted at hiv integrase in combination therapy | |
| AU3648801A (en) | Alpha v integrin receptor antagonists | |
| CN101151254A (en) | Diketo acids with nucleobase scaffolds: anti-HIV replication inhibitors targeted at HIV integrase | |
| CN108530444A (en) | A kind of novel NAMPT and IDO double inhibitors and preparation method thereof and medical usage | |
| EP2831056B1 (en) | New anti-mycobacterial drugs against tuberculosis | |
| US8664248B2 (en) | Derivatives of pyridoxine for inhibiting HIV integrase | |
| KR20150093796A (en) | Pyridone derivatives and uses thereof in the treatment of tuberculosis | |
| AU2012202993B2 (en) | Pim kinase inhibitors and methods of their use |
Legal Events
| Date | Code | Title | Description |
|---|---|---|---|
| C06 | Publication | ||
| PB01 | Publication | ||
| C10 | Entry into substantive examination | ||
| SE01 | Entry into force of request for substantive examination | ||
| REG | Reference to a national code |
Ref country code: HK Ref legal event code: DE Ref document number: 1130201 Country of ref document: HK |
|
| C02 | Deemed withdrawal of patent application after publication (patent law 2001) | ||
| WD01 | Invention patent application deemed withdrawn after publication |
Open date: 20090826 |
|
| REG | Reference to a national code |
Ref country code: HK Ref legal event code: WD Ref document number: 1130201 Country of ref document: HK |