CN100575352C - Synthetic and the application of 1-(4-chloroanilino)-4-(4-picolyl)-2 - Google Patents
Synthetic and the application of 1-(4-chloroanilino)-4-(4-picolyl)-2 Download PDFInfo
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- CN100575352C CN100575352C CN200610045239A CN200610045239A CN100575352C CN 100575352 C CN100575352 C CN 100575352C CN 200610045239 A CN200610045239 A CN 200610045239A CN 200610045239 A CN200610045239 A CN 200610045239A CN 100575352 C CN100575352 C CN 100575352C
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Abstract
The synthetic method and the application of 1-(4-chloroanilino)-4-(4-picolyl)-2 belong to angiogenesis inhibitor antitumor drug synthesis technical field.Structural formula of compound is as follows: the preparation method of (seeing right formula) this compound is to be raw material with the phthalide, obtain intermediate 3-hydroxyl-2-(4-pyridyl) 1-indenes with the reaction of formaldehyde pyridine, in hydrazine hydrate, obtain another intermediate 4-(4-pyridyl) methyl-2H-1-2 again through ring expansion, the 3-naphthyridine, last and p-Chlorobenzoic acid amide reacts under molten state and obtains product 1-(4-chloroanilino)-4-(4-picolyl)-2 (I).Compound of the present invention is a kind of selectivity angiogenesis inhibitor, can pass through to suppress vascular endothelial growth factor, and oral absorption is effective, and low dose of use can suppress tumor vascular formation and propagation, reaches the effect of control tumor growth.
Description
(1) technical field
The present invention relates to the synthetic of 1-(4-chloroanilino)-4-(4-picolyl)-2 (I) and use, belong to angiogenesis inhibitor antitumor drug synthesis technical field.
(2) background technology
In antineoplaston, chemotherapy is to use more a kind of whole body therapeutic, both can use separately, again can with the additive method combined utilization.Even in the treatment that can't undergo surgery, terminal cancer still can treat.Nearly ten or twenty year, the fast development of science of cellular elements biology and chemotherapeutic, chemotherapeutics just by the new type anticancer medicine transition of traditional cytotoxic drug to too many levels, novel targets, cancer cells differentiating inducer, telomerase inhibitor even therapy of tumor have occurred.The transfer of tumour is the process of a complexity, but the formation of most of metastasis and development all need rely on the formation of blood vessel, referring to Volkmann. anti-angiogenesis: solid tumor treatment new ideas. surgery annals .1972,175,409-416. (Folkman, J.Anti-Angiogenesis:New Concept for Therapy of Solid Tumors.Ann.Surg.1972,175,409-416).Therefore suppressing tumor vessel forms, cut off tumor growth and shift " lifeblood " that is relied on, become important anticancer strategy, referring to Volkmann. by attacking its blood supply system beat cancer. U.S. science .1996,2-5. (Folkman, J.Fighting Cancer by Attacking Its Blood Supply.Sci.Am.1996,2-5.).Vascular endothelial growth factor (VEGF), the regulating and controlling effect that the propagation of vascular endothelial cell, hydrolysis basement membrane, migration and blood vessel are made up is stronger, and specificity height, referring to Bu Liye etc. the effect of vasculai endothelium growth factor in vascularization. biomass cells trend .1996,6,454-456. (Breier, G.; Risau, W.The role of vascularendothelial growth factor in blood vessel formation.Trends Cell Biol.1996,6,454-456).The VEGF of tumor cell secretion focuses mostly on around tumor vessel, and immunohistochemical methods detects and only finds VEGF in endotheliocyte, does not detect VEGF away from the endotheliocyte of tumour.Vegf receptor is expressed high cell, its VEGF recall rate is higher than the low cell of expression of receptor, the prompting VEGF focus mostly on target cell bonded position, being tumor vessel is higher than normal blood vessels to the reaction of VEGF, referring to Lin Desi etc. are with VEGF is the angiogenesis inhibitor and the antineoplaston of target: where we in now? international pathology prospect .1998,79,339-346. (Leenders, W.P.J.Targetting VEGFin antiangiogenic and anti-tumour therapy:Where are we now? Int.J.Exp.Pathol.1998,79,339-346), this studies show that, the angiogenesis inhibitor of anti-VEGF can optionally act on tumor tissues and to the not influence of neonatal blood vessels endotheliocyte of healthy tissues.Therefore, the VEGF inhibitor is expected to become the antitumor drug of safety, easy tolerance.
Discover that 1-anilino-(4-pyridylmethyl)-phthalazines micromolecular compound has very high selective inhibitory to human VEGF Tyrosylprotein kinase KDR acceptor.According to cellular KDR kinase inhibition theory, this type of micromolecular compound is with its special configuration, can by with the receptors bind of a-protein TP end, produce a series of biological effects, the automatic phosphorylation that has suppressed KDR, referring to Bao De etc. adjacent phthalide piperazine suppresses angiogenesis factor. the patent No.: WO-98/35958A1, date of application: 1997,02,13. date of publication: 1998,08,20. (Bold, G.; Frel, J.; Traxier, P.; Altmann, K.H.; Mett, H.; Stover, D.R.; Wood, J.Phthalazines with angiogenesis inhibitingactivity.WO-98/35958A1, priority date, Febrary 13,1997; Publication date, August 20,1998), and than VEGF inhibitor such as the 3-substituted-dihydro indole-2-ketone compound found before, this type of micromolecular compound has better pharmacokinetics feature after the animal and human is oral, wait the synthetic and biological assessment of .3-substituted-dihydro indol-2-one referring to grandson: what a class was new shows the tyrosine kinase inhibitor of selective inhibitory to the Tyrosylprotein kinase specific receptor. U.S. pharmaceutical journal .1998,41, (2588-2603).(Sun,L.;Tran,N.;Tang,F.;Hirth,P.;McMahon,G.;Tang,C.Synthesis?and?Biological?Evaluations?of3-substituted?indolin-2-ones:A?Novel?Class?of?Tyrosine?Kinase?Inhibitors?ThatExhibit?Selectivity?toward?Particular?Receptor?Tyrosine?Kinases.J.Med.Chem.1998,41,2588-2603)。
(3) summary of the invention
In order to remedy the deficiencies in the prior art, the invention provides compound shown in the molecular formula (I):
Compound shown in the molecular formula (I) is that similar is in the micromolecular compound 1-of 1-anilino-(4-pyridylmethyl)-phthalazines class (4-chloroanilino)-4-(4-picolyl)-2,3-naphthyridine (I) is a kind of new VEGF Tyrosylprotein kinase KDR acceptor inhibitor.
The synthetic method of 1-of the present invention (4-chloroanilino)-4-(4-picolyl)-2 (I), divided for three steps carried out:
(1) be raw material with the phthalide, under strong alkali environment, obtain intermediate 3-hydroxyl-2-(4-pyridyl) 1-indenes (III) with the reaction of formaldehyde pyridine,
(2) this intermediate obtains another intermediate 4-(4-pyridyl) methyl-2H-1-2 through ring expansion again in hydrazine hydrate, 3-naphthyridine (IV),
(3) with 4-(4-pyridyl) methyl-2H-1-2,3-naphthyridine and p-Chlorobenzoic acid amide react under molten state and obtain product 1-(4-chloroanilino)-4-(4-picolyl)-2 (I).
Preferably, the strong alkali environment of the described reaction of step (1) is to select the strong alkali catalyst sodium methylate for use.
Preferably, the reagent of the described ring expansion adding of step (2) is hydrazine hydrate.
Preferably, the described reaction of step (3) is frit reaction, and used dewatering agent is a Vanadium Pentoxide in FLAKES, and used phase-transfer catalyst is a triethylamine hydrochloride, and used solubility promoter is a tetramethyl-urea.
Below preferred synthetic concrete steps are described in detail respectively.
1. intermediate 3-hydroxyl-2-(4-pyridyl) 1-indenes (III) is synthetic
With phthalide (II) is raw material, under 65 ℃, and 1: 1 in molar ratio, with the reaction of 4-formaldehyde pyridine, strong alkali catalyst is selected sodium methylate for use, and the mol ratio of sodium methylate and reactant is 1-3: 1, generate 3-hydroxyl-2-(4-pyridyl) 1-indenes (III), reaction times 1-3h, reaction formula is as follows:
2. intermediate 4-(4-pyridyl) methyl-2H-1-2,3-naphthyridine (IV) synthetic
3-hydroxyl-2-(4-pyridyl) 1-indenes (III) is added in single hydrazine hydrate, volume ratio 0.1-0.3g/ml, 110 ℃ of temperature, reaction generates 4-(4-pyridyl) methyl-2H-1-2,3-naphthyridine (IV), reaction times 5-15h, reaction formula is as follows:
3. product 1-(4-chloroanilino)-4-(4-picolyl)-2 (I) is synthetic
With 4-chloroaniline, 4-(4-pyridyl) methyl-2H-1-2,3-naphthyridine (IV) is 1-4 in molar ratio: 1, and temperature 150-190 ℃, frit reaction obtains product 1-(4-chloroanilino)-4-(4-picolyl)-2 (I).Reaction times 1-3h.Reaction formula is as follows:
Preferably, in the above-mentioned steps 3, the carrying out of frit reaction also need add the Vanadium Pentoxide in FLAKES dehydration, triethylamine hydrochloride is made phase-transfer catalyst, when reaction finishes tetramethyl-urea added in the reactive system, adds the mixture cooling reactant of entry and ammoniacal liquor then.
Compound 1-of the present invention (4-chloroanilino)-4-(4-picolyl)-2,3-naphthyridine (I) is a kind of selectivity angiogenesis inhibitor, can suppress neonate tumour blood vessel and growth by suppressing vascular endothelial growth factor (VEGF) Tyrosylprotein kinase KDR acceptor.And oral absorption is effective, and low dose of use can suppress tumor vascular formation and propagation, reaches the effect of control tumor growth.
Compound 1-of the present invention (4-chloroanilino)-4-(4-picolyl)-2 (I) is used to prepare the medicine of anti-human malignant tumor.
Compound 1-of the present invention (4-chloroanilino)-4-(4-picolyl)-2,3-naphthyridine (I) plays and suppresses tumor growth and prevent the effect of tumour cell through the blood diffusion as selectivity tumor vascular endothelium somatomedin Tyrosylprotein kinase KDR acceptor inhibitor.
The present invention has also carried out experimentation on animals to the anti-malignant tumor effect of described compound 1-(4-chloroanilino)-4-(4-picolyl)-2 (I).Experimental result shows that the succinate that gives the oral 1-of mouse (4-chloroanilino)-4-(4-picolyl)-2 (I) can obviously suppress its tumor growth, and does not influence the survival condition of mouse.
(4) embodiment
Embodiment 1:
The molecular formula of 1-(4-chloroanilino)-4-(4-picolyl)-2 (I):
The preparation method is as follows:
(1) 3-hydroxyl-2-(4-pyridyl) 1-indenes (III) is synthetic
In the 250ml there-necked flask of whipping appts and reflux exchanger is housed, add 20.2g (0.15mol) phthalide (II), 14.1ml (0.15mol) 4-formaldehyde pyridine is a solvent with 75ml ethyl propionate and 150ml methyl alcohol, is cooled to this mixture ice-water bath ice-cold.Add 24.3g (0.45mol) sodium methylate, this reaction mixture is heated to 65 ℃, reaction 2h.The concentrating under reduced pressure reaction mixture.Dilute this mixture with 700ml water, obtain the solution of dark red.With this solution of ether extraction.With acetate acidifying water layer, stir and produce the yellow suspension thing, filter.Filter cake is water, ether washing respectively, obtains 17g product 3-hydroxyl-2-(4-pyridyl) 1-indenes (III), and yield is 50.8%.
Product structure confirms with mass spectrometric detection, m/z:223 (M)
(2) 4-(4-pyridyl) methyl-2H-1-2,3-naphthyridine (IV) synthetic
In the 500ml there-necked flask of whipping appts and reflux exchanger is housed, add single hydrazine hydrate 250ml, 3-hydroxyl-2-(4-pyridyl) 1-indenes (III) 58g (0.26mol) is heated to 110 ℃ and obtains dark red solution.Reaction 15h obtains new precipitation.Filter this reaction mixture.Solid matter adopts ethanol, ether to wash respectively, obtains 49g product 4-(4-pyridyl) methyl-2H-1-2, and 3-naphthyridine (1-), yield are 79.5%.
Product structure confirms with mass spectrometric detection, m/z:237 (M)
(3) 1-(4-chloroanilino)-4-(4-picolyl)-2 (I) is synthetic
Vanadium Pentoxide in FLAKES 14.2g (0.1mol), triethylamine hydrochloride 13.8g (0.1mol), 4-chloroaniline 12.8g (0.1mol), 4-(4-pyridyl) methyl-2H-1-2,3-naphthyridine (1-) 6g (25mmol) mixes in the rearmounted 250ml reaction flask, oil bath adds the 23.1ml tetramethyl-urea in the reactive system after being heated to 170 ℃ of reaction 2h, adds the mixture cooling reactant of entry and ammoniacal liquor then.Add ether again, the sedimentation and filtration of generation.Solid matter adopts water and ether to wash respectively, obtains 6.1g product 1-(4-chloroanilino)-4-(4-picolyl)-2 (I), and yield is 70.5%.
Product structure confirms with mass spectrometric detection, m/z:346 (M)
Nuclear-magnetism detects:
1H NMR (DMSO-d6) δ 9.30 (sb, 1H), 8.60 (d, 1H), 8.46 (d, 2H), 8.0 (m, 5H), 7.40 (d, 2H), 7.33 (d, 2H), 4.59 (s, 2H).
Embodiment 2:
As described in embodiment 1, the amount that step (1) that different is adds sodium methylate is 8.1g (0.15mol), with the mol ratio of reactant be 1: 1, reaction obtains the 8g product, yield is 24%.
Embodiment 3:
As described in embodiment 1, the amount that step (1) that different is adds sodium methylate is 16.2g (0.3mol), with the mol ratio of reactant be 2: 1, reaction obtains the 15g product, yield is 44.8%.
Embodiment 4:
As described in embodiment 1, different is that step (2) reaction times is 5h, and reaction obtains the 15g product, and yield is 24.3%.
Embodiment 5:
As described in embodiment 1, different is that step (2) reaction times is 10h, and reaction obtains the 32g product, and yield is 52%.
Embodiment 6:
As described in embodiment 1, different is that step (3) oil bath temperature is 150 ℃, and reaction obtains the 2.1g product, and yield is 24.2%.
Embodiment 7:
As described in embodiment 1, different is that step (3) oil bath temperature is 180 ℃, and reaction obtains the 4.3g product, and yield is 49.7%.
Embodiment 8:
Suppress the experiment of mouse malignant growth:
The laboratory mice of suffering from tumour is divided into 4 groups, control group gives the physiological saline filling and feeds, the administration component for high (75mg/kg/day), in (50mg/kg/day), low (25mg/kg/day) dosage group give 1-(4-chloroanilino)-4-(4-picolyl)-2, the succinate solution of 3-naphthyridine (I) is irritated and is fed, regularly measure gross tumor volume, the results are shown in following table:
The result shows that compound 1-(4-chloroanilino)-4-(4-picolyl)-2 (I) can effectively suppress tumor growth.
Claims (2)
1, the preparation method of compound shown in the following molecular formula I:
Several steps synthesize below it is characterized in that branch:
(1) intermediate 3-hydroxyl-2-(4-pyridyl) 1-indenes is synthetic:
With the phthalide is raw material, and under 65 ℃, 1: 1 in molar ratio, with the reaction of 4-formaldehyde pyridine, strong alkali catalyst was selected sodium methylate for use, and the mol ratio of sodium methylate and reactant is 1-3: 1, and generation 3-hydroxyl-2-(4-pyridyl) 1-indenes, reaction times 1-3 hour;
(2) intermediate 4-(4-pyridyl) methyl-2H-1-2,3-naphthyridine synthetic:
3-hydroxyl-2-(4-pyridyl) 1-indenes is added in single hydrazine hydrate, volume ratio 0.1-0.3g/ml, 110 ℃ of temperature, reaction generates 4-(4-pyridyl) methyl-2H-1-2,3-naphthyridine, reaction times 5-15 hour;
(3) compound of molecular formula I is synthetic:
With 4-chloroaniline, 4-(4-pyridyl) methyl-2H-1-2, the 3-naphthyridine is 1-4 in molar ratio: 1, and temperature 150-190 ℃, frit reaction obtains 1-(4-chloroanilino)-4-(4-picolyl)-2, reaction times 1-3 hour.
2. according to the preparation method of the described compound of claim 1, in the described frit reaction of step (3), dewatering agent, phase-transfer catalyst and solubility promoter have been used; Wherein used dewatering agent is a Vanadium Pentoxide in FLAKES, and used phase-transfer catalyst is a triethylamine hydrochloride, and used solubility promoter is a tetramethyl-urea.
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