WO2018086546A1 - 2-多取代芳环-嘧啶类衍生物及制备和医药用途 - Google Patents

2-多取代芳环-嘧啶类衍生物及制备和医药用途 Download PDF

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WO2018086546A1
WO2018086546A1 PCT/CN2017/110029 CN2017110029W WO2018086546A1 WO 2018086546 A1 WO2018086546 A1 WO 2018086546A1 CN 2017110029 W CN2017110029 W CN 2017110029W WO 2018086546 A1 WO2018086546 A1 WO 2018086546A1
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alkyl
group
methyl
halogenated
cyano
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French (fr)
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刘滔
李佳
胡永洲
周宇波
董晓武
高安慧
宋品娆
王培培
童乐仙
胡小蓓
苏明波
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Zhejiang University ZJU
Shanghai Institute of Materia Medica of CAS
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Zhejiang University ZJU
Shanghai Institute of Materia Medica of CAS
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Priority to JP2019523735A priority Critical patent/JP6954566B2/ja
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Priority to CA3043519A priority patent/CA3043519C/en
Priority to EP17870509.1A priority patent/EP3530657B1/en
Publication of WO2018086546A1 publication Critical patent/WO2018086546A1/zh
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P35/00Antineoplastic agents
    • A61P35/02Antineoplastic agents specific for leukemia
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D401/00Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom
    • C07D401/14Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing three or more hetero rings
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D405/00Heterocyclic compounds containing both one or more hetero rings having oxygen atoms as the only ring hetero atoms, and one or more rings having nitrogen as the only ring hetero atom
    • C07D405/14Heterocyclic compounds containing both one or more hetero rings having oxygen atoms as the only ring hetero atoms, and one or more rings having nitrogen as the only ring hetero atom containing three or more hetero rings
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D409/00Heterocyclic compounds containing two or more hetero rings, at least one ring having sulfur atoms as the only ring hetero atoms
    • C07D409/14Heterocyclic compounds containing two or more hetero rings, at least one ring having sulfur atoms as the only ring hetero atoms containing three or more hetero rings
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D413/00Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and oxygen atoms as the only ring hetero atoms
    • C07D413/14Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and oxygen atoms as the only ring hetero atoms containing three or more hetero rings
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D417/00Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and sulfur atoms as the only ring hetero atoms, not provided for by group C07D415/00
    • C07D417/14Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and sulfur atoms as the only ring hetero atoms, not provided for by group C07D415/00 containing three or more hetero rings

Definitions

  • the present invention relates to the field of medicine, and in particular to a 2-polysubstituted aromatic ring-pyrimidine derivative and an optical isomer thereof, or a pharmaceutically acceptable salt or solvate thereof, a pharmaceutical composition therewith and the same in the field of antitumor Applications.
  • DNA-damaging drugs due to its poor selectivity, it can cause a variety of toxic side effects, and it will produce significant drug resistance during the treatment. Therefore, according to the action characteristics of DNA-damaging drugs, drugs with low toxicity are developed to be combined with DNA-damaging drugs, which can reduce the therapeutic effect of DNA-damaging drugs while reducing the toxic side effects and more. The risk of drug resistance. Among them, the development of cell cycle-related drugs and their strategies in combination with DNA-damaging drugs have attracted great interest and attention from drug researchers in recent years.
  • Eukaryotic cells have their own regulatory mechanisms. When exposed to external stimuli such as radiotherapy or chemotherapy, it can be temporarily blocked in the G1, S or G2/M phase for DNA repair, and after completion of the repair, it will enter the next phase.
  • a large number of protein kinases in cells interact with the same or different signaling pathways, forming an intricate signal network that regulates cell growth, proliferation, angiogenesis, metastasis, apoptosis and other life activities.
  • the tumor gene suppressor protein p53 is mainly responsible for the regulation of the G1 checkpoint, while the S and G2/M phases are mainly regulated by the cell cycle checkpoint kinase 1 (Checkpoint kinase 1).
  • Chk1 inhibitor can be used as an adjuvant therapy to selectively enhance the sensitivity of tumor cells to radiotherapy or chemotherapy and improve the therapeutic effect.
  • Chk1 inhibitors can also be used alone, killing tumor cells through a "synthetic lethal" mechanism to achieve therapeutic purpose. Based on this therapeutic strategy, Chk1 inhibitors can be used alone in the treatment of B-cell lymphoma, leukemia, neuroblastoma, and some sensitive tumors with high expression of proto-oncogenes such as breast and lung cancer.
  • Chk1 inhibitors small molecular compounds of different structural types have been discovered as Chk1 inhibitors, and these compounds have shown strong anti-tumor effects in preclinical evaluation.
  • 11 small molecule Chk1 inhibitors have entered clinical research, which proves the correctness of Chk1 as a tumor treatment target.
  • An object of the present invention is to provide a 2-polysubstituted aromatic ring-pyrimidine derivative and an optical isomer thereof, or a pharmaceutically acceptable salt or solvate thereof. It is a novel 2-polysubstituted aromatic ring-pyrimidine derivative with strong anticancer activity and Chk1 inhibition.
  • the 2-polysubstituted aromatic ring-pyrimidine derivatives provided by the present invention have the structure of the general formula (I):
  • Ring A is selected from substituted or unsubstituted five- or six-membered aryl groups, and contains one to three five- or six-membered heterocyclic aryl groups selected from O, N and S, the substituted substituents being selected from the group consisting of And an R 5 group; wherein ring A is preferably the following five to six membered nitrogen-containing aromatic heterocyclic ring:
  • B is selected from -NH, Wherein B 1 is from H, C 1-4 alkyl, halogenated C 1-4 alkyl, C 1-4 alkoxy, halogenated C 1-4 alkoxy;
  • R 1 is selected from a halogen atom, a C 1-6 alkyl group, a halogenated C 1-6 alkyl group, a C 3-6 cycloalkyl group, a halogenated C 3-6 cycloalkyl group, a C 1-6 alkoxy group.
  • the group is selected from the group consisting of R a ; preferably, the aryl or heterocyclic aryl group is selected from the group consisting of a benzene ring, a furan, a thiophene, a pyrazole, a thiazole, and a pyrimidine;
  • R b is optionally selected from H, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1- 3 alkoxy, C 1-7 alkylamino;
  • R 2 is selected from the group consisting of H, -NHRc, -N(Rc) 2 , -ORc, -SRc; Rc is selected from C 1-7 alkyl, halogenated C 1-7 alkyl, C 1-7 hydroxyalkyl, C 1-7 aminoalkyl;
  • R 3 is selected from the group consisting of halogen, nitro, cyano, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1-3 alkoxy, C 1 a -3 alkylamino group, a halogenated C 1-3 alkylamino group;
  • L 1 is selected from O, S, NH or a deletion
  • R 4 is selected from C 1-7 alkyl, halo C 1-7 alkyl, hydroxy substituted C 1-7 alkyl, C 1-7 alkylamino, halo C 1-7 alkylamino, a C 1-7 alkoxy group, a halogenated C 1-7 alkoxy group, a five- to eight-membered nitrogen-containing aliphatic heterocyclic ring;
  • R 5 is selected from the group consisting of halogen, nitro, cyano, trifluoromethyl, C 1-3 alkyl, C 1-3 alkoxy, amide, substituted alkyl amide.
  • preferred compounds of the invention have the structure of formula (II) or formula (III):
  • W, X, Y and Z are the same or different and are independently selected from N, C and O;
  • B is selected from -NH, Wherein B 1 is selected from the group consisting of H, C 1 -4 alkyl, halogenated C 1-4 alkyl, C 1-4 alkoxy, halogenated C 1-4 alkoxy;
  • R 1 is selected from a halogen atom, a C 1-6 alkyl group, a halogenated C 1-6 alkyl group, a C 3-6 cycloalkyl group, a halogenated C 3-6 cycloalkyl group, a C 1-6 alkoxy group.
  • R b is optionally selected from H, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1- 3 alkoxy, C 1-7 alkylamino;
  • R 2 is selected from the group consisting of H, -NHRc, -N(Rc) 2 , -ORc, -SRc; Rc is selected from C 1-7 alkyl, halogenated C 1-7 alkyl, C 1-7 hydroxyalkyl, C 1-7 aminoalkyl, C 1-7 alkoxy;
  • R 3 is selected from the group consisting of halogen, nitro, cyano, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1-3 alkoxy, C 1 a -3 alkylamino group, a halogenated C 1-3 alkylamino group;
  • L 1 is selected from O, S, NH or a deletion
  • R 5 is selected from the group consisting of halogen, nitro, cyano, trifluoromethyl, C 1-3 alkyl, C 1-3 alkoxy, amide, substituted alkyl amide.
  • W, X, Y and Z are the same or different and are each independently selected from N or C;
  • B is selected from -NH, Wherein B 1 is selected from the group consisting of H, C 1 -4 alkyl, halogenated C 1-4 alkyl, C 1-4 alkoxy, halogenated C 1-4 alkoxy;
  • R 1 is selected from a halogen atom, a C 1-6 alkyl group, a halogenated C 1-6 alkyl group, a C 3-6 cycloalkyl group, a halogenated C 3-6 cycloalkyl group, a C 1-6 alkoxy group.
  • R b is optionally selected from H, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1- 3 alkoxy, C 1-7 alkylamino;
  • R 2 is selected from the group consisting of H, -NHRc, -N(Rc) 2 , -ORc, -SRc; Rc is selected from the group consisting of C 1-7 alkyl, C 1-7 hydroxyalkyl, C 1-7 aminoalkyl;
  • R 3 is selected from the group consisting of halogen, nitro, cyano, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1-3 alkoxy, C 1 a -3 alkylamino group, a halogenated C 1-3 alkylamino group;
  • L 1 is selected from O, S, NH or a deletion
  • R 4 is selected from H, C 1-7 alkyl, halogenated C 1-7 alkyl, hydroxy substituted C 1-7 alkyl, C 1-7 alkylamino group, a halogenated C 1- 7 alkyl amine a group, a C 1-7 alkoxy group, a halogenated C 1-7 alkoxy group, a five- to eight-membered nitrogen-containing aliphatic heterocyclic ring;
  • R 5 is selected from the group consisting of halogen, nitro, cyano, trifluoromethyl, C 1-3 alkyl, C 1-3 alkoxy, amide, substituted alkyl amide.
  • preferred compounds of the invention have the structure of formula (IV) or formula (V):
  • W, X, Y and Z are the same or different and are independently selected from N, C and O;
  • R 1 is selected from a halogen atom, a C 1-6 alkyl group, a halogenated C 1-6 alkyl group, a C 3-6 cycloalkyl group, a halogenated C 3-6 cycloalkyl group, a C 1-6 alkoxy group.
  • the group is selected from the group consisting of R a ;
  • R b is optionally selected from H, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1- 3 alkoxy, C 1-7 alkylamino;
  • R 2 is selected from the group consisting of H, -NHRc, -N(Rc) 2 , -ORc, -SRc; Rc is selected from the group consisting of C 1-7 alkyl, C 1-7 hydroxyalkyl, C 1-7 aminoalkyl;
  • R 3 is selected from the group consisting of halogen, nitro, cyano, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1-3 alkoxy, C 1 a -3 alkylamino group, a halogenated C 1-3 alkylamino group;
  • L 1 is selected from O, S, NH or a deletion
  • R 4 is selected from H, C 1-7 alkyl, halogenated C 1-7 alkyl, hydroxy substituted C 1-7 alkyl, C 1-7 alkylamino group, a halogenated C 1- 7 alkyl amine a group, a C 1-7 alkoxy group, a halogenated C 1-7 alkoxy group, a five- to eight-membered nitrogen-containing aliphatic heterocyclic ring;
  • R 5 is selected from the group consisting of halogen, nitro, cyano, trifluoromethyl, C 1-3 alkyl, C 1-3 alkoxy, amide, substituted alkyl amide.
  • preferred compounds of the formula (IV) of the present invention are selected from the group consisting of:
  • W, X, Y and Z are the same or different and are each independently selected from N or C;
  • R 1 is selected from a halogen atom, a C 1-6 alkyl group, a halogenated C 1-6 alkyl group, a C 3-6 cycloalkyl group, a halogenated C 3-6 cycloalkyl group, a C 1-6 alkoxy group.
  • the group is selected from the group consisting of R a ;
  • R b is optionally selected from H, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1- 3 alkoxy, C 1-7 alkylamino;
  • R 2 is selected from the group consisting of H, -NHRc, -N(Rc) 2 , -ORc, -SRc; Rc is selected from the group consisting of C 1-7 alkyl, C 1-7 hydroxyalkyl, C 1-7 aminoalkyl;
  • R 3 is selected from the group consisting of halogen, nitro, cyano, C 1-3 alkyl, halogenated C 1-3 alkyl, C 1-3 alkoxy, halogenated C 1-3 alkoxy, C 1 a -3 alkylamino group, a halogenated C 1-3 alkylamino group;
  • L 1 is selected from O, S, NH or a deletion
  • R 4 is selected from H, C 1-7 alkyl, halogenated C 1-7 alkyl, hydroxy substituted C 1-7 alkyl, C 1-7 alkylamino group, a halogenated C 1- 7 alkyl amine a group, a C 1-7 alkoxy group, a halogenated C 1-7 alkoxy group, a five- to eight-membered nitrogen-containing aliphatic heterocyclic ring;
  • R 5 is selected from the group consisting of halogen, nitro, cyano, trifluoromethyl, C 1-3 alkyl, C 1-3 alkoxy, amide, substituted alkyl amide.
  • preferred compounds of the general structure (V) of the present invention are selected from the group consisting of:
  • the present invention can prepare salts of the 2-substituted pyrimidine compounds of the present invention by methods well known to those skilled in the art.
  • the salt may be an organic acid salt, a mineral acid salt or the like, and the organic acid salt includes a decanoate, a fumarate, an oxalate, a malate, an L-malate, and a D-malic acid. Salt, lactate, camphorsulfonate, p-toluenesulfonate, methanesulfonate, benzoate, etc.; the inorganic acid salt includes a hydrohalide, a sulfate, a phosphate, a nitrate, and the like.
  • a lower alkylsulfonic acid such as methanesulfonic acid, trifluoromethanesulfonic acid or the like may form a mesylate salt, a triflate salt; and an arylsulfonic acid such as benzenesulfonic acid or p-toluenesulfonic acid.
  • Corresponding salts may also be formed with inorganic acids such as hydrohalic acids (e.g., hydrofluoric acid, hydrobromic acid, hydroiodic acid, hydrochloric acid), nitric acid, carbonic acid, sulfuric acid or phosphoric acid.
  • hydrohalic acids e.g., hydrofluoric acid, hydrobromic acid, hydroiodic acid, hydrochloric acid
  • nitric acid e.g., carbonic acid, sulfuric acid or phosphoric acid.
  • a second object of the present invention is to provide a pharmaceutical composition comprising at least one active ingredient together with one or more pharmaceutically acceptable carriers or excipients, said active ingredient It may be a 2-substituted pyrimidine compound of the present invention, an optical isomer of the compound, a solvate of the compound or an optical isomer thereof in a pharmaceutically acceptable salt, the compound or an optical isomer thereof Any one or any of a variety of them.
  • the carrier includes conventional diluents, excipients, fillers, binders, wetting agents, disintegrating agents, absorption enhancers, surfactants, adsorption carriers, lubricants, etc. in the pharmaceutical field, and may also be added if necessary. Agent, sweetener, etc.
  • the medicament of the present invention can be prepared into various forms such as tablets, powders, granules, capsules, oral liquids and injectable preparations, and the medicaments of the above respective dosage forms can be prepared according to a conventional method in the pharmaceutical field.
  • the present invention also provides a compound of the formula (I) to the formula (V), and an optical isomer thereof, or a pharmaceutically acceptable salt or solvate thereof, and an optical isomer thereof, or a pharmaceutically acceptable compound thereof
  • the cell proliferative diseases include tumors, and the tumors are breast cancer, ovarian cancer, sarcoma, lung cancer, prostate cancer, colon cancer, rectal cancer, renal cancer, pancreatic cancer, blood cancer, lymphoma, neuroblastoma, and nerve.
  • Glioma head cancer, neck cancer, thyroid cancer, liver cancer, vulvar cancer, cervical cancer, endometrial cancer, testicular cancer, bladder cancer, esophageal cancer, stomach cancer, nasopharyngeal cancer, buccal cancer, oral cancer, gastrointestinal Interstitial tumor, skin cancer, multiple myeloma.
  • Antitumor agents for use in combination with pharmaceutically acceptable salts include, but are not limited to, at least one of the following classes: antimetabolites (gemcitabine, 5-fluorouracil, hydroxyurea, pemetrexed); alkylating agents (eg, cisplatin, card) Platinum); topoisomerase inhibitors (irinotecan, doxorubicin); small molecule inhibitors (MEK inhibitors, PARP inhibitors, Scr family kinase inhibitors, mTOR inhibitors, farnesyltransferase inhibitors) Wait).
  • antimetabolites gemcitabine, 5-fluorouracil, hydroxyurea, pemetrexed
  • alkylating agents eg, cisplatin, card
  • topoisomerase inhibitors irinotecan, doxorubicin
  • small molecule inhibitors MEK inhibitors, PARP inhibitors, Scr family kinase inhibitors, mTOR inhibitors, farnesyltransferas
  • Another object of the present invention is to provide a process for the preparation of the above target compound by the following steps:
  • Compound 7-16 was prepared according to the following synthetic route:
  • the inventors of the present invention have experimentally confirmed that most of the compounds of the present invention have moderate to strong Chk1 kinase inhibitory activity and are useful for the treatment of solid tumors or blood cancers associated with cell proliferation in human or animal cells.
  • a series of novel small molecule Chk1 inhibitors were designed and synthesized by using 2-aminopyrimidine as a lead compound obtained by structure-based virtual screening, and the compounds were tested for molecular level Chk1 kinase inhibitory activity. The results showed that most of the compounds exhibited moderate to strong Chk1 inhibitory activity and were promising Chk1 inhibitors, providing new drugs for cancer therapy.
  • Figure 1 shows the activity of a CHK1 inhibitor in combination with other drugs on MV 4-11 cells.
  • N-tert-Butoxycarbonyl-4-hydroxypiperidine (460 mg, 2.29 mmol) was dissolved in anhydrous THF (7.2 mL), EtOAc (EtOAc) Stir under 10 min. The temperature was raised to 35 ° C and stirred for 10 min. 3-Bromo-1-methyl-5-nitropyrazole (360 mg, 1.75 mmol) was placed in a 50 mL three-necked flask, and anhydrous THF (4.8 mL) was added under nitrogen to dissolve the sodium salt obtained above slowly. The mixture was added dropwise to the reaction solution (completed in about 20 min), and stirred at room temperature for 1 h.
  • EtOAc EtOAc
  • 5-Bromo-2,4-dichloropyrimidine 500 mg, 2.194 mmol was dissolved in anhydrous methanol (5 mL), and a solution of sodium methoxide (sodium 56 mg, 2.42 mmol) in methanol (1.85 mL) Stir at room temperature overnight. Saturated ammonium chloride solution was added to quench the reaction, recovery of the solvent under reduced pressure, added to the washed CH 2 Cl 2 (30mL), washed with water (30 mL) under reduced pressure to recover the solvent.
  • Step 4. Prepare compound 2-21 to 2-33 with intermediate 1-5 and the corresponding boronic acid as a white solid.
  • Step 2 N 4 -Methyl-5-bromo-N 2 -(2-cyano-3-(N-tert-butoxycarbonylpiperidin-3-yloxy)pyridin-5-yl)-2,4- Synthesis of diaminopyrimidine (intermediate 2-45)
  • step 2 of the embodiment 2 step 2 of the first embodiment, and the compound 2-49/2-51 is obtained.
  • Step 5 Prepare compound 46-50 from 2-16, 2-13, 2-35, 2-44 and intermediate 2-50/2-52, respectively, to give a white solid.
  • the nuclear magnetic and mass spectrometry data of the intermediates 2-21 to 2-33, 2-36 to 2-42, and the compounds 19-31 and 34-43 are shown in Tables 1-1, 1-2, 1-3, and 1-4.
  • the Chk1 enzyme inhibitory activity (IC 50 ) was evaluated using the ADP-Glo kit with Staurosporine as a positive control.
  • the compound acts on Chk1 protein kinase and inhibits its phosphorylation substrate Cdc25C.
  • the phosphorylation process consumes ATP.
  • ADP-Glo TM Reagent is used to consume the remaining ATP.
  • the ADP produced during the reaction can be ADP-Glo Detection Reagent. is converted to ATP, ATP can be used as a substrate TM luciferase-catalyzed reaction Ultra-Glo, generating an optical signal.
  • test compound was dissolved in DMSO to make a 10 mM stock solution, and diluted to a certain concentration in a certain ratio for testing.
  • DMSO DMSO
  • 384-well plate add 1 ⁇ L of the test compound to each well, 2 ⁇ L of 2.5X Chk1 kinase, add 2 ⁇ L of 1X buffer to the control group, incubate for 10 min at room temperature, add 2 ⁇ L of 2.5X substrate, incubate at 37 ° C for 1 h, add ADP- Glo TM Reagent 5 ⁇ L to terminate the reaction, incubated for 1h at 37 °C.
  • Chk1 inhibitory activity of 24 compounds is comparable to that of the positive compound Staurosporine, and the 5 compounds are superior to the positive control Staurosporine. Therefore, the 2-substituted pyrimidine derivatives useful as Chk1 inhibitors of the present invention have broad antitumor application prospects.
  • Cell lines human multiple myeloma cells RPMI 8226, human mantle cell lymphoma cells Mino, Jeko-1, human lymphoma cells Romas, human acute monocytic leukemia cells MV-4-11, human breast cancer cells MCF-7 Human lung cancer cell A549, human prostate cancer cell LnCAP, human gastric cancer cell BGC-823, human colon cancer cell HCT116, Colo205, human ovarian cancer cell OVCAR-8
  • Experimental method MTS assay for in vitro proliferation of compounds against different tumor cell lines Inhibitory activity (IC 50 ).
  • the cells in the logarithmic growth phase were trypsinized, counted, and seeded at a density of 1 ⁇ 10 4 cells/well in a 96-well plate at 100 ⁇ L per well in a 37 ° C incubator containing 5% CO 2 overnight.
  • For the culture six concentration gradients were set for each compound, and three sets of duplicate wells were set for each concentration.
  • the cells were cultured for 72 hours, and 20 ⁇ L of MTS was added. After incubation at 37 ° C for 2 hours, the absorbance at 490 nm (L1) was measured with a SpectraMAX 340 plate reader.
  • the reference wavelength was 690 nm (L2), and the (L1-L2) value was plotted against the different concentrations of the inhibitor.
  • the half-inhibitory concentration IC 50 was fitted.
  • Table 3-1 Compound inhibits proliferation of each tumor cell line
  • IC 50 average of three experiments; b not measured.
  • MV 4-11 cells were seeded at 5000/well into 96-well plates.
  • the drug is determined according to the ratio of IC 50 of the two drugs.
  • the concentration of each drug is selected from IC 20 to IC 80 (or 1/8, 1/4, 1/2, 1, 2 and 4 of IC 50 ).
  • cell viability was measured by the addition of MTS reagent, and the inhibition rate Fa was calculated as 100% of the unmedicated group.
  • the Chou-Talalay method was used to analyze the inhibition rate Fa and the corresponding drug concentration into CompuSyn software, and the CI value and Fa-CI curve of single concentration drug were obtained.
  • the drug concentration at X, DA and DB are the concentrations of the two drugs when the growth inhibition rate reaches X when the two drugs are combined. The results are shown in Figure 1.
  • CHK1 inhibitor 35
  • FLT3 inhibitor Crenolanib Cre
  • Quizartinib Q
  • Akt inhibitor GSK2141795 GSK
  • CI combination index, according to the judgment method of Soriano et al, 0.9 ⁇ CI ⁇ 1.1 Superposition effect, 0.8 ⁇ CI ⁇ 0.9 is a low degree synergy, 0.6 ⁇ CI ⁇ 0.8 is a moderate synergy, 0.4 ⁇ CI ⁇ 0.6 is a highly synergistic effect, and 0.2 ⁇ CI ⁇ 0.4 is a strong synergistic effect.

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Abstract

本发明提供一种2-多取代芳环-嘧啶类衍生物及其光学异构体或其药学上可接受的盐或溶剂合物,所述的化合物、及其光学异构体或其药学上可接受的盐或溶剂合物可在制备抗肿瘤药物中的应用。本发明以通过基于结构的虚拟筛选得到的N-取代吡啶-2-氨基嘧啶为先导化合物,设计并合成了一系列全新的小分子Chk1抑制剂,并对该类化合物进行了分子水平的Chk1激酶抑制活性测试。实验证实,所述化合物是一种抗癌作用强,具有Chk1激酶抑制活性,是有前景的Chk1抑制剂,是新的癌症治疗药物,可应用于治疗人或动物细胞增殖性相关的实体瘤或血癌。本发明提供的2-多取代芳环-嘧啶类衍生物具有通式Ⅰ结构:

Description

2-多取代芳环-嘧啶类衍生物及制备和医药用途 技术领域
本发明涉及药物领域,具体涉及2-多取代芳环-嘧啶类衍生物及其光学异构体或其药学上可接受的盐或溶剂合物、含其的药物组合物及其在抗肿瘤领域的应用。
背景技术
随着人类生存环境的变化及人口老龄化,恶性肿瘤正严重威胁着人类的生命,在我国恶性肿瘤已成为第一大致死疾病。传统的癌症的治疗方法主要有手术治疗、放射治疗和药物化疗等,其中以药物化疗最为重要。近年来,随着肿瘤分子靶标被逐渐阐释,不少靶向抗肿瘤药物己进入临床应用,但由于肿瘤的复杂性、遗传的多样性,单一靶向药物并不足以治愈肿瘤。传统的化疗药物大多为DNA损伤药物,其通过直接干扰肿瘤细胞的DNA合成,调控DNA的转录、修复等过程诱导肿瘤细胞凋亡,延长癌症患者的生存期。但因其选择性差,会引起多种毒副作用,且治疗过程中会产生明显的耐药性。因此,根据DNA损伤药物的作用特点,开发本身毒性低的药物,使之与DNA损伤药物联合用药,在降低DNA损伤药物用药剂量的同时,增强DNA损伤药物的治疗效果,可降低毒副作用及多药耐药发生的风险。其中,针对细胞周期相关药物的研发及其与DNA损伤药物联合用药的策略近年来引起了药物研究人员的极大兴趣和广泛关注。
真核细胞具有自身调控机制。在受到放、化疗等外界刺激时,可暂时被阻滞在G1,S或G2/M期进行DNA修复,完成修复后进入下一时相。细胞中大量的蛋白激酶相互作用于同一或不同的信号通路,构成了错综复杂的信号网络,共同调节着细胞的生长、增殖、血管生成、转移、凋亡等生命活动。其中,肿瘤基因抑制蛋白p53主要负责G1期检查点的调控,而S和G2/M期则主要由细胞周期检查点激酶1(Checkpoint kinase 1)调控。大部分肿瘤细胞因p53功能的缺失而更加依赖S或G2/M期的阻滞作为DNA损伤诱导凋亡的防御机制。针对p53缺失的肿瘤细胞,抑制Chk1蛋白可清除细胞周期阻滞,直接诱导肿瘤细胞凋亡,而正常细胞由于存在完整的p53调控机制,会被暂时阻滞在G1期而不受影响。因此,Chk1抑制剂可作为辅助治疗药物,选择性地增强肿瘤细胞对放疗或化疗的敏感性,改善治疗效果。
此外,在特定基因缺陷的背景下,如固有DNA损伤过高而造成较大复制压力存在的情况下,Chk1抑制剂也可单独使用,通过“合成致死”的机制杀死肿瘤细胞,达到治疗的目的。基于这一治疗策略,Chk1抑制剂可单用于B细胞淋巴癌、白血病、成神经细胞瘤及一些乳腺癌和肺癌等原癌基因高表达的敏感肿瘤的治疗。
过去的二十年中,不同结构类型的小分子化合物已经作为Chk1抑制剂被发现,这些化合物在临床前体内外评价中表现出了较强的抗肿瘤作用。目前,已有11个小分子Chk1抑制剂进入了临床研究,更加验证了Chk1作为肿瘤治疗靶点的正确性。
发明内容
本发明的目的是提供一种2-多取代芳环-嘧啶类衍生物及其光学异构体或其药学上可接受的盐或溶剂合物。是一种抗癌作用强,具有Chk1抑制作用的新型2-多取代芳环-嘧啶类衍生物。
本发明所提供的2-多取代芳环-嘧啶类衍生物具有通式(Ⅰ)结构:
Figure PCTCN2017110029-appb-000001
及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
环A选自取代或无取代的五元或六元芳基、包含1~3个选自O、N和S的五元或六元杂环芳基,所述取代的取代基选自
Figure PCTCN2017110029-appb-000002
和R5基团;其中环A优选下列五元~六元的含氮芳杂环:
Figure PCTCN2017110029-appb-000003
B选自-NH、
Figure PCTCN2017110029-appb-000004
其中B1自H、C1-4烷基、卤代的C1-4烷基、C1-4烷氧基、卤代的C1-4烷氧基;
R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基、无取代或取代的五元或六元芳环或芳杂环,所述的芳杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;作为优选,所述的芳基或者杂环芳基选自苯环、呋喃、噻吩、吡唑、噻唑、嘧啶;
Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、卤代的C1-7烷基、C1-7羟烷基、C1-7胺烷基;
R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
L1选自O、S、NH或者缺失;
m=0~2;
R4选自C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1-7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
进一步地,本发明优选的化合物具有通式(Ⅱ)或通式(III)的结构:
Figure PCTCN2017110029-appb-000005
及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
W、X、Y和Z相同或不同,分别独立选自N、C和O;
B选自-NH、
Figure PCTCN2017110029-appb-000006
其中B1选自H、C1- 4烷基、卤代的C1-4烷基、C1-4烷氧基、卤代的C1-4烷氧基;
R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基,无取代或取代的五元或六元芳环或芳杂环,所述的杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;
Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、卤代的C1-7烷基、C1-7羟烷基、C1-7胺烷基、C1-7烷氧基;
R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
L1选自O、S、NH或者缺失;
m=0~2;
R4选自H、C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1- 7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
Figure PCTCN2017110029-appb-000007
及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
W、X、Y和Z相同或不同,分别独立选自N或C;
B选自-NH、
Figure PCTCN2017110029-appb-000008
其中B1选自H、C1- 4烷基、卤代的C1-4烷基、C1-4烷氧基、卤代的C1-4烷氧基;
R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基、无取代或取代的五元或六元芳环或芳杂环,所述的杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;
Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、C1-7羟烷基、C1-7胺烷基;
R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
L1选自O、S、NH或者缺失;
m=0~2;
R4选自H、C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1- 7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
更进一步地,本发明优选的化合物具有通式(Ⅳ)或通式(V)的结构:
Figure PCTCN2017110029-appb-000009
及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
W、X、Y和Z相同或不同,分别独立选自N、C和O;
R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基,无取代或取代的五元或六元芳环或芳杂环,所述的芳杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;
Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、C1-7羟烷基、C1-7胺烷基;
R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
L1选自O、S、NH或者缺失;
m=0~2
R4选自H、C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1- 7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
更具体地,本发明通式(Ⅳ)结构的优选化合物选自:
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(1-甲基-5-(哌啶-4-氧基)吡唑-3-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(3-(哌啶-4-氧基)异恶唑-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(1-甲基-2-(哌啶-4-氧基)咪唑-4-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)异噻唑-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)-4,5-2H-恶唑啉-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)噻唑-5-基)-2,4-二氨基嘧啶
进一步地,本发明优选的化合物具有通式(V)结构
Figure PCTCN2017110029-appb-000010
及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
W、X、Y和Z相同或不同,分别独立选自N或C;
R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基、无取代或取代的五元或六元芳环或芳杂环,所述的芳杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;
Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、C1-7羟烷基、C1-7胺烷基;
R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
L1选自O、S、NH或者缺失;
m=0~2;
R4选自H、C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1- 7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
更具体地,本发明通通式(V)结构的优选化合物选自:
5-苯基-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
5-(3-氟苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
5-(4-氟苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
5-(3-甲氧基苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
5-(4-甲氧基苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
5-(吡啶-3-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
5-(吡啶-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
5-(噻吩-2-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
5-(呋喃-2-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
5-三氟甲基-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
(R)-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
(S)-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
4-甲氧基-5-(3-氟苯基)-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶
4-甲氧基-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶
4-甲氧基-5-(3-氟苯基)-N-(2-氰基-3-(2-二甲氨基乙氧基)吡啶-5-基)-2-氨基嘧啶
4-甲氧基-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(2-二甲氨基乙氧基)吡啶-5-基)-2-氨基嘧啶
4-甲氧基-5-三氟甲基-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶
N4-甲基-5-苯基-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(3-氟苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(4-氟苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(2-氟苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(3-甲氧基苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(4-甲氧基苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(2,4-二甲氧基苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(吡啶-3-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(吡啶-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(噻吩-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(呋喃-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(5-氯-呋喃-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(5-甲氧羰基噻吩-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-5-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-三氟甲基-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2,4-二氨基嘧啶
(R)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
(S)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
(R)-N4-甲基-5-三氟甲基-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
(S)-N4-甲基-5-三氟甲基-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
(R)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(吡咯-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
(S)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(吡咯-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-4-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(2-二甲氨基乙氧基)吡啶-5-基)-2,4-二氨基嘧啶
(R)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(1-二甲氨基丙基-2-氧基)吡啶-5-基)-2,4-二氨基嘧啶
(S)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(1-二甲氨基丙基-2-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(N-甲基哌啶-4-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-三氟甲基-N2-(2-氰基-3-(N-甲基哌啶-4-氧基)吡啶-5-基)-2,4-二氨基嘧啶
N4-甲基-5-(4-甲基噻唑-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
及其上述化合物的药学上可接受的盐或溶剂合物。
本发明采用本领域技术人员所熟知的方法可以制备本发明所述的2-取代嘧啶类化合物的盐。所述的盐可以是有机酸盐、无机酸盐等,所述的有机酸盐包括枸橼酸盐、富马酸盐、草酸盐、苹果酸盐、L-苹果酸盐、D-苹果酸盐、乳酸盐、樟脑磺酸盐、对甲苯磺酸盐、甲磺酸盐、苯甲酸盐等;所述的无机酸盐包括氢卤酸盐、硫酸盐、磷酸盐、硝酸盐等。例如,与低级烷基磺酸,如甲磺酸,三氟甲磺酸等可形成甲磺酸盐、三氟甲磺酸盐;与芳基磺酸,如苯磺酸或对甲苯磺酸等可形成对甲苯磺酸盐、苯磺酸盐;与有机羧酸,如乙酸,富马酸,酒石酸盐、L-酒石酸,D-酒石酸草酸,马来酸,苹果酸盐、L-苹果酸,D-苹果酸,琥珀酸或柠檬酸等可形成相应的盐;与氨基酸,如谷氨酸或天冬氨酸可形成谷氨酸盐或天冬氨酸盐。与无机酸,如氢卤酸(如氢氟酸、氢溴酸、氢碘酸、氢氯酸),硝酸,碳酸,硫酸或磷酸等也可形成相应的盐。
本发明的第二个目的是提供一种药物组合物,所述药物组合物包含至少一种活性组分以及一种或多种药学上可接受的载体或赋形剂,所述的活性组分可以是本发明的2-取代嘧啶类化合物、所述化合物的光学异构体、所述化合物或其光学异构体在药学上可接受的盐、所述化合物或其光学异构体的溶剂合物中的任意一种或任意多种。
所述载体包括药学领域的常规稀释剂,赋形剂,填充剂,粘合剂,湿润剂,崩解剂,吸收促进剂,表面活性剂,吸附载体,润滑剂等,必要时还可以加入香味剂,甜味剂等。本发明药物可以制成片剂,粉剂,粒剂,胶囊,口服液及注射用药等多种形式,上述各剂型的药物均可以按照药学领域的常规方法制备。
本发明还提供通式(I)~通式(V)所述的化合物、及其光学异构体或其药学上可接受的盐或溶剂合物、及其光学异构体或其药学上可接受的盐或溶剂合物单独和/或与放疗、其他药物联合使用在制备Chk1抑制剂中的应用,特别是在制备治疗细胞增生疾病中的应用。所述的细胞增生疾病包括肿瘤,所述的肿瘤为乳腺癌、卵巢癌、肉瘤、肺癌、前列腺癌、结肠癌、直肠癌、肾癌、胰腺癌、血癌、淋巴癌、成神经细胞瘤、神经胶质瘤、头癌、颈癌、甲状腺癌、肝癌、外阴癌、子宫颈癌、子宫内膜癌、睾丸癌、膀胱癌、食管癌、胃癌、鼻咽癌、颊癌、口腔癌、胃肠道间质瘤、皮肤癌、多发性骨髓瘤。能和本发明所提供的化合物或 其可药用盐联合使用的抗肿瘤药包括但并非限定至少一种以下种类:抗代谢药物(吉西他滨,5-氟尿嘧啶,羟基脲,培美曲赛);烷基化试剂(如顺铂、卡铂);拓扑异构酶抑制剂(伊立替康、多柔比星);小分子抑制剂(MEK抑制剂,PARP抑制剂,Scr家族激酶抑制剂,mTOR抑制剂,法尼基转移酶抑制剂等)。
本发明的另一个目的是提供上述目标化合物的制备方法,通过以下步骤实现:
方法一:
(1)5-溴-2-取代-3-硝基吡啶(或5-溴-2-氰基-3-硝基吡啶)在碱性条件(NaH存在的条件)下,与不同的脂肪醇经取代反应得到不同取代的吡啶片段;
(2)以5-溴-2,4-二氯嘧啶为起始原料,依次经甲醚化(或甲胺化)和氨化得到5-溴-2,4-二取代嘧啶或以2-氨基嘧啶为原料经溴代后得到5-溴-2-氨基嘧啶,先经Suzuki偶联,再与上述吡啶片段发生钯催化的Buchwald-Hartwig交叉偶联反应,最后脱Boc保护基得到目标化合物;也可以采用2-氨基嘧啶中间体先与取代的5-溴吡啶经Buchwald-Hartwig交叉偶联,然后经Suzuki偶联反应,酸性条件下脱Boc保护基得到目标分子;
化合物1-6按照下列合成路线制备:
Figure PCTCN2017110029-appb-000011
化合物7-16按照下列合成路线制备:
Figure PCTCN2017110029-appb-000012
化合物17-43按照下列合成路线制备:
Figure PCTCN2017110029-appb-000013
化合物44按照下列合成路线制备:
Figure PCTCN2017110029-appb-000014
方法二:
(1)5-溴-2-氰基-3-硝基吡啶在碱性条件(NaH存在的条件)下,与不同的脂肪醇经取代反应得到不同取代的吡啶片段;
(2)以2,4-二氯-5-三氟甲基嘧啶为起始原料,依次经甲醚化(或甲胺化)和氨化得到2,4-二取代-5-三氟甲基嘧啶或以2-氯-5-三氟甲基嘧啶为原料经氨化,再与上述吡啶片段发生钯催化的Buchwal-Hartwig交叉偶联反应,最后脱Boc保护基得到目标化合物。
化合物45合成路线如下:
Figure PCTCN2017110029-appb-000015
化合物46-50合成路线如下:
Figure PCTCN2017110029-appb-000016
本发明发明人通过实验证实,本发明中的大部分化合物具有中等到强的Chk1激酶抑制活性,可应用于治疗人或动物细胞增殖性相关的实体瘤或血癌的药物中。本发明以通过基于结构的虚拟筛选得到的2-氨基嘧啶为先导化合物,设计并合成了一系列全新的小分子Chk1抑制剂,并对该类化合物进行了分子水平的Chk1激酶抑制活性测试。结果表明,大部分化合物表现出中等到强的Chk1抑制活性,是有前景的Chk1抑制剂,为癌症治疗提供了新的药物。
附图说明
图1是CHK1抑制剂与其他药物在MV 4-11细胞上联用的活性。
具体实施方式
本发明结合实施例作进一步的说明,以下实施例仅是说明本发明,而不是以任何方式限制本发明。
制备实施例1.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(1-甲基-5-(哌啶-4-氧基)吡唑-3-基)-2,4-二氨基嘧啶(化合物1)
Figure PCTCN2017110029-appb-000017
步骤1.N-叔丁氧羰基-4-((3-溴-1-甲基-1H-吡唑-5-基)氧基)哌啶(中间体1-2)合成
Figure PCTCN2017110029-appb-000018
将N-叔丁氧羰基-4-羟基哌啶(460mg,2.29mmol)溶于无水THF(7.2mL)中,冰浴冷却下,分批加入60%氢化钠(108mg,4.5mmol),室温下搅拌10min。升温至35℃,搅拌10min。将3-溴-1-甲基-5-硝基吡唑(360mg,1.75mmol)置于50mL三颈瓶中,氮气保护下加入无水THF(4.8mL),将上述制得的钠盐缓慢滴加入反应液中(约20min滴加完毕),室温下搅拌1h。加入饱和氯化铵溶液淬灭反应,减压回收溶剂。用硅胶柱层析纯化,以PE:EtOAc(50:9)为洗脱剂,得金黄色油状物。Yield:79%;LCMS:m/z=361[M+1]+
步骤2. 4-甲氨基-2-氯-5-溴嘧啶(中间体1-4)合成
Figure PCTCN2017110029-appb-000019
将5-溴-2,4-二氯嘧啶(5g,22mmol)溶于甲醇(42mL)中,冰浴冷却下滴加33%的甲胺乙醇溶液(6.75mL),室温下搅拌30min。减压回收溶剂,用硅胶柱层析纯化,以PE:EtOAc(5:1)为洗脱剂,得白色固体。Yield:88%;mp:139-141℃;1H NMR(500MHz,DMSO-d6):δ8.85(s,Ar-H,1H),7.75(br,NH,1H),2.85(d,J=3.9Hz,CH3,3H);ESI-MS:m/z=222[M+1]+
步骤3. 5-溴-N4-甲基-2,4-二氨基嘧啶(中间体1-5)合成
Figure PCTCN2017110029-appb-000020
将化合物1-4(275mg,1.23mmol)置于封管中,加入氨气饱和的乙醇溶液(20mL),100℃下搅拌24h。冷却至室温,减压回收溶剂得残余物。用硅胶柱层析纯化,以PE:EtOAc(2:1)为洗脱剂,得白色固体。Yield:78%;1H NMR(500MHz,CDCl3):δ7.86(s,Ar-H,1H),5.22(br,NH,1H),4.85(br,NH2,2H),2.99(d,J=6.0Hz,CH3,3H);ESI-MS:m/z=204[M+1]+
步骤4. 5-(1-甲基-1H-吡唑-4-基)-N4-甲基-2,4-二氨基嘧啶(中间体1-6)合成
Figure PCTCN2017110029-appb-000021
氮气保护下,向化合物1-5(290mg,1.43mmol),1-甲基-1H-吡唑-4-硼酸频哪醇酯(358mg,1.72mmol),Pd(dppf)Cl2(54mg,0.07mmol)的混合物中加入乙二醇二甲醚(14mL),1N Na2CO3水溶液(2.8mL),回流搅拌过夜。减压回收溶剂得残余物。用硅胶柱层析纯化,以CH2Cl2:EtOH(25:1)为洗脱剂,得白色固体。Yield:75%;mp:226-228℃;1H NMR(500MHz,DMSO-d6):δ7.88(s,Ar-H,1H),7.49(s,Ar-H,1H),7.35(s,Ar-H,1H),6.22(br,NH2,2H),5.96(q,J=4.5Hz,NH,1H),3.51(s,CH3,3H),2.86(d,J=4.5Hz,CH3,3H);ESI-MS:m/z=205[M+1]+
步骤5.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(1-甲基-5-(哌啶-4-氧基)吡唑-3-基)-2,4-二氨基嘧啶(化合物1)合成
Figure PCTCN2017110029-appb-000022
氮气保护下,向化合物5a(169mg,0.986mmol),2a(376mg,0.986mmol),三(二亚苄基丙酮)二钯(9mg,0.00986mmol),4,5-双二苯基膦-9,9-二甲基氧杂蒽(15mg,0.026mmol),碳酸铯(450mg,1.38mmol)的混合物中加入无水二氧六环(6mL),回流搅拌过夜。抽滤,减压回收溶剂得残余物。用硅胶柱层析纯化,以CH2Cl2:EtOH(30:1)为洗脱剂,得白色固体。用三氟乙酸脱Boc保护基得白色固体。Yield:65%;LCMS:m/z=385[M+1]+
制备实施例2.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(3-(哌啶-4-氧基)异恶唑-5-基)-2,4-二氨基嘧啶(化合物2)
Figure PCTCN2017110029-appb-000023
步骤1.N-叔丁氧羰基-4-((5-溴-异恶唑-3-基)氧基)哌啶(中间体1-8)合成
Figure PCTCN2017110029-appb-000024
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,从5-溴-3-硝基吡唑(化合物1-7)制备化合物1-8。Yield:63%;LCMS:m/z=348[M+1]+
步骤2.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(3-(哌啶-4-氧基)异恶唑-5-基)-2,4-二氨基嘧啶(化合物2)合成
Figure PCTCN2017110029-appb-000025
合成步骤参考实施案例1步骤5.用类似于化合物1的合成方法,以中间体1-8和1-6为原料,制备得到化合物2。Yield:65%;LCMS:m/z=371[M+1]+
制备实施例3.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(1-甲基-2-(哌啶-4-氧基)咪唑-4-基)-2,4-二氨基嘧啶(化合物3)
Figure PCTCN2017110029-appb-000026
步骤1.N-叔丁氧羰基-4-((4-溴-1-甲基-1H-咪唑-2-基)氧基)哌啶(中间体1-10)合成
Figure PCTCN2017110029-appb-000027
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,从4-溴-1-甲基-2-硝基咪唑(化合物1-9)制备化合物1-10。Yield:67%;LCMS:m/z=361[M+1]+
步骤2.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(1-甲基-2-(哌啶-3-氧基)咪唑-4-基)-2,4-二氨基嘧啶(化合物3)合成
Figure PCTCN2017110029-appb-000028
合成步骤参考实施案例1步骤5.用类似于化合物1的合成方法,以中间体1-10和1-6为原料,制备得到化合物3。Yield:65%;LCMS:m/z=384[M+1]+
制备实施例4.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)异噻唑-5-基)-2,4-二氨基嘧啶(化合物4)
Figure PCTCN2017110029-appb-000029
步骤1.N-叔丁氧羰基-4-((5-溴-异噻唑-3-基)氧基)哌啶(中间体1-12)合成
Figure PCTCN2017110029-appb-000030
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,从5-溴-3-硝基咪唑(化合物1-11)制备化合物1-12。Yield:66%;LCMS:m/z=364[M+1]+
步骤2.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)异噻唑-5-基)-2,4-二氨基嘧啶(化合物4)合成
Figure PCTCN2017110029-appb-000031
合成步骤参考实施案例1步骤5.用类似于化合物1的合成方法,以中间体1-12和1-6为原料,制备得到化合物4。Yield:65%;LCMS:m/z=387[M+1]+
制备实施例5.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)-4,5-2H-恶唑啉-5-基)-2,4-二氨基嘧啶(化合物5)
Figure PCTCN2017110029-appb-000032
步骤1.N-叔丁氧羰基-4-((5-溴--4,5-2H-恶唑啉-2-基)氧基)哌啶(中间体1-14)合成
Figure PCTCN2017110029-appb-000033
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,从5-溴-2-硝基-4,5-2H恶唑啉化合物1-13)制备化合物1-14。Yield:67%;LCMS:m/z=361[M+1]+
步骤2.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)-4,5-2H-恶唑啉-5-基)-2,4-二氨基嘧啶(化合物5)合成
Figure PCTCN2017110029-appb-000034
合成步骤参考实施案例1步骤5.用类似于化合物1的合成方法,以中间体1-14和1-6为原料,制备得到化合物5。Yield:65%;LCMS:m/z=373[M+1]+
制备实施例6.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)噻唑-5-基)-2,4-二氨基嘧啶(化合物6)
Figure PCTCN2017110029-appb-000035
步骤1.N-叔丁氧羰基-4-((5-溴-噻唑-2-基)氧基)哌啶(中间体1-16)合成
Figure PCTCN2017110029-appb-000036
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,从5-溴-2-硝基噻唑(化合物1-15)制备化合物1-16。Yield:63%;LCMS:m/z=364[M+1]+
步骤2.N4-甲基-5-(1-甲基-1H-咪唑-4-基)-N2-(1-甲基-2-(哌啶-4-氧基)吡唑-4-基)-2,4-二氨基嘧啶(化合物3)合成
Figure PCTCN2017110029-appb-000037
合成步骤参考实施案例1步骤5.用类似于化合物1的合成方法,以中间体1-16和1-6为原料,制备得到化合物6。Yield:65%;LCMS:m/z=387[M+1]+
制备实施例7. 5-苯基-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物7)
Figure PCTCN2017110029-appb-000038
步骤1. 2-氰基-5-溴-3-(N-叔丁氧羰基哌啶-3-氧基)吡啶(中间体2-2)合成
Figure PCTCN2017110029-appb-000039
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,以5-溴-3-硝基-2-氰基吡啶(化合物2-1)和N-叔丁氧羰基-3-羟基哌啶为原料制备化合物2-2。Yield:79%;1H NMR(500MHz,DMSO-d6):δ8.26(s,Ar-H,1H),7.53(s,Ar-H,1H),4.38(br,CH,1H),3.63(br,CH,1H),3.51(br,CH,1H),3.38(br,CH,2H),1.98-1.96(m,CH,1H),1.91-1.85(m,CH,2H),1.51(br,CH,1H),1.36(s,CH3×3,9H);ESI-MS:m/z=382[M+1]+
步骤2. 5-溴-2-氨基嘧啶(中间体2-4)合成
Figure PCTCN2017110029-appb-000040
将2-氨基嘧啶(2.5g,26.29mmol)溶于乙腈(25mL)中,冰浴冷却下加入N-溴代丁二酰亚胺(4.6g,27.9mmol),室温下避光搅拌过夜。减压回收溶剂,用水(100mL)洗涤,抽滤,真空干燥得白色固体。Yield:97%;mp:241-243℃。
步骤3. 2-氨基-5-苯基嘧啶(中间体2-5)合成
Figure PCTCN2017110029-appb-000041
合成步骤参考实施案例1步骤4.以中间体2-4和苯硼酸为原料制备化合物2-5。Yield:86%;mp:159-161℃;1H NMR(400MHz,DMSO-d6):δ8.57(s,Ar-H,2H),7.62(d,J= 7.6Hz,Ar-H,2H),7.45(t,J=7.2Hz,Ar-H,2H),7.34(t,J=7.2Hz,Ar-H,1H),6.77(s,NH,2H);ESI-MS:m/z=172[M+1]+
步骤4. 5-苯基-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物7)合成
Figure PCTCN2017110029-appb-000042
合成步骤参考实施案例1步骤5.以中间体2-5和2-2为原料制备化合物7。Yield:65%;mp:84-86℃;1H NMR(500MHz,DMSO-d6):δ10.55(s,NH,1H),8.99(s,Ar-H,2H),8.65(d,J=2.0Hz,Ar-H,1H),8.39(d,J=2.0Hz,Ar-H,1H),7.78(d,J=7.0Hz,Ar-H,2H),7.52(t,J=7.5Hz,Ar-H,2H),7.43(t,J=7.0Hz,Ar-H,1H),4.42-4.37(m,CH,1H),3.19(d,J=12.0Hz,2.0Hz,CH2,1H),2.81-2.77(m,CH2,1H),2.66-2.62(m,CH2,1H),2.56-2.53(m,CH2,1H),2.14-2.11(m,CH2,1H),1.76-1.71(m,CH2,1H),1.65-1.58(m,CH2,1H),1.54-1.46(m,CH2,1H);13C NMR(100MHz,DMSO-d6):δ160.22,158.43,157.73,153.05,142.82,137.60,133.83,129.37,116.42,113.77,111.72,106.92,104.53,86.99,57.06,45.54,38.63,28.17;ESI-MS:m/z=373[M+1]+
制备实施例8. 5-(3-氟苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物8)
Figure PCTCN2017110029-appb-000043
步骤1. 2-氨基-5-(3-氟苯基)嘧啶(中间体2-6)合成
Figure PCTCN2017110029-appb-000044
合成步骤参考实施案例1步骤4.以中间体2-4和3-氟苯硼酸为原料制备化合物2-6,得白色固体。Yield:83%;mp:168-170℃;1H NMR(400MHz,DMSO-d6):δ8.62(s,Ar-H,2H),7.53-7.43(m,Ar-H,3H),7.16-7.11(m,Ar-H,1H),6.86(s,NH2,2H);ESI-MS:m/z=190[M+1]+
步骤2. 5-(3-氟苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物8)合成
Figure PCTCN2017110029-appb-000045
合成步骤参考实施案例1步骤5.以中间体2-6和2-2为原料制备化合物8,得白色固体。Yield:72%;mp:107-109℃;1H NMR(500MHz,DMSO-d6):δ10.59(br,NH,1H),9.03(s,Ar-H,2H),8.65(d,J=1.5Hz,Ar-H,1H),8.37(s,Ar-H,1H),7.70(d,J=10.5Hz,Ar-H,1H),7.65(d,J=8.0Hz,Ar-H,1H),7.56(dd,J=14.0Hz,8.0Hz,Ar-H,1H),7.26(td,J=8.5Hz,2.5Hz,Ar-H,1H),4.42-4.37(m,CH,1H),3.19(dd,J=12.0Hz,2.0Hz,CH2,1H),2.82-2.78(m,CH2,1H),2.67-2.63(m,CH2,1H),2.57-2.52(m,CH2,1H),2.14-2.11(m,CH2,1H),1.77-1.71(m,CH2,1H),1.66-1.59(m,CH2,1H),1.54-1.47(m,CH2,1H);ESI-MS:m/z=391[M+1]+
制备实施例9. 5-(4-氟苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物9)
Figure PCTCN2017110029-appb-000046
步骤1. 2-氨基-5-(4-氟苯基)嘧啶(中间体2-7)合成
Figure PCTCN2017110029-appb-000047
合成步骤参考实施案例1步骤4.以中间体2-4和4-氟苯硼酸为原料制备化合物2-7,得白色固体。Yield:85%;mp:172-174℃;1H NMR(400MHz,DMSO-d6):δ8.58(s,Ar-H,2H),7.68-7.64(m,Ar-H,2H),7.29(t,J=8.8Hz,Ar-H,2H),6.78(s,NH2,2H);ESI-MS:m/z=190[M+1]+
步骤2. 5-(4-氟苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物9)合成
Figure PCTCN2017110029-appb-000048
合成步骤参考实施案例1步骤5.以中间体2-7和2-2为原料制备化合物9,得白色固体。Yield:78%;mp:182-184℃;1H NMR(500MHz,DMSO-d6):δ10.54(br,NH,1H),8.96(s,Ar-H,2H),8.65(d,J=2.0Hz,Ar-H,1H),8.36(s,Ar-H,1H),7.83(dd,J=8.5Hz,5.5Hz,Ar-H,2H),7.35(t,J=8.0Hz,Ar-H,2H),4.41-4.36(m,CH,1H),3.20(dd,J=12.0Hz,2.5Hz,CH2,1H),2.82-2.78(m,CH2,1H),2.67-2.63(m,CH2,1H),2.57-2.52(m,CH2,1H),2.14-2.11(m,CH2,1H),1.77-1.71(m,CH2,1H),1.65-1.58(m,CH2,1H),1.54-1.46(m,CH2,1H);13C NMR(100MHz,DMSO-d6):δ163.09,161.14,158.27,157.25,155.90,141.82,134.15,130.59,128.17,128.11,125.15,116.21,116.08,115.91,113.84,109.21,74.69,49.65,45.28,29.82,24.27;ESI-MS:m/z=391[M+1]+
制备实施例10. 5-(3-甲氧基苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物10)
Figure PCTCN2017110029-appb-000049
步骤1. 2-氨基-5-(3-甲氧基苯基)嘧啶(中间体2-8)合成
Figure PCTCN2017110029-appb-000050
合成步骤参考实施案例1步骤4.以中间体2-4和3-甲氧基苯硼酸为原料制备化合物2-8,得白色固体。Yield:87%;mp:133-135℃;1H NMR(400MHz,DMSO-d6):δ8.58(s,Ar-H,2H),7.36(t,J=8.0Hz,Ar-H,1H),7.18(d,J=7.6Hz,Ar-H,2H),6.90(dd,J=8.4Hz,1.6Hz,Ar-H,1H),6.78(s,NH2,2H),3.81(s,CH3,3H);ESI-MS:m/z=202[M+1]+
步骤2.5-(3-甲氧基苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物10)合成
Figure PCTCN2017110029-appb-000051
合成步骤参考实施案例1步骤5.以中间体2-8和2-2为原料制备化合物10,得白色固体。Yield:74%;mp:102-104℃;1H NMR(500MHz,DMSO-d6):δ10.54(br,NH,1H),8.98(s,Ar-H,2H),8.65(d,J=2.0Hz,Ar-H,1H),8.37(d,J=2.0Hz,Ar-H,1H),7.42(t,J=8.0Hz,Ar-H,1H),7.33-7.32(m,Ar-H,2H),6.99-6.97(m,Ar-H,1H),4.42-4.37(m,CH,1H),3.85(s,CH3,3H),3.20(dd,J=12.0Hz,2.0Hz,CH2,1H),2.82-2.78(m,CH2,1H),2.68-2.64(m,CH2,1H),2.57-2.53(m,CH2,1H),2.14-2.11(m,CH2,1H),1.77-1.71(m,CH2,1H),1.66-1.59(m,CH2,1H),1.55-1.47(m,CH2,1H);13C NMR(100MHz,DMSO-d6):δ159.92,158.41,157.25,156.03,141.83,135.43,134.18,130.23,125.86,118.19,116.23,113.84,113.65,111.37,109.21,74.66,55.22,49.63,45.29,29.81,24.24;ESI-MS:m/z=403[M+1]+
制备实施例11. 5-(4-甲氧基苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物11)
Figure PCTCN2017110029-appb-000052
步骤1. 2-氨基-5-(4-甲氧基苯基)嘧啶(中间体2-9)合成
Figure PCTCN2017110029-appb-000053
合成步骤参考实施案例1步骤4.以中间体2-4和4-甲氧基苯硼酸为原料制备化合物2-9,得白色固体。Yield:82%;mp:165-167℃;1H NMR(400MHz,DMSO-d6):δ8.51(s,Ar-H,2H),7.55(d,J=8.8Hz,Ar-H,2H),7.01(d,J=8.8Hz,Ar-H,2H),6.67(s,NH2,2H),3.78(s,CH3,3H);ESI-MS:m/z=202[M+1]+
步骤2. 5-(4-甲氧基苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物11)合成
Figure PCTCN2017110029-appb-000054
合成步骤参考实施案例1步骤5.以中间体2-9和2-2为原料制备化合物11,得白色固体。Yield:75%;mp:218-220℃;1H NMR(400MHz,DMSO-d6):δ10.47(s,NH,1H),8.91(s,Ar-H,2H),8.64(s,Ar-H,1H),8.36(s,Ar-H,1H),7.71(d,J=8.8Hz,Ar-H,2H),7.06(d,J=8.8Hz,Ar-H,2H),4.40-4.36(m,CH,1H),3.81(s,CH3,3H),3.20(d,J=12.0Hz,CH2,1H),2.81-2.78(m,CH2,1H),2.67-2.62(m,CH2,1H),2.56-2.51(m,CH2,1H),2.14-2.12(m,CH2,1H),1.76-1.72(m,CH2,1H),1.66-1.57(m,CH2,1H),1.54-1.46(m,CH2,1H);13C NMR(100MHz,DMSO-d6):δ159.25,157.86,157.26,155.34,141.92,134.08,127.20,126.29,125.85,116.24,114.61,113.65,109.00,74.69,55.20,49.69,45.31,29.84,24.31;ESI-MS:m/z=403[M+1]+
制备实施例12. 5-(吡啶-3-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合12)
Figure PCTCN2017110029-appb-000055
步骤1. 2-氨基-5-(吡啶-3-基)嘧啶(中间体2-10)合成
Figure PCTCN2017110029-appb-000056
合成步骤参考实施案例1步骤4.以中间体2-4和吡啶-3-硼酸为原料制备化合物2-10,得白色固体。Yield:79%;mp:183-185℃;1H NMR(400MHz,DMSO-d6):δ8.87(s,Ar-H,1H),8.64(s,Ar-H,2H),8.53(br,Ar-H,1H),8.05(d,J=7.6Hz,Ar-H,1H),7.46(d,J=4.0Hz,Ar-H,1H),6.89(s,NH2,2H);ESI-MS:m/z=173[M+1]+
步骤2. 5-(吡啶-3-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物12)合成
Figure PCTCN2017110029-appb-000057
合成步骤参考实施案例1步骤5.以中间体2-10和2-2为原料制备化合物12,得白色固体。Yield:75%;mp:221-223℃;1H NMR(500MHz,DMSO-d6):δ10.61(br,NH,1H),9.06(s,Ar-H,2H),9.00(d,J=2.5Hz,Ar-H,1H),8.67(d,J=1.5Hz,Ar-H,1H),8.62(dd,J=4.5Hz,1.5Hz,Ar-H,1H),8.37(d,J=2.0Hz,Ar-H,1H),8.21(td,J=8.0Hz,2.0Hz,Ar-H,1H),7.54(dd,J=8.0Hz,4.0Hz,Ar-H,1H),4.43-4.39(m,CH,1H),3.20(dd,J=12.0Hz,2.0Hz,CH2,1H),2.83-2.78(m,CH2,1H),2.69-2.65(m,CH2,1H),2.59-2.54(m,CH2,1H),2.15-2.12(m,CH2,1H),1.78-1.72(m,CH2,1H),1.67-1.60(m,CH2,1H),1.55-1.47(m,CH2,1H);ESI-MS:m/z=374[M+1]+
制备实施例13. 5-(噻吩-2-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合13)
Figure PCTCN2017110029-appb-000058
步骤1. 2-氨基-5-(噻吩-2-基)嘧啶(中间体2-11)合成
Figure PCTCN2017110029-appb-000059
合成步骤参考实施案例1步骤4.以中间体2-4和噻吩-2-硼酸为原料制备化合物2-11,得白色固体。Yield:84%;mp:156-158℃;1H NMR(400MHz,DMSO-d6):δ8.53(s,Ar-H,2H),7.49(d,J=4.8Hz,Ar-H,1H),7.38(d,J=2.8Hz,Ar-H,1H),7.12(t,J=4.4Hz,Ar-H,1H),6.87(s,NH2,2H):ESI-MS:m/z=178[M+1]+
步骤2. 5-(噻吩-2-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物13)合成
Figure PCTCN2017110029-appb-000060
合成步骤参考实施案例1步骤5.以中间体2-11和2-2为原料制备化合物13,得白色固体。Yield:74%;mp:212-214℃;1H NMR(500MHz,DMSO-d6):δ10.58(br,NH,1H),8.93(s,Ar-H,2H),8.61(d,J=2.0Hz,Ar-H,1H),8.35(d,J=2.0Hz,Ar-H,1H),7.63-7.61(m,Ar-H,2H),7.20(dd,J=5.0Hz,3.5Hz,Ar-H,1H),4.42-4.37(m,CH,1H),3.19(dd,J=12.0Hz,2.0Hz,CH2,1H),2.82-2.78(m,CH2,1H),2.67-2.63(m,CH2,1H),2.57-2.52(m,CH2,1H),2.14-2.10(m, CH2,1H),1.77-1.71(m,CH2,1H),1.66-1.59(m,CH2,1H),1.54-1.46(m,CH2,1H);13C NMR(100MHz,DMSO-d6):δ158.00,157.25,154.63,141.67,136.46,134.18,128.55,126.15,124.27,121.13,116.20,113.91,109.24,74.64,49.63,45.30,29.81,24.26;ESI-MS:m/z=379[M+1]+
制备实施例14. 5-(呋喃-2-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合14)
Figure PCTCN2017110029-appb-000061
步骤1. 2-氨基-5-(呋喃-2-基)嘧啶(中间体2-12)合成
Figure PCTCN2017110029-appb-000062
合成步骤参考实施案例1步骤4.以中间体2-4和呋喃-2-硼酸为原料制备化合物2-12,得白色固体。Yield:83%;mp:156-158℃;1H NMR(400MHz,DMSO-d6):δ8.57(s,Ar-H,2H),7.69(s,Ar-H,1H),6.88(s,NH,2H),6.78(d,J=2.0Hz,Ar-H,1H),6.56(s,Ar-H,1H);ESI-MS:m/z=162[M+1]+
步骤2. 5-(呋喃-2-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物14)合成
Figure PCTCN2017110029-appb-000063
合成步骤参考实施案例1步骤5.以中间体2-12和2-2为原料制备化合物14,得白色固体。Yield:70%;mp:200-202℃;1H NMR(400MHz,DMSO-d6):δ10.58(br,NH,1H),8.95(s,Ar-H,2H),8.59(d,J=1.2Hz,Ar-H,1H),8.36(s,Ar-H,1H),7.81(s,Ar-H,1H),7.05(d,J=2.8Hz,Ar-H,1H),6.65(t,J=1.6Hz,Ar-H,1H),4.41-4.37(m,CH,1H),3.20(d,J=12Hz,CH2,1H),2.82-2.79(m,CH2,1H),2.67-2.62(m,CH2,1H),2.57-2.55(m,CH2,1H),2.14-2.12(m,CH2,1H),1.76-1.73(m,CH2,1H),1.67-1.58(m,CH2,1H),1.54-1.49(m,CH2,1H);13C NMR(100MHz,DMSO-d6):δ157.76,157.23,153.18,148.23,143.35,141.62,134.17,117.90,116.19,113.89,112.08,109.23,106.19,74.66,49.63,45.30,29.81,24.27;ESI-MS:m/z=363[M+1]+
制备实施例15.(R)-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合15)
Figure PCTCN2017110029-appb-000064
步骤1.(R)-2-氰基-5-溴-3-(N-叔丁氧羰基哌啶-3-氧基)吡啶(中间体2-13)合成
Figure PCTCN2017110029-appb-000065
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,以5-溴-3-硝基-2-氰基吡啶(化合物2-1)和(R)-N-叔丁氧羰基-3-羟基哌啶为原料制备化合物2-13,得金黄色油状物。Yield:76%;1H NMR(500MHz,DMSO-d6):δ8.26(s,Ar-H,1H),7.53(s,Ar-H,1H),4.38(br,CH,1H),3.63(br,CH,1H),3.51(br,CH,1H),3.38(br,CH,2H),1.98-1.96(m,CH,1H),1.91-1.85(m,CH,2H),1.51(br,CH,1H),1.36(s,CH3×3,9H);ESI-MS:m/z=382[M+1]+
步骤2. 2-氨基-5-(1-甲基-1H-吡唑-4-基)嘧啶(中间体2-14)合成
Figure PCTCN2017110029-appb-000066
合成步骤参考实施案例1步骤4.以中间体2-4和1-甲基吡唑-4-硼酸频哪醇酯为原料制备化合物2-14,得白色固体。Yield:85%;mp:174-176℃;1H NMR(400MHz,DMSO-d6):δ8.46(s,Ar-H,2H),8.03(s,Ar-H,1H),7.78(s,Ar-H,1H),6.57(s,NH2,2H),3.84(s,CH3,3H);ESI-MS:m/z=176[M+1]+
步骤3.(R)-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物15)合成
Figure PCTCN2017110029-appb-000067
合成步骤参考实施案例1步骤5.以中间体2-14和2-13为原料制备化合物15,得白色固体。Yield:73%;mp:230℃(分解);1H NMR(500MHz,DMSO-d6):δ10.42(br,NH,1H), 8.87(s,Ar-H,2H),8.59(d,J=1.5Hz,Ar-H,1H),8.35(d,J=2.0Hz,Ar-H,1H),8.23(s,Ar-H,1H),7.97(s,Ar-H,1H),4.41-4.36(m,CH,1H),3.89(s,CH3,3H),3.19(dd,J=12.0Hz,2.0Hz,CH2,1H),2.82-2.78(m,CH2,1H),2.68-2.64(m,CH2,1H),2.58-2.53(m,CH2,1H),2.14-2.11(m,CH2,1H),1.78-1.72(m,CH2,1H),1.65-1.58(m,CH2,1H),1.54-1.46(m,CH2,1H);13C NMR(125MHz,DMSO-d6):δ157.28,154.26,141.98,135.75,134.02,127.58,119.77,116.28,115.46,113.46,108.76,74.59,49.62,45.27,38.74,29.78,24.19;ESI-MS:m/z=377[M+1]+
制备实施例16.(R)-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合16)
Figure PCTCN2017110029-appb-000068
步骤1.(S)-2-氰基-5-溴-3-(N-叔丁氧羰基哌啶-3-氧基)吡啶(中间体2-15)合成
Figure PCTCN2017110029-appb-000069
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,以5-溴-3-硝基-2-氰基吡啶(化合物2-1)和(S)-N-叔丁氧羰基-3-羟基哌啶为原料制备化合物2-15,得金黄色油状物。Yield:78%;1H NMR(500MHz,DMSO-d6):δ8.26(s,Ar-H,1H),7.53(s,Ar-H,1H),4.38(br,CH,1H),3.63(br,CH,1H),3.51(br,CH,1H),3.38(br,CH,2H),1.98-1.96(m,CH,1H),1.91-1.85(m,CH,2H),1.51(br,CH,1H),1.36(s,CH3×3,9H);ESI-MS:m/z=382[M+1]+
步骤2.(S)-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物16)合成
Figure PCTCN2017110029-appb-000070
合成步骤参考实施案例1步骤5.以中间体2-14和2-15为原料制备化合物16,得白色固体。Yield:72%;mp:230℃(分解);1H NMR(500MHz,DMSO-d6):δ10.42(br,NH,1H), 8.87(s,Ar-H,2H),8.59(d,J=1.5Hz,Ar-H,1H),8.35(d,J=2.0Hz,Ar-H,1H),8.23(s,Ar-H,1H),7.97(s,Ar-H,1H),4.41-4.36(m,CH,1H),3.89(s,CH3,3H),3.19(dd,J=12.0Hz,2.0Hz,CH2,1H),2.82-2.78(m,CH2,1H),2.68-2.64(m,CH2,1H),2.58-2.53(m,CH2,1H),2.14-2.11(m,CH2,1H),1.78-1.72(m,CH2,1H),1.65-1.58(m,CH2,1H),1.54-1.46(m,CH2,1H);13C NMR(125MHz,DMSO-d6):δ157.28,154.26,141.98,135.75,134.02,127.58,119.77,116.28,115.46,113.46,108.76,74.59,49.62,45.27,38.74,29.78,24.19;ESI-MS:m/z=377[M+1]+
制备实施例17. 4-甲氧基-5-(3-氟苯基)-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶(化合17)
Figure PCTCN2017110029-appb-000071
步骤1. 2-氰基-5-溴-3-(N-叔丁氧羰基哌啶-4-甲基)氧基吡啶(中间体2-16)合成
Figure PCTCN2017110029-appb-000072
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,以5-溴-3-硝基-2-氰基吡啶(化合物2-1)和N-叔丁氧羰基哌啶-4-甲醇为原料制备化合物2-16,得金黄色油状物。Yield:80%;1H NMR(500MHz,CDCl3):δ8.34(s,Ar-H,1H),7.51(s,Ar-H,1H),4.20(d,J=11.5Hz,CH2,2H),3.95(br,CH2,2H),2.80(br,CH2,2H),2.14-2.05(m,CH,1H),1.89(br,CH2,2H),1.47(s,CH3×3,9H),1.33-1.26(m,CH2,2H);ESI-MS:m/z=206[M+1]+
步骤2. 4-甲氧基-2-氯-5-溴嘧啶(中间体2-17)合成
Figure PCTCN2017110029-appb-000073
将5-溴-2,4-二氯嘧啶(500mg,2.194mmol)溶于无水甲醇(5mL)中,氮气保护下,滴加甲醇钠(钠56mg,2.42mmol)的甲醇溶液(1.85mL),室温下搅拌过夜。加入饱和氯化铵溶液淬灭反应,减压回收溶剂,加入CH2Cl2(30mL),用水(30mL)洗涤,减压回收溶剂。用硅胶柱层析纯化,以PE:EtOAc(4:1)为洗脱剂,得白色固体。Yield:90%;1H NMR(400MHz,CDCl3):δ8.44(s,Ar-H,1H),4.11(s,CH3,3H);ESI-MS:m/z=223[M+1]+
步骤3. 4-甲氧基-5-溴-2-氨基嘧啶(中间体2-18)合成
Figure PCTCN2017110029-appb-000074
合成步骤参考实施案例1步骤3.用类似于化合物1-5的合成方法,中间体2-17为原料制备化合物2-18,得白色固体。Yield:75%;1H NMR(500MHz,CDCl3):δ8.13(s,Ar-H,1H),5.41(s,NH2,2H),3.91(s,CH3,3H);ESI-MS:m/z=205[M+1]+
步骤4.4-甲氧基-5-(3-氟苯基)-2-氨基嘧啶(中间体2-19)合成
Figure PCTCN2017110029-appb-000075
合成步骤参考实施案例1步骤4.以中间体2-18和3-氟苯硼酸为原料制备化合物2-19,得白色固体。Yield:88%;mp:127-128℃;1H NMR(500MHz,CDCl3):δ7.98(s,Ar-H,1H),7.46-7.42(m,Ar-H,1H),7.18(d,J=7.5Hz,Ar-H,1H),7.12-7.08(m,Ar-H,2H),5.19(s,NH2,2H),4.10(s,NH2,2H),3.96(s,CH3,3H);ESI-MS:m/z=220[M+1]+
步骤4. 4-甲氧基-5-(3-氟苯基)-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶(化合物17)合成
Figure PCTCN2017110029-appb-000076
合成步骤参考实施案例1步骤5.以中间体2-16和2-19为原料制备化合物17,得白色固体。Yield:79%;mp:139-141℃;1H NMR(500MHz,CDCl3):δ8.36(d,J=2.0Hz,Ar-H,1H),8.18(s,Ar-H,1H),8.08(d,J=2.0Hz,Ar-H,1H),7.58-7.54(m,Ar-H,1H),7.24-7.21(m,Ar-H,2H),7.15-7.12(m,Ar-H,1H),7.04(br,NH,1H),4.05(s,CH3,3H),3.97(d,J=6.5Hz,CH2,2H),3.20-3.18(m,CH2,2H),2.73-2.72(m,CH2,2H),2.13-2.06(m,CH,1H),1.93-1.91(m,CH2, 2H),1.40-1.32(m,CH2,2H);13C NMR(125MHz,DMSO-d6):δ163.85,163.46,161.52,158.92,158.03,157.93,141.22,136.25,135.99,135.92,131.07,131.01,125.40,116.22,116.05,115.84,114.98,114.82,114.64,114.14,111.54,72.92,55.50,44.11,34.25,27.19;ESI-MS:m/z=435[M+1]+
制备实施例18. 4-甲氧基-5-(3-氟苯基)-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶(化合18)
Figure PCTCN2017110029-appb-000077
步骤1. 4-甲氧基-5-(1-甲基-1H-吡唑-4-基)-2-氨基嘧啶(中间体2-20)合成
Figure PCTCN2017110029-appb-000078
合成步骤参考实施案例1步骤4.以中间体2-18和1-甲基吡唑-4-硼酸频那醇酯为原料制备化合物2-20,得白色固体。Yield:85%;1H NMR(500MHz,CDCl3):δ7.96(s,Ar-H,1H),7.58(s,Ar-H,1H),7.47(s,Ar-H,1H),5.18(s,NH2,2H),3.97(s,CH3,3H),3.94(s,CH3,3H);ESI-MS:m/z=206[M+1]+
步骤2. 4-甲氧基-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶(化合物18)合成
Figure PCTCN2017110029-appb-000079
合成步骤参考实施案例1步骤5.以中间体2-16和2-20为原料制备化合物18,得白色固体。Yield:82%;mp:213-215℃;1H NMR(500MHz,DMSO-d6):δ9.02(s,Ar-H,1H),8.69(d,J=2.0Hz,Ar-H,1H),8.25(s,Ar-H,1H),8.24(d,J=2.0Hz,Ar-H,1H),8.05(s,NH,1H),7.70(s,Ar-H,1H),5.33(s,NH,1H),4.05(d,J=6.5Hz,CH2,2H),3.92(s,CH3,3H),3.91(s,CH3,3H),3.31-3.28(m,CH2,2H),2.93-2.87(m,CH2,2H),2.19-2.11(m,CH,1H),1.93-1.91(m,CH2,2H),1.55-1.47(m,CH2,2H);ESI-MS:m/z=421[M+1]+
制备实施例19.化合物19~31的制备
Figure PCTCN2017110029-appb-000080
步骤1.中间体2-21~2-33合成
合成步骤参考实施案例1步骤4.以中间体1-5和相应的硼酸为原料制备化合物2-21~2-33,得白色固体。
步骤2.化合物19-31合成
合成步骤参考实施案例1步骤5.以中间体2-21~2-33和2-2为原料制备化合物19-31,得白色固体。
其中化合物30的合成方法如下:
Figure PCTCN2017110029-appb-000081
合成步骤参考实施案例1步骤5.以中间体2-31和2-2为原料制备化合物30的中间体,将Boc保护的中间体(100mg,0.203mmol)溶于DMF/THF(1:1)的混合溶液(2mL),滴加N-氯代丁二酰亚胺(27mg,0.203mmol),60℃下搅拌5小时,减压回收溶剂,加入乙酸乙酯,用水洗除DMF,合并有机层,用无水硫酸钠干燥,减压回收溶剂的残余物,用三氟乙酸脱保护基得黄色固体。
制备实施例20.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶(化合物32)
Figure PCTCN2017110029-appb-000082
步骤1.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶(化合物32)合成
Figure PCTCN2017110029-appb-000083
合成步骤参考实施案例1步骤5.以中间体1-6和2-2为原料制备化合物32,得白色固体。Yield:79%;mp:207-209℃;1H NMR(500MHz,DMSO-d6):δ9.92(s,NH,1H),8.51(s,Ar-H,2H),7.91(s,Ar-H,1H),7.90(s,Ar-H,1H),7.61(s,Ar-H,1H),6.74(q,J=4.5Hz,NH,1H),4.40-4.35(m,CH,1H),3.89(s,CH3,3H),3.15(dd,J=12.0Hz,2.0Hz,CH2,1H),2.94(d,J=5.0Hz,CH3,3H),2.79-2.74(m,CH2,1H),2.63-2.59(m,CH2,1H),2.54-2.48(m,CH2,1H),2.11-2.07(m,CH2,1H),1.74-1.68(m,CH2,1H),1.62-1.55(m,CH2,1H),1.45-1.37(m,CH2,1H);ESI-MS:m/z=406[M+1]+
制备实施例21.N4-甲基-5-(1-甲基-1H-吡唑-5-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶(化合物33)
Figure PCTCN2017110029-appb-000084
步骤1. 5-(1-甲基-1H-吡唑-5-基)-N4-甲基-2,4-二氨基嘧啶(中间体2-35)合成
Figure PCTCN2017110029-appb-000085
合成步骤参考实施案例1步骤4.以中间体1-5和1-甲基-1H-吡唑-5-硼酸频哪醇酯为原料制备化合物2-35,得白色固体。Yield:65%;1H NMR(500MHz,DMSO-d6):δ7.54(s,Ar-H,1H),7.47(d,J=1.5Hz,Ar-H,1H),6.24(br,NH2,2H),6.20(d,J=1.5Hz,Ar-H,1H),6.07(q,J=4.5Hz,NH,1H),3.61(s,CH3,3H),2.75(d,J=4.5Hz,CH3,3H);ESI-MS:m/z=205[M+1]+
步骤2.N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶(化合物33)合成
Figure PCTCN2017110029-appb-000086
合成步骤参考实施案例1步骤5.以中间体2-35和2-2为原料制备化合物33,得白色固体。Yield:74%;1H NMR(400MHz,DMSO-d6):δ10.07(br,NH,1H),8.55(s,Ar-H,1H),8.51(s,Ar-H,1H),7.87(s,Ar-H,1H),7.54(d,J=1.6Hz,Ar-H,1H),6.78(q,J=4.0Hz,NH,1H),6.32(d,J=1.6Hz,Ar-H,1H),4.41-4.36(m,CH,1H),3.67(s,CH3,3H),3.16(dd,J=9.6Hz,2.0Hz,CH2,1H),2.93(d,J=3.6Hz,CH3,3H),2.79-2.75(m,CH2,1H),2.64-2.59(m,CH2,1H),2.54-2.49(m,CH2,1H),2.11-2.07(m,CH2,1H),1.74-1.68(m,CH2,1H),1.63-1.56(m,CH2,1H),1.45-1.37(m,CH2,1H);13C NMR(100MHz,DMSO-d6):δ160.55,159.15,157.30,155.63,142.41,138.23,135.67,134.32,116.34,113.22,108.60,107.38,101.53,74.30,49.78,45.27,36.50,29.89,28.14,24.20;ESI-MS:m/z=406[M+1]+
制备实施例22.化合物34~43的制备
Figure PCTCN2017110029-appb-000087
步骤1.中间体2-36~2-42合成
合成步骤参考实施案例1步骤1.用类似于化合物1-2的合成方法,以5-溴-3-硝基-2-氰基吡啶(化合物2-1)和相应的醇为原料制备化合物2-36~2-42,得产物。
步骤2.化合物34-43合成
合成步骤参考实施案例1步骤5.分别以2-13、2-15、2-16、2-36~2-42和中间体2-34为原料制备化合物34-43,得白色固体。
制备实施例23.N4-甲基-5-(4-甲基噻唑-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶(化合物44)
Figure PCTCN2017110029-appb-000088
步骤1.锂(4-甲基噻唑-2-基)硼酸三异丙酯(中间体2-44)合成
Figure PCTCN2017110029-appb-000089
氮气保护下,将4-甲基噻唑(1g,10.09mmol),硼酸三异丙酯(2.35mL,10.09mmol)溶于无水甲苯和THF的混合溶液(32mL,v/v,4:1)中。冷却至-78℃,缓慢滴加正丁基锂(3.83mL,2.5mol/L,9.58mmol),约85min滴完,搅拌135min。缓慢升温至0℃(约1.5h),加入异丙醇(2.84mL),搅拌过夜。减压回收溶剂,加入无水丙酮(17mL),减压旋蒸至均相,冷却至室温。在氮气保护下抽滤,用55℃的乙腈洗涤,真空干燥得白色固体,无需纯化,直接进行下一步反应。
步骤2.N4-甲基-5-溴-N2-(2-氰基-3-(N-叔丁氧羰基哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧(中间体2-45)合成
Figure PCTCN2017110029-appb-000090
合成步骤参考实施案例1步骤5.以中间体1-5和2-2为原料制备中间体2-45,得白色固体。Yield:70%;1H NMR(400MHz,DMSO-d6):δ10.05(s,NH,1H),8.46(s,Ar-H,1H),8.41(s,Ar-H,1H),8.13(s,Ar-H,1H),7.32(q,J=4.5Hz,NH,1H),4.59(br,CH,1H),3.96-3.93(m,CH2,1H),3.77-3.70(m,CH2,1H),3.54-3.43(m,CH2,1H),3.07-2.96(m,CH2,1H),2.93(d,J=4.5Hz,CH3,3H),1.94(br,CH2,2H),1.85-1.80(m,CH2,1H),1.48-1.46(m,CH2,1H),1.38(s,CH3×3,9H);ESI-MS:m/z=504[M+1]+
步骤3.N4-甲基-5-(4-甲基噻唑-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶(化合物44)合成
Figure PCTCN2017110029-appb-000091
氮气保护下,向化合物2-45(85.3mg,0.211mmol),2-44(124mg,0.422mmol),Pd(dppf)Cl2(7.7mg,0.011mmol),CuCl(2.1mg,0.021mmol),ZnCl2(28.8mg,0.211mmol),Cs2CO3(137.5mg,0.422mmol)的混合物中加入无水DMF(10mL),加热至100℃搅拌过夜。抽滤,减压回收溶剂得残余物。用硅胶柱层析纯化,以CH2Cl2:EtOH(30:1)为洗脱剂,得白色固体。将得到的白色固体溶于二氯甲烷(3mL),冰浴下滴加三氟乙酸(3mL),搅拌30分钟,室温下搅拌4.5小时,用饱和碳酸氢钠溶液中和pH至9,加入乙酸乙酯(40mL),用饱和氯化钠溶液洗涤,无水硫酸钠干燥,减压回收溶剂得残余物。用硅胶柱层析纯化,以CH2Cl2/EtOH(NH3)(100:3)为洗脱剂,得白色固体。Yield:40%;1H NMR(400MHz,DMSO-d6):δ10.05(s,NH,1H),8.46(s,Ar-H,1H),8.41(s,Ar-H,1H),8.13(s,Ar-H,1H),7.32(q,J=4.5Hz,NH,1H),4.59(br,CH,1H),3.96-3.93(m,CH2,1H),3.77-3.70(m,CH2,1H),3.54-3.43(m,CH2,1H),3.07-2.96(m,CH2,1H),2.93(d,J=4.5Hz,CH3,3H),1.94(br,CH2,2H),1.85-1.80(m,CH2,1H),1.48-1.46(m,CH2,1H),1.38(s,CH3×3,9H);ESI-MS:m/z=504[M+1]+
制备实施例24. 5-三氟甲基-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物45)
Figure PCTCN2017110029-appb-000092
步骤1. 5-三氟甲基-二氨基嘧啶(中间体2-47)合成
Figure PCTCN2017110029-appb-000093
将化合物2-46(225mg,1.23mmol)置于封管中,加入氨水(10mL),N-甲基吡咯烷酮(10mL),120℃下搅拌24h。冷却至室温,减压回收溶剂得残余物。用硅胶柱层析纯化,以PE:EtOAc(2:1)为洗脱剂,得白色固体。LC-MS:m/z=164[M+1]+
步骤2. 5-三氟甲基-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶(化合物45)合成
Figure PCTCN2017110029-appb-000094
合成步骤参考实施案例1步骤5.以中间体2-47和2-2为原料制备化合物45,得白色固体。LC-MS:m/z=365[M+1]+
制备实施例25.化合物46-50的制备
Figure PCTCN2017110029-appb-000095
步骤1.中间体2-49/2-51合成
合成步骤分别参考实施案例17步骤2、实施案例1步骤2,得化合物2-49/2-51,质谱数据分别为LC-MS:m/z=194[M+1]+;LC-MS:m/z=193[M+1]+
步骤2.中间体2-50/2-52合成
合成步骤参考实施案例24步骤1.分别以2-49/2-51为原料制备化合物2-50/2-52,得白色固体。质谱数据分别为LC-MS:m/z=194[M+1]+;LC-MS:m/z=193[M+1]+
步骤3.化合物46-50合成
合成步骤参考实施案例1步骤5.分别以2-16、2-13、2-35、2-44和中间体2-50/2-52为原料制备化合物46-50,得白色固体。质谱数据分别为LC-MS:m/z=409[M+1]+;LC-MS:m/z=394[M+1]+;LC-MS:m/z=394[M+1]+;LC-MS:m/z=394[M+1]+;LC-MS:m/z=393[M+1]+
中间体2-21~2-33、2-36~2-42和化合物19-31、34-43的核磁及质谱数据见表1-1、1-2、1-3、1-4。
表1-1
Figure PCTCN2017110029-appb-000096
Figure PCTCN2017110029-appb-000097
表1-2
Figure PCTCN2017110029-appb-000098
Figure PCTCN2017110029-appb-000099
Figure PCTCN2017110029-appb-000100
Figure PCTCN2017110029-appb-000101
Figure PCTCN2017110029-appb-000102
Figure PCTCN2017110029-appb-000103
表1-3
Figure PCTCN2017110029-appb-000104
Figure PCTCN2017110029-appb-000105
表1-4
Figure PCTCN2017110029-appb-000106
Figure PCTCN2017110029-appb-000107
Figure PCTCN2017110029-appb-000108
本发明公开的化合物的Chk1抑制作用
以Staurosporine为阳性对照,采用ADP-Glo试剂盒评价Chk1酶抑制活性(IC50)。化合物作用于Chk1蛋白激酶,抑制其磷酸化底物Cdc25C,磷酸化过程需消耗ATP,反应结束后利用ADP-GloTM Reagent消耗掉剩余ATP,反应过程中所产生的ADP可被ADP-Glo Detection Reagent转化为ATP,ATP可作为Ultra-GloTM萤光素酶催化反应的底物,产生光信号。将待测化合物溶于DMSO中制成10mM的储备液,并按一定比例稀释至12个不同浓度以备测试。于384孔板中,每孔加入待测化合物1μL,2.5X Chk1激酶2μL,对照组加入1X缓冲液2μL,室温下孵育10min,加入2.5X底物2μL,在37℃下孵育1h,加入ADP-GloTM Reagent 5μL终止反应,在37℃下孵育1h。加入ADP-Glo Detection Reagent10μL,在37℃下孵育30min,并且每个样品设置三个平行孔,采用luminescence荧光检测酶标仪测定吸光度,利用GraphPad Prism 5软件处理数据,计算IC50值。
本发明公开的化合物对Chk1激酶的抑制活性
表2化合物对Chk1激酶的IC50(μM)
Figure PCTCN2017110029-appb-000109
Figure PCTCN2017110029-appb-000110
从表中数据可以看出,大部分化合物是Chk1蛋白激酶的高效抑制剂,有24个化合物的Chk1抑制活性与阳性化合物Staurosporine相当,5个化合物优于阳性对照Staurosporine。因此,本发明所涉及的可用作Chk1抑制剂的2-取代嘧啶类衍生物具有广阔的抗肿瘤应用前景。
本发明公开的化合物对各种肿瘤细胞的增殖抑制活性
细胞株:人多发性骨髓瘤细胞RPMI 8226、人套细胞淋巴瘤细胞Mino、Jeko-1、人淋巴瘤细胞Romas、人急性单核细胞白血病细胞MV-4-11、人乳腺癌细胞MCF-7、人肺癌细胞A549、人前列腺癌细胞LnCAP、人胃癌细胞BGC-823、人结肠癌细胞HCT116、Colo205、人卵巢癌细胞OVCAR-8实验方法:MTS法测定化合物对不同的肿瘤细胞株的体外增殖抑制活性(IC50)。
将处于对数生长期的细胞用胰酶消化,计数,以1×104细胞/孔的密度接种在96孔板中,每孔100μL,置于含5%CO2的37℃培养箱中过夜培养,每一化合物设六个浓度梯度,每一浓度设三组复孔,加入后,培养72小时,加入20μL MTS。37℃下孵育2小时后,用SpectraMAX 340酶标仪测490nm(L1)下的光吸收值,参考波长690nm(L2),将(L1-L2)值对抑制剂的不同浓度作图,经公式拟合得半数抑制浓度IC50
表3-1化合物对各肿瘤细胞株的增殖抑制作用
Figure PCTCN2017110029-appb-000111
Figure PCTCN2017110029-appb-000112
表3-2
Figure PCTCN2017110029-appb-000113
Figure PCTCN2017110029-appb-000114
aIC50:三次实验平均值;b未测。
本发明公开的化合物与其他药物联用活性
MV 4-11细胞以5000/孔接种至96孔板。联用时,药物按两药IC50之比确定药物的配比,各药浓度选择范围为IC20~IC80(或者1/8,1/4,1/2,1,2and 4of IC50)。72小时后,加入MTS试剂检测细胞活力,以未加药组为100%计算出抑制率Fa。采用Chou-Talalay method将抑制率Fa及相应药物浓度输入CompuSyn软件进行分析,得出单一浓度药物联用CI值及Fa-CI曲线。CI(combination index)的计算公式是CI=DA/ICX,A+DB/ICX,B(A,B代表两种不同药物,ICX,A和ICX,B是两种药物单独使用时生长抑制率达X时的药物浓度,DA和DB是两药联用时生长抑制率达X时两种药物的浓度)。结果见图1。图中:CHK1抑制剂(35);FLT3抑制剂Crenolanib(Cre)、Quizartinib(Qui);Akt抑制剂GSK2141795(GSK);CI=联用指数,根据Soriano等的判断方法,0.9≤CI≤1.1为叠加作用,0.8≤CI<0.9为低度协同作用,0.6≤CI<0.8为中度协同作用,0.4≤CI<0.6为高度协同作用,0.2≤CI<0.4为强协同作用。

Claims (10)

  1. 一种2-多取代芳环-嘧啶类衍生物,其特征在于,具有通式Ⅰ的结构:
    Figure PCTCN2017110029-appb-100001
    及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
    环A选自取代或无取代的包含1~3个选自O、N和S的五元或六元杂环芳基,所述取代的取代基选自
    Figure PCTCN2017110029-appb-100002
    和R5基团;
    B选自-NH、
    Figure PCTCN2017110029-appb-100003
    其中B1选自H、C1-4烷基、卤代的C1-4烷基、C1-4烷氧基、卤代的C1-4烷氧基;
    R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基、无取代或取代的五元或六元芳环或芳杂环,所述的芳杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;
    Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
    R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、卤代的C1-7烷基、C1-7羟烷基、C1-7胺烷基;
    R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
    L1选自O、S、NH或缺失;
    m=0~2;
    R4选自C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1-7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
    R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
  2. 根据权利要求1所述的一种2-多取代芳环-嘧啶类衍生物,其特征在于,所述的化合物具有通式Ⅱ的结构:
    Figure PCTCN2017110029-appb-100004
    Figure PCTCN2017110029-appb-100005
    及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
    W、X、Y和Z相同或不同,分别独立选自N、C和O;
    B选自-NH、
    Figure PCTCN2017110029-appb-100006
    其中B1选自H、C1-4烷基、卤代的C1-4烷基、C1-4烷氧基、卤代的C1-4烷氧基;
    R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基、无取代或取代的五元或六元芳环或芳杂环,所述的芳杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;
    Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
    R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、卤代的C1-7烷基、C1-7羟烷基、C1-7烷胺基、C1-7烷氧基;
    R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
    L1选自O、S、NH或者缺失;
    m=0~2;
    R4选自H、C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1-7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
    R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
  3. 根据权利要求1所述的一种2-多取代芳环-嘧啶类衍生物,其特征在于,所述的化合物具有通式Ⅲ的结构:
    Figure PCTCN2017110029-appb-100007
    及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
    W、X、Y和Z相同或不同,分别独立选自N或C;
    B选自-NH、
    Figure PCTCN2017110029-appb-100008
    其中B1选自H、C1-4烷基、卤代的C1-4烷基、C1-4烷氧基、卤代的C1-4烷氧基;
    R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基、无取代或取代的五元或六元芳环或芳杂环,所述的芳杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;
    Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
    R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、卤代的C1-7烷基、C1-7羟烷基、C1-7烷胺基、C1-7烷氧基;
    R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
    L1选自O、S、NH或者缺失;
    m=0~2;
    R4选自H、C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1-7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
    R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
  4. 根据权利要求1所述的一种2-多取代芳环-嘧啶类衍生物,其特征在于,所述的化合物具有通式Ⅳ的结构:
    Figure PCTCN2017110029-appb-100009
    及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
    W、X、Y和Z相同或不同,分别独立选自N、C和O;
    R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基、无取代或取代的五元或六元芳环或芳杂环,所述的芳杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;
    Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
    R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、卤代的C1-7烷基、C1-7羟烷基、C1-7烷胺基、C1-7烷氧基;
    R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
    L1选自O、S、NH或者缺失;
    m=0~2;
    R4选自H、C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1-7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
    R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
  5. 根据权利要求4所述的2-多取代芳环-嘧啶类衍生物,其特征在于,所述的化合物选自:
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(1-甲基-5-(哌啶-4-氧基)吡唑-3-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(3-(哌啶-4-氧基)异恶唑-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(1-甲基-2-(哌啶-4-氧基)咪唑-4-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)异噻唑-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)-4,5-2H-恶唑啉-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-(哌啶-4-氧基)噻唑-5-基)-2,4-二氨基嘧啶。
  6. 根据权利要求3所述的2-多取代芳环-嘧啶类衍生物,其特征在于,所述的化合物具有通式Ⅴ的结构:
    Figure PCTCN2017110029-appb-100010
    及其光学异构体或其药学上可接受的盐或溶剂合物,其中:
    W、X、Y和Z相同或不同,分别独立选自N或C;
    R1选自卤原子、C1-6烷基、卤代的C1-6烷基、C3-6环烷基、卤代的C3-6环烷基、C1-6烷氧基、卤代的C1-6烷氧基、C2-6烯基、C2-6羟基取代的烯基、C2-6炔基、C2-6羟基取代的炔基、无取代或取代的五元或六元芳环或芳杂环,所述的芳杂环包含1~3个选自O、N和S的杂原子,取代为单取代、双取代或三取代,所述的取代基选自Ra基团;
    Ra任选自H、卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、-C(=O)ORb、-C(=O)NHRb、-NHRb、-ORb、-NHCORb;Rb任选自H、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-7烷胺基;
    R2选自H、-NHRc、-N(Rc)2、-ORc、-SRc;Rc选自C1-7烷基、卤代的C1-7烷基、C1-7羟烷基、C1-7烷胺基、C1-7烷氧基;
    R3选自卤素、硝基、氰基、C1-3烷基、卤代的C1-3烷基、C1-3烷氧基、卤代的C1-3烷氧基、C1-3烷胺基、卤代的C1-3烷胺基;
    L1选自O、S、NH或者缺失;
    m=0~2;
    R4选自H、C1-7烷基、卤代的C1-7烷基、羟基取代的C1-7烷基、C1-7烷胺基、卤代的C1-7烷胺基、C1-7烷氧基、卤代的C1-7烷氧基、五元~八元含氮脂杂环;
    R5选自卤素、硝基、氰基、三氟甲基、C1-3烷基、C1-3烷氧基、酰胺基、取代烷基酰胺。
  7. 根据权利要求6所述的2-多取代芳环-嘧啶类衍生物,其特征在于,所述的化合物为:
    5-苯基-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    5-(3-氟苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    5-(4-氟苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    5-(3-甲氧基苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    5-(4-甲氧基苯基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    5-(吡啶-3-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    5-(吡啶-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    5-(噻吩-2-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    5-(呋喃-2-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    5-三氟甲基-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    (R)-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    (S)-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2-氨基嘧啶
    4-甲氧基-5-(3-氟苯基)-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶
    4-甲氧基-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶
    4-甲氧基-5-(3-氟苯基)-N-(2-氰基-3-(2-二甲氨基乙氧基)吡啶-5-基)-2-氨基嘧啶
    4-甲氧基-5-(1-甲基-1H-吡唑-4-基)-N-(2-氰基-3-(2-二甲氨基乙氧基)吡啶-5-基)-2-氨基嘧啶
    4-甲氧基-5-三氟甲基-N-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2-氨基嘧啶
    N4-甲基-5-苯基-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(3-氟苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(4-氟苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(2-氟苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(3-甲氧基苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(4-甲氧基苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(2,4-二甲氧基苯基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(吡啶-3-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(吡啶-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(噻吩-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(呋喃-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(5-氯-呋喃-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(5-甲氧羰基噻吩-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-5-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-三氟甲基-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-4-甲基)氧基吡啶-5-基)-2,4-二氨基嘧啶
    (R)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    (S)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    (R)-N4-甲基-5-三氟甲基-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    (S)-N4-甲基-5-三氟甲基-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    (R)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(吡咯-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    (S)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(吡咯-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(哌啶-4-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(2-二甲氨基乙氧基)吡啶-5-基)-2,4-二氨基嘧啶
    (R)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(1-二甲氨基丙基-2-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    (S)-N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(1-二甲氨基丙基-2-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(1-甲基-1H-吡唑-4-基)-N2-(2-氰基-3-(N-甲基哌啶-4-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-三氟甲基-N2-(2-氰基-3-(N-甲基哌啶-4-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    N4-甲基-5-(4-甲基噻唑-2-基)-N2-(2-氰基-3-(哌啶-3-氧基)吡啶-5-基)-2,4-二氨基嘧啶
    及其上述化合物的药学上可接受的盐或溶剂合物。
  8. 根据权利要求1~7任一所述的2-多取代芳环-嘧啶类衍生物的制备方法,其特征在于,通过以下步骤实现:
    方法一:
    (1)5-溴-2-取代-3-硝基吡啶(或5-溴-2-氰基-3-硝基吡啶)在NaH存在的条件下,与不同的脂肪醇经取代反应得到不同取代的吡啶片段;
    (2)以5-溴-2,4-二氯嘧啶为起始原料,依次经甲醚化或甲胺化和氨化得到5-溴-2,4-二取代嘧啶或以2-氨基嘧啶为原料经溴代后得到5-溴-2-氨基嘧啶,先经Suzuki偶联,再与上述吡啶片段发生钯催化的Buchwald-Hartwig交叉偶联反应,最后脱Boc保护基得到目标化合物;或采用2-氨基嘧啶中间体先与取代的5-溴吡啶经Buchwald-Hartwig交叉偶联,然后经Suzuki偶联反应,酸性条件下脱Boc保护基得到目标分子;
    方法二:
    (1)5-溴-2-氰基-3-硝基吡啶在碱性条件(NaH存在的条件)下,与不同的脂肪醇经取代反应得到不同取代的吡啶片段;
    (2)以2,4-二氯-5-三氟甲基嘧啶为起始原料,依次经甲醚化或甲胺化和氨化得到2,4-二取代-5-三氟甲基嘧啶或以2-氯-5-三氟甲基嘧啶为原料经氨化,再与上述吡啶片段发生钯催化的Buchwal-Hartwig交叉偶联反应,最后脱Boc保护基得到目标化合物。
  9. 权利要求1~7任一所述的2-多取代芳环-嘧啶类衍生物在制备抗肿瘤药物中的应用,其特征在于,所述的肿瘤为乳腺癌、肺癌、前列腺癌、胃癌、结肠癌、直肠癌、肾癌、胰腺癌、白血病、成神经细胞瘤、神经胶质瘤、头颈癌、卵巢癌、骨髓瘤、黑素瘤、非何杰 金淋巴瘤;所述的2-多取代芳环-嘧啶类衍生物包括其光学异构体或其药学上可接受的盐或溶剂合物。
  10. 权利要求1~7任一项所述的2-多取代芳环-嘧啶类衍生物在制备由Chk1介导所致疾病的药物中的应用,其特征在于,所述药物由2-多取代芳环-嘧啶类衍生物单独和/或与其他放疗药物联合制备,所述2-多取代芳环-嘧啶类衍生物包括其光学异构体或其药学上可接受的盐或溶剂合物。
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Cited By (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2021019514A1 (en) 2019-08-01 2021-02-04 Integral Biosciences Pvt. Ltd. Heterocyclic compounds as kinase inhibitor and uses thereof
WO2022162606A1 (en) * 2021-01-30 2022-08-04 Sperogenix Therapeutics Limited Heterocyclic compounds as kinase inhibitor and uses thereof

Families Citing this family (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP3620457A4 (en) * 2017-05-02 2021-01-06 Korea Research Institute of Chemical Technology PYRIMIDE-DERIVATIVE COMPOUND, OPTICAL ISOMER THEREOF, OR PHARMACEUTICAL SALT THEREOF AND COMPOSITION FOR THE PREVENTION OR TREATMENT OF TYRO-3 RELATED DISEASES THEREOF AS ACTIVE SUBSTANCE
KR102440296B1 (ko) * 2017-09-07 2022-09-06 한국화학연구원 피라졸기로 치환된 피리미딘 유도체 화합물, 이의 광학이성질체, 또는 이의 약학적으로 허용 가능한 염, 및 이를 유효성분으로 포함하는 암 예방 또는 치료용 조성물
CN111253370B (zh) * 2020-03-24 2021-08-03 浙江大学 N-多取代吡啶-2-氨基嘧啶类衍生物及用途
CN112920124B (zh) * 2021-01-29 2024-03-01 安徽医科大学 一种嘧啶-2,4-二胺类化合物及其制备方法与应用
CN117924277A (zh) * 2023-06-06 2024-04-26 中国药科大学 肟醚类化合物及其制备方法、药物组合物和应用

Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN102264725A (zh) * 2008-12-22 2011-11-30 伊莱利利公司 蛋白激酶抑制剂
WO2016141881A1 (zh) * 2015-03-11 2016-09-15 南京明德新药研发股份有限公司 作为抗癌药物的取代的2-氢-吡唑衍生物

Family Cites Families (10)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US8013154B2 (en) * 2007-10-09 2011-09-06 Niyaz Noormohamed M Insecticidal substituted azinyl derivatives
JP2012501982A (ja) * 2008-09-03 2012-01-26 バイエル・クロップサイエンス・アーゲー 殺真菌剤として使用するためのチエニルアミノピリミジン
HRP20172006T1 (hr) * 2010-11-10 2018-02-09 Genentech, Inc. Derivati pirazol-aminopiridina kao lrrk2-modulatori
EP2785381B1 (en) * 2011-11-30 2016-05-18 F.Hoffmann-La Roche Ag Fluorine-18 and carbon-11 labeled radioligands for positron emission tomography (pet) imaging for lrrk2
PT2840080T (pt) * 2012-04-17 2018-02-06 Fujifilm Corp Composto heterocíclico que contém azoto ou sal do mesmo
RU2637947C2 (ru) * 2012-05-03 2017-12-08 Дженентек, Инк. Производные пиразоламинопиримидина в качестве модуляторов обогащенной лейциновыми повторами киназы 2
EP2988744A4 (en) * 2013-04-26 2016-11-02 Merck Sharp & Dohme THIAZOLSUBSTITUTED AMINOHETEROARYLE AS MILZTYROSINKINASE INHIBITOR
EP3166637B1 (en) * 2014-07-10 2020-01-29 The J. David Gladstone Institutes Compositions and methods for treating dengue virus infection
US10829484B2 (en) * 2015-07-28 2020-11-10 Plexxikon Inc. Compounds and methods for kinase modulation, and indications therefor
EP3365334B1 (en) * 2015-10-21 2024-07-17 Otsuka Pharmaceutical Co., Ltd. Benzolactam compounds as protein kinase inhibitors

Patent Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN102264725A (zh) * 2008-12-22 2011-11-30 伊莱利利公司 蛋白激酶抑制剂
WO2016141881A1 (zh) * 2015-03-11 2016-09-15 南京明德新药研发股份有限公司 作为抗癌药物的取代的2-氢-吡唑衍生物

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
See also references of EP3530657A4 *

Cited By (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2021019514A1 (en) 2019-08-01 2021-02-04 Integral Biosciences Pvt. Ltd. Heterocyclic compounds as kinase inhibitor and uses thereof
WO2022162606A1 (en) * 2021-01-30 2022-08-04 Sperogenix Therapeutics Limited Heterocyclic compounds as kinase inhibitor and uses thereof

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