WO2024046504A1 - 一种ep300/cbp调节剂及其制备方法和用途 - Google Patents

一种ep300/cbp调节剂及其制备方法和用途 Download PDF

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WO2024046504A1
WO2024046504A1 PCT/CN2023/125452 CN2023125452W WO2024046504A1 WO 2024046504 A1 WO2024046504 A1 WO 2024046504A1 CN 2023125452 W CN2023125452 W CN 2023125452W WO 2024046504 A1 WO2024046504 A1 WO 2024046504A1
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alkyl
alkoxy
halogen
mmol
methyl
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李小林
齐龙武
许树森
别建波
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北京沐华生物科技有限责任公司
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    • A61K31/505Pyrimidines; Hydrogenated pyrimidines, e.g. trimethoprim
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    • A61K31/535Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with at least one nitrogen and one oxygen as the ring hetero atoms, e.g. 1,2-oxazines
    • A61K31/53751,4-Oxazines, e.g. morpholine
    • A61K31/53771,4-Oxazines, e.g. morpholine not condensed and containing further heterocyclic rings, e.g. timolol
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    • A61K31/55Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having seven-membered rings, e.g. azelastine, pentylenetetrazole
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    • C07D487/04Ortho-condensed systems

Definitions

  • the present invention requires the following:
  • the present disclosure belongs to the field of medicine, and specifically relates to an EP300/CBP regulator and its preparation method and use.
  • Histone acetyltransferase (HAT) and histone deacetylase (HDAC) can affect the acetylation of histones.
  • HAT and HDAC histone deacetylase
  • CBP cAMP response element-binding protein
  • EP300/CBP can also acetylate non-histone proteins, form transcriptional complexes with transcription factors, and play a role in transcriptional co-activation, such as nuclear receptors and other transcription factors to regulate gene expression.
  • EP300 and CBP are protein molecules with multiple functional domains and regulate the interactions between many proteins.
  • EP300 and CBP as transcriptional co-activators, participate in regulating the expression of target genes by binding to different transcription factors. Changes in protein expression affect many basic functions of cells, including proliferation, cell cycle, cell differentiation and DNA damage response, etc., and thus It affects the phenotype of cells and plays an important role in the occurrence and development of various tumors.
  • Current research shows that EP300/CBP is highly expressed and activated in a variety of different tumors.
  • EP300/CBP is closely related to a variety of tumor diseases and is a promising tumor treatment target. Therefore, EP300/CBP modulators are increasingly popular. researchers' attention.
  • the bromodomain of EP300/CBP is a domain of approximately 110 amino acids that can recognize acetylated lysine residues.
  • the bromodomain is the "readers" of lysine acetylation and is responsible for transduction of acetylated lysine.
  • the residues carry the signal while translating the signal into a normal or abnormal phenotype.
  • the bromodomain of EP300/CBP has a broad range of functions, ranging from histone acetyltransferase activity and chromatin remodeling to mediating transcriptional coactivation functions. There is currently a lot of evidence proving that bromodomains play an important role in the malignant progression of tumors. Modulators targeting the characteristic bromodomains of EP300/CBP have important development value and clinical significance in a variety of tumors.
  • the present disclosure provides a compound represented by Formula I and its racemate, stereoisomers, tautomers, isotope derivatives, nitrogen oxides, Solvates, polymorphs, metabolites, esters, prodrugs or pharmaceutically acceptable salts thereof:
  • n 0,1,2;
  • X 1 , X 2 , X 3 , X 4 are independently selected from C or N;
  • the following substituted groups: C 1-12 alkyl, C 1-12 alkoxy, -(C O)R;
  • the R is selected from C 1-12 alkyl, C 1-12 alkoxy, NH 2 -, C 1-12 alkyl-NH-, N, N-di-C 1-12 alkylamino, C 3- 12 cycloalkyl;
  • R 2 ' is selected from H, halogen, CN, NH 2 , COOH, OH, the following groups that are unsubstituted or optionally substituted by 1, 2 or more R 2 a: C 6-14 aryl, 5-14 membered heteroaryl, 3-14 membered heterocyclyl, C 3-12 cycloalkyl, C 1-12 alkyl;
  • CN NH 2
  • COOH hydroxy
  • OH hydroxy
  • R 5 a The following substituted groups: C 1-12 alkyl, C 1-12 alkoxy;
  • R 6 and R 7 together form the following groups that are unsubstituted or optionally substituted by 1, 2 or more Rsa: 5-14-membered heteroaryl, 3-14-membered heterocyclyl; the 5 -14-membered heteroaryl, 3-14-membered heterocyclyl contains at least one N atom;
  • X 1 , X 2 , X 3 , and X 4 are selected from C;
  • X 1 and X 2 are N, X 3 and X 4 are C;
  • Parts are selected from the following structures:
  • the structure has R 1 and R 2 substituents as defined above.
  • R1 is a substituent on the N atom of the ring, for example, such as (* represents the stated R 1 substitution position).
  • R 2 ' is selected from H, Cl, C 6-10 aryl which is unsubstituted or optionally substituted by 1, 2 or more R 2 a, 5-9 membered heteroaryl , 3-12 membered heterocyclic group, C 3-8 cycloalkyl, C 1-3 alkyl; the heterocyclic group contains 1-4 (1, 2, 3, 4) selected from N , O, S heteroatoms;
  • R 2 ' is selected from H, Cl, unsubstituted or optionally substituted with 1, 2 or more R 2 a as follows:
  • R 2 ' is selected from the following structures:
  • R 2 ' is selected from the following structures: H, Cl,
  • R 3 is selected from the group consisting of H, unsubstituted or optionally substituted by 1, 2 or more R 3 a: C 1-6 alkyl, C 1-6 alkoxy Base, C 3-8 cycloalkyl; each R 3 a is the same or different, independently selected from halogen, CN, NH 2 , COOH, OH;
  • R3 is selected from H, -CHF2 ,
  • R4 is selected from
  • each R 5 is the same or different and is independently selected from H, halogen, C 1-6 alkyl, C 1-6 alkoxy;
  • R 6 is selected from H, halogen, C 1-6 alkyl, C 1-6 alkoxy;
  • R is selected from H
  • R 7 is selected from H, halogen, C 1-6 alkyl, C 1-6 alkoxy;
  • R is selected from F
  • R 6 and R 7 together form the following groups that are unsubstituted or optionally substituted by 1, 2 or more Rsa: 5-6 membered heteroaryl, 5-6 membered heterocycle base.
  • R 6 and R 7 together form the following structure unsubstituted or optionally substituted with 1, 2 or more Rsa:
  • formula I is further selected from the structure shown in the following formula I-1:
  • X1 , X2 , X3 , X4 ,R1, R2 , R2 ',R3, R4 , R5 , R6 , R7 , R,n,m,p,q are as follows : (I) Compounds as defined;
  • R 1 ' has the definition stated in R 1 ;
  • formula I is further selected from the following structures represented by formula II, formula III, and formula IV:
  • formula I is further selected from the following structures shown in formula IIa and formula IIIa:
  • exemplary specific compounds of the compound represented by formula (I) are as follows:
  • the present disclosure also provides a pharmaceutical composition
  • a pharmaceutical composition comprising a compound represented by formula I (including formula II, III, IV, IIa, IIIa) and its racemates, stereoisomers, tautomers, isotopic derivatives, nitrogen oxides, solvates, polymorphs, metabolites, esters, prodrugs or pharmaceutically acceptable salts thereof.
  • the present disclosure also provides compounds represented by formula I (including formulas II, III, IV, IIa, IIIa) and their racemates, stereoisomers, tautomers, isotope derivatives, nitrogen Oxides, solvates, polymorphs, metabolites, esters, prodrugs or pharmaceutically acceptable salts thereof and pharmaceutical compositions containing the same for the preparation of prevention and/or treatment of CBP and/or EP300 mediated diseases or Use in medicines for medical conditions.
  • the present disclosure also provides a method for preventing and/or treating CBP and/or EP300-mediated diseases or conditions, comprising administering to a patient in need a therapeutically effective amount of Formula I (including Formulas II, III, IV, Compounds represented by IIa and IIIa) and their racemates, stereoisomers, tautomers, isotope derivatives, nitrogen oxides, solvates, polymorphs, metabolites, esters, prodrugs or their Pharmaceutically acceptable salts and pharmaceutical compositions containing the same.
  • Formula I including Formulas II, III, IV, Compounds represented by IIa and IIIa
  • the diseases or conditions mediated by CBP and/or EP300 of the present disclosure are selected from the group consisting of cancer, heart disease, metabolic disease, inflammatory disease, fibrosis disease and viral infection.
  • the cancers include, but are not limited to, prostate cancer, breast cancer, bladder cancer, lung cancer, melanoma, colorectal cancer, gastric cancer, ovarian cancer, cervical cancer, bladder cancer, laryngeal cancer, multiple myeloma, liver cancer, lymphoma and leukemia. wait.
  • the prostate cancer may be, for example, castration-resistant prostate cancer (CRPC).
  • Lung cancer may be, for example, non-small cell lung cancer or small cell lung cancer.
  • the lymphoma may be selected from non-Hodgkin's lymphoma, diffuse large B-cell lymphoma, and the like.
  • the compounds of the present disclosure may be used in combination with other drugs or other therapies.
  • the compounds described above in this disclosure are used in combination with radiation therapy.
  • the invention also provides for use of the compounds in combination with an immunomodulatory agent for the treatment of diseases or conditions associated with CBP and/or EP300 mediated diseases (eg, multiple myeloma).
  • an immunomodulatory agent for the treatment of diseases or conditions associated with CBP and/or EP300 mediated diseases (eg, multiple myeloma).
  • the immune modulators include tumor necrosis factor; interferons alpha, beta, and gamma; IL-2 and other cytokines; F42K and other cytokine analogs; or MIP-1, MIP-1 beta, MCP -1.
  • RANTES and other chemokines include tumor necrosis factor; interferons alpha, beta, and gamma; IL-2 and other cytokines; F42K and other cytokine analogs; or MIP-1, MIP-1 beta, MCP -1.
  • the compounds described above are used in combination with a second therapeutic agent, which may be selected from the group consisting of those conventionally used to treat cancer, heart disease, metabolic diseases, inflammatory diseases, fibrotic diseases, and viral infections.
  • a second therapeutic agent which may be selected from the group consisting of those conventionally used to treat cancer, heart disease, metabolic diseases, inflammatory diseases, fibrotic diseases, and viral infections.
  • Drug may include androgen receptor antagonists, such as enzalutamide, and inhibitors of CYP17A1 (17 ⁇ -hydroxylase/C17,20 lyase), e.g.
  • Cytotoxic chemotherapeutic agents such as docetaxel
  • Class of therapeutic agents used to treat lung cancer including cytotoxic chemotherapeutic agents, such as cisplatin, carboplatin, docetaxel
  • Class of therapeutic agents used to treat bladder cancer include cytotoxic chemotherapeutic agents such as gemcitabine, cisplatin or immunotherapies such as Bacillus Calmette-Guérin (BCG).
  • BCG Bacillus Calmette-Guérin
  • the class of second therapeutic agent may also be selected from immune checkpoint inhibitors such as pembrolizumab, nivolumab, atezolizumab, ipilimumab; PARP (poly ADP ribose polymerase) inhibitors such as olaparib ; and CDK4/6 (cyclin-dependent kinase 4 and 6) inhibitors.
  • the second therapeutic agent can be selected from the group consisting of combination drugs with KRAS inhibitors, etc., for the treatment of various tumors such as lung cancer, rectal cancer, pancreatic cancer, liver cancer, and hematoma.
  • the present disclosure provides a combination composition, including the compound represented by formula I (including formula II, III, IV, IIa, IIIa) and its racemate, stereoisomer, tautomer, Isotopic derivatives, nitrogen oxides, solvates, polymorphs, metabolites, esters, prodrugs or pharmaceutically acceptable salts thereof and the second therapeutic agent;
  • the present disclosure also provides a method for the combined prevention and/or treatment of diseases or conditions mediated by CBP and/or EP300, which comprises administering to a patient in need a therapeutically effective amount of Formula I (including Formula II, III, IV, IIa, IIIa ) and its racemates, stereoisomers, tautomers, isotope derivatives, nitrogen oxides, solvates, polymorphs, metabolites, esters, prodrugs or their pharmaceutically acceptable Accept salt as well as a second therapeutic agent.
  • Formula I including Formula II, III, IV, IIa, IIIa
  • Pharmaceutically acceptable salts of the compounds of the present disclosure can be inorganic salts or organic salts. If these compounds have a basic center, they can form acid addition salts; if these compounds have an acidic center, they can form base addition salts. ; If these compounds contain both acidic centers (eg carboxyl) and basic centers (eg amino), they can also form internal salts.
  • Compounds of the present disclosure may exist in specific geometric or stereoisomeric forms. For example, cis and trans isomers, (-)- and (+)-enantiomers, (R)- and (S)-enantiomers, diastereomers, (D)-isomers isomer, the (L)-isomer, racemic mixtures and other mixtures, as well as enantiomeric or diastereomerically enriched mixtures, all of which are within the scope of the present disclosure. Additional asymmetric carbon atoms may be present in substituents such as alkyl groups. All such isomers, as well as mixtures thereof, are included within the scope of this disclosure.
  • Tautomers refer to structural isomers of different energies that can interconvert via a low energy barrier.
  • proton tautomers also called proton transfer tautomers
  • proton migration tautomers include tautomers via proton migration, such as keto-enol isomerization, imine-enamine isomerization, and lactam-lactam isomerization. Isomerization of imides. All tautomeric forms of all compounds in this disclosure are within the scope of this disclosure. The name of a compound named in a single way does not exclude any tautomers.
  • the present disclosure also includes compounds of the present disclosure that have the same structure as described herein, but are isotopically labeled with one or more atoms replaced by atoms of an atomic weight or mass number different from those typically found in nature.
  • the actual isotopes that can be bound to the compounds of the present disclosure Examples include isotopes of hydrogen, carbon, nitrogen, oxygen, phosphorus, sulfur, fluorine, iodine, and chlorine, such as 2 H, 3 H, 11 C, 13 C, 14 C, 13 N, 15 N, 15 O, and 17 respectively O, 18 O, 31 P, 32 P, 35 S, 18 F, 123 I, 125 I and 36 Cl, etc. All variations in the isotopic composition of the compounds of the present disclosure, whether radioactive or not, are included within the scope of the present disclosure.
  • deuterium when a position is specifically designated as deuterium (D), that position is understood to have an abundance of deuterium that is at least 1000 times greater than the natural abundance of deuterium (which is 0.015%) (i.e., at least 10 % deuterium incorporation).
  • Examples of compounds having a natural abundance greater than deuterium may be at least 1000 times the abundance of deuterium, at least 2000 times the abundance of deuterium, at least 3000 times the abundance of deuterium, at least 4000 times the abundance of deuterium, at least 5000 times more abundant deuterium, at least 6000 times more abundant deuterium, or more abundant deuterium.
  • Each available hydrogen atom attached to a carbon atom can be independently replaced by a deuterium atom.
  • deuterated starting materials may be used in the preparation of deuterated forms of the compounds, or they may be synthesized using conventional techniques using deuterated reagents including, but not limited to, deuterated borane, trideuterated borane in tetrahydrofuran. , Deuterated lithium aluminum hydride, deuterated ethyl iodide and deuterated methyl iodide, etc.
  • modulator refers to a compound that alters (i.e., increases or decreases) the activity of a target biomolecule, such as an enzyme. Generally speaking, modulators will be small molecules.
  • modulate refers to the ability of a compound to increase or decrease the function and/or expression of a target, such as EP300 or CBP, where such function may include transcriptional regulatory activity and/or binding. Modulation can occur in vitro or in vivo. As used herein, modulation includes direct or indirect inhibition, antagonism, partial antagonism, degradation, activation, agonism or partial agonism of a function or characteristic associated with EP300 or CBP, and/or direct or indirect up-regulation or down-regulation of expression of EP300 or CBP . In another embodiment, the adjustment is direct.
  • An inhibitor or antagonist or degrader is a compound that (eg, binds to) partially or completely blocks stimulation, reduces, prevents, inhibits, delays activation, inactivates, inactivates, or downregulates signal transduction.
  • An activator or agonist is a compound that (eg, binds to) stimulates, increases, turns on, activates, promotes, enhances activation, activates, sensitizes, or upregulates signal transduction. Therefore, "EP300&CBP modulator” can further cover “EP300&CBP inhibitor", "EP300&CBP degrader", and "EP300&CBP agonist".
  • CBP and/or EP300-mediated disease or condition refers to a disease or condition in which the biological function of EP300, CBP, or both EP300 and CBP affects the development and/or course of the disease or condition, and/or wherein modulation of EP300, CBP, or both EP300 and CBP alters development, course, and/or symptoms.
  • EP300 or CBP mediated diseases or conditions include diseases or conditions in which EP300 inhibition, CBP inhibition, or both EP300 and CBP inhibition provide a therapeutic benefit, such as in which patients with the disease are treated with an EP300 or CBP inhibitor, including a compound described herein. or condition or to a subject at risk for the disease or condition.
  • EP300 or CBP Diseases or conditions mediated by EP300 or CBP are intended to include cancers with mutated loss of function of CBP or EP300, or cancers in which activation of EP300 or CBP is present.
  • EP300 or CBP mediated diseases or conditions are also intended to include cancers expressing androgen receptors.
  • the "therapeutically effective amount” of this disclosure refers to the amount of active compound or drug that researchers, veterinarians, physicians or other clinicians seek to cause a biological or medical response in tissues, systems, animals, individuals or humans, and it includes One or more of the following: (1) Prevention of disease: e.g., prevention of a disease, disorder, or condition in an individual who is susceptible to the disease, disorder, or condition but who has not yet experienced or developed the pathology or symptoms of the disease. (2) Inhibition of disease: e.g., inhibition of a disease, disorder, or condition (i.e., preventing further progression of pathology and/or symptoms) in an individual who is experiencing or developing pathology or symptoms of the disease, disorder, or condition.
  • Prevention of disease e.g., prevention of a disease, disorder, or condition in an individual who is susceptible to the disease, disorder, or condition but who has not yet experienced or developed the pathology or symptoms of the disease.
  • Inhibition of disease e.g., inhibition of a disease, disorder, or condition (i.e
  • a "therapeutically effective amount” refers to a non-toxic amount of the drug or agent that is sufficient to achieve the desired effect. The determination of the effective amount varies from person to person, depends on the age and general condition of the recipient, and also depends on the specific active substance. The appropriate effective amount in individual cases can be determined by those skilled in the art based on routine experiments.
  • the present disclosure provides a class of novel compounds having the structure represented by formula (I), which have good EP300/CBP regulatory activity (such as inhibitory activity) and medicinal prospects.
  • alkyl refers to a saturated aliphatic hydrocarbon group that is a straight aliphatic hydrocarbon group containing 1 to 12 carbon atoms (e.g., 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, and 12). Chain or branched chain groups, preferably alkyl groups containing 1 to 6 carbon atoms (C 1-6 alkyl).
  • alkyl groups include methyl, ethyl, n-propyl, isopropyl, n-butyl, isobutyl, tert-butyl, sec-butyl, n-pentyl, 1,1-dimethylpropyl 1,2-dimethylpropyl, 2,2-dimethylpropyl, 1-ethylpropyl, 2-methylbutyl, 3-methylbutyl, n-hexyl, 1-ethyl -2-Methylpropyl, 1,1,2-trimethylpropyl, 1,1-dimethylbutyl, 1,2-dimethylbutyl, 2,2-dimethylbutyl, 1,3-dimethylbutyl, 2-ethylbutyl, 2-methylpentyl, 3-methylpentyl, 4-methylpentyl, 2,3-dimethylbutyl, and Various branched chain isomers, etc. Alkyl groups may be substituted or unsubstituted.
  • alkoxy refers to -O-(alkyl), where alkyl is as defined herein.
  • alkoxy include: methoxy, ethoxy, propoxy and butoxy.
  • Alkoxy groups may be substituted or unsubstituted.
  • cycloalkyl refers to a saturated or partially unsaturated monocyclic or polycyclic cyclic hydrocarbon substituent.
  • the cycloalkyl ring preferably contains 3 to 12 or 3 to 8 (e.g. such as 3, 4, 5, 6, 7 and 8) carbon atoms, more preferably containing 3 to 6 carbon atoms.
  • Non-limiting examples of monocyclic cycloalkyl groups include cyclopropyl, cyclobutyl, cyclopentyl, cyclopentenyl, cyclohexyl, cyclohexenyl, cyclohexadienyl, cycloheptyl, cycloheptatriene base, cyclooctyl, etc.; polycyclic cycloalkyl includes spiro ring, fused ring and bridged ring cycloalkyl.
  • spirocycloalkyl refers to a polycyclic group in which each single ring in the system shares one carbon atom (called a spiro atom), which may contain one or more double bonds.
  • a spiro atom Preferably it is 6 to 12 yuan, more preferably 7 to 10 yuan (for example, 7, 8, 9 or 10 yuan).
  • the spirocycloalkyl group is divided into a single spirocycloalkyl group, a double spirocycloalkyl group or a polyspirocycloalkyl group, and is preferably a single spirocycloalkyl group and a double spirocycloalkyl group. More preferably, it is a 3-membered/5-membered, 3-membered/6-membered, 4-membered/4-membered, 4-membered/5-membered, 4-membered/6-membered, 5-membered/5-membered or 5-membered/6-membered monospirocyclic alkyl group.
  • spirocycloalkyl groups include:
  • fused cycloalkyl refers to an all-carbon polycyclic group in which each ring in the system shares an adjacent pair of carbon atoms with every other ring in the system, where one or more rings may contain one or more double bonds.
  • it is 6 to 12 yuan, more preferably 7 to 10 yuan (for example, 7, 8, 9 or 10 yuan).
  • bicyclic, tricyclic, tetracyclic or polycyclic fused ring alkyl groups preferably bicyclic or tricyclic, more preferably 3-membered/4-membered, 3-membered/5-membered, 3-membered/6-membered , 4 yuan/4 yuan, 4 yuan/5 yuan, 4 yuan/6 yuan, 5 yuan/4 yuan, 5 yuan/5 yuan, 5 yuan/6 yuan, 6 yuan/3 yuan, 6 yuan/4 yuan, 6 1/5-membered and 6-membered/6-membered bicycloalkyl groups.
  • fused cycloalkyl groups include:
  • bridged cycloalkyl refers to an all-carbon polycyclic group in which any two rings share two non-directly connected carbon atoms, which may contain one or more double bonds. Preferably it is 6 to 12 yuan, more preferably 7 to 10 yuan (for example, 7, 8, 9 or 10 yuan). According to the number of constituent rings, it can be divided into bicyclic, tricyclic, tetracyclic or polycyclic bridged cycloalkyl groups, preferably bicyclic, tricyclic or tetracyclic, more preferably bicyclic or tricyclic.
  • bridged cycloalkyl groups include:
  • the cycloalkyl ring includes a cycloalkyl group (including monocyclic, spiro, fused and bridged rings) as described herein fused to an aryl, heteroaryl or heterocycloalkyl ring, wherein with the parent
  • the rings linked together by the structure are cycloalkyl, non-limiting examples include etc; preferred
  • the cycloalkyl group may be substituted or unsubstituted.
  • heterocyclyl refers to a saturated or partially unsaturated monocyclic or polycyclic cyclic substituent containing 3 to 14 ring atoms, one or more of which are heteroatoms selected from nitrogen, oxygen and sulfur,
  • the sulfur may optionally be oxosubstituted (i.e., to form a sulfoxide or sulfone), but does not include the -O-O-, -O-S- or -S-S- ring moiety, and the remaining ring atoms are carbon.
  • 1 to 4 eg 1, 2, 3 and 4
  • 3 to 8 ring atoms eg 3, 4, 5, 6, 7 and 8
  • Non-limiting examples of monocyclic heterocyclyl groups include pyrrolidinyl, tetrahydropyranyl, 1,2,3,6-tetrahydropyridyl, piperidinyl, piperazinyl, morpholinyl, thiomorpholine base, homopiperazine base, etc.
  • Polycyclic heterocyclyl groups include spirocyclic, fused cyclic and bridged cyclic heterocyclyl groups.
  • spiroheterocyclyl refers to a polycyclic heterocyclic group in which each single ring in the system shares one atom (called a spiro atom), in which one or more
  • the ring atoms are heteroatoms selected from nitrogen, oxygen and sulfur, the sulfur may be optionally oxo-substituted (ie, forming sulfoxide or sulfone), and the remaining ring atoms are carbon. It may contain one or more double bonds.
  • it is 6 to 14 yuan, more preferably 7 to 10 yuan (for example, 7, 8, 9 or 10 yuan).
  • the spiroheterocyclyl group is divided into a single spiroheterocyclyl group, a double spiroheterocyclyl group or a polyspiroheterocyclyl group, and is preferably a single spiroheterocyclyl group and a double spiroheterocyclyl group.
  • spiroheterocyclyl include:
  • fused heterocyclyl refers to a polycyclic heterocyclyl group in which each ring in the system shares an adjacent pair of atoms with other rings in the system.
  • One or more rings may contain one or more double bonds, one of which Or more of the ring atoms are heteroatoms selected from nitrogen, oxygen and sulfur, the sulfur may be optionally oxo-substituted (ie, forming sulfoxide or sulfone), and the remaining ring atoms are carbon.
  • it is 6 to 14 yuan, more preferably 7 to 10 yuan (for example, 7, 8, 9 or 10 yuan).
  • bicyclic, tricyclic, tetracyclic or polycyclic fused heterocyclic groups preferably bicyclic or tricyclic, more preferably 3-membered/4-membered, 3-membered/5-membered, 3-membered/6-membered , 4 yuan/4 yuan, 4 yuan/5 yuan, 4 yuan/6 yuan, 5 yuan/4 yuan, 5 yuan/5 yuan, 5 yuan/6 yuan, 6 yuan/3 yuan, 6 yuan/4 yuan, 6 One-membered/5-membered and 6-membered/6-membered bicyclic fused heterocyclic groups.
  • fused heterocyclyl groups include:
  • bridged heterocyclyl refers to a polycyclic heterocyclic group in which any two rings share two atoms that are not directly connected, which may contain one or more double bonds, in which one or more ring atoms are selected from nitrogen, Heteroatoms of oxygen and sulfur, the sulfur may be optionally oxo-substituted (i.e., forming sulfoxide or sulfone), and the remaining ring atoms are carbon.
  • it is 6 to 14 yuan, more preferably 7 to 10 yuan (for example, 7, 8, 9 or 10 yuan).
  • bridged heterocyclyl groups preferably bicyclic, tricyclic or tetracyclic, more preferably bicyclic or tricyclic.
  • bridged heterocyclyl groups include:
  • the heterocyclyl ring includes a heterocyclyl (including monocyclic, spiroheterocyclic, fused heterocyclic and bridged heterocyclic) as described herein fused to an aryl, heteroaryl or cycloalkyl ring, wherein
  • the ring attached to the parent structure is a heterocyclyl group, non-limiting examples of which include:
  • the heterocyclyl group may be substituted or unsubstituted.
  • aryl refers to a 6 to 14-membered all-carbon monocyclic or fused polycyclic (fused polycyclic is a ring that shares adjacent pairs of carbon atoms) group having a conjugated ⁇ electron system, preferably 6 to 10 members , such as phenyl and naphthyl.
  • the aryl ring includes an aryl ring fused to a heteroaryl, heterocyclyl or cycloalkyl ring as described herein, where the ring attached to the parent structure is an aryl ring, which is not limited to Examples include: Aryl groups may be substituted or unsubstituted.
  • heteroaryl refers to a heteroaromatic system containing from 1 to 4 (eg, 1, 2, 3, and 4) heteroatoms, and from 5 to 14 ring atoms, wherein the heteroatoms are selected from oxygen, sulfur, and nitrogen.
  • the heteroaryl group is preferably 5 to 10 yuan (such as 5, 6, 7, 8, 9 or 10 yuan), more preferably 5 yuan or 6 yuan, such as furyl, thienyl, pyridyl, pyrrolyl, N-alkyl pyrrolyl, pyrimidinyl, pyrazinyl, pyridazinyl, imidazolyl, pyrazolyl, triazolyl, tetrazolyl, etc.
  • yuan such as 5, 6, 7, 8, 9 or 10 yuan
  • 6 yuan such as furyl, thienyl, pyridyl, pyrrolyl, N-alkyl pyrrolyl, pyrimidinyl, pyrazinyl, pyridazinyl, imidazolyl, pyrazolyl, triazolyl, tetrazolyl, etc.
  • the heteroaryl ring includes a heteroaryl fused to an aryl, heterocyclyl or cycloalkyl ring as described herein, where the ring attached to the parent structure is a heteroaryl ring, which is not limited to sexual examples include: Heteroaryl groups may be substituted or unsubstituted.
  • cycloalkyl, heterocyclyl, aryl, heteroaryl, etc. include residues derived from removing one hydrogen atom from the parent ring atom, or from the same or two different parent ring atoms. Residues derived from removing two hydrogen atoms from the ring atom, namely "bivalent cycloalkyl”, “bivalent heterocyclyl", “arylene”, “heteroarylene”.
  • halogen refers to F, Cl, Br or I.
  • heterocycloalkyl group optionally substituted by alkyl means that alkyl groups may but need not be present, and this description includes the case where the heterocycloalkyl group is substituted by an alkyl group and the heterocycloalkyl group is not substituted by an alkyl group. replacement situation.
  • the term "more” includes 3, 4, 5 and more.
  • 5,6-cyclo(isoindole) compounds can be synthesized by referring to this method.
  • 6-Chloro-8-(7-(difluoromethyl)-6-(1-methyl-1H-pyrazol-4-yl)-3,4-dihydroquinolin-1(2H)-yl) -3.4-Dihydroxyisoquinoline-2(1H)-tert-butylcarboxylate 200mg, 378.06 ⁇ mol
  • morpholine 164.68mg, 1.89mmol
  • XPhos 36.05mg, 75.61 ⁇ mol
  • Pd 2 (dba)3 34.62 mg, 37.81 ⁇ mol
  • t-BuONa 72.67 mg, 756.12 ⁇ mol
  • 6,6-cyclo(dihydroisoquinoline) compounds can be synthesized by referring to this method.
  • M001301 was used as raw material to further prepare M001320 and M001321.
  • N-((1s,4s)-4-(2-acetyl-7) as a white solid -(7-(Difluoromethyl)-6-(1-methyl-1H-pyrazol-4-yl)-3,4-dihydroquinolin-1(2H)-yl)isoindoline- 5-yl)cyclohexyl)acetamide (2.8 mg, 4% yield) and N-((1r,4r)-4(2-acetyl-7-(7-[difluoromethyl]-6-( 1-ethyl-1H-pyrazol-4-yl)-3,4-dihydroquinolin-1(2H)-yl)isoindolin-5-yl)cyclohexyl)acetamide (11.7 mg, 18 %Yield).
  • reaction mixture was filtered, concentrated in vacuo, and the residue was purified by Pre-HPLC (chromatographic column: -Xbridge-C18 150x19x19mm, 5um mobile phase: ACN-H 2 O (0.1% FA)) to obtain 1-(4-(7-( Difluoromethyl)-6-(1-methyl-1H-pyrazol-4-yl)-3,4-dihydroquinolin-1(2H)-yl)-6-(4-(methylsulfonate) Acyl)cyclohexyl)isoindolin-2-yl)ethan-1-one (30 mg, 33%).
  • Pre-HPLC chromatographic column: -Xbridge-C18 150x19x19mm, 5um mobile phase: ACN-H 2 O (0.1% FA)
  • the reaction mixture was concentrated under reduced pressure to obtain a residue .
  • reaction mixture was added to water (20 mL), the aqueous phase was extracted with ethyl acetate (50 ⁇ 2 mL), the combined organic phases were washed with NaCl aqueous solution (10 mL ⁇ 2), dried over Na 2 SO 4 , filtered, and concentrated under reduced pressure.
  • the ester (20.0 mg, yield 29%) was a white solid.
  • reaction was purified by preparative HPLC, eluting from 27% to 57% in 7 min with CH3CN in 0.1% FA/water to give 8-(7-(difluoromethyl)-6-(1-methyl- 1H-pyrazol-4-yl)-3,4-dihydroquinolin-1(2H)-yl)-N-methyl-6-(2,2',6'-trioxy-[1, 3'-bipyridyl]-4-yl)-3,4-dihydroisoquinoline-2(1H)-carboxamide (0.9 mg, yield 3%), as a white solid.
  • 6-Chloro-8-(7-(difluoromethyl)-6-(1-methyl-1H-pyrazol-4-yl)-3,4-dihydroquinolin-1(2H)-yl) -3,4-Dihydroisoquinoline-2(1H)-tert-butylcarboxylate (0.7g, 1.32mmol), potassium ethylene trifluoroborate (265.86mg, 1.98mmol), Pd2(dba)3 (121.17mg, 132.32 ⁇ mol), a solution of s-Phos (108.64 mg, 264.64 ⁇ mol) and t-BuONa (381.49 mg, 3.97 mmol) in dioxane (10 mL) was degassed and replaced with N 3 times, and then the mixture was incubated in N atmosphere Stir at 100°C for 16 hours.
  • Phenylboronic acid (19.38 mg, 158.92 ⁇ mol), 6-chloro-4-(7-(difluoromethyl)-6-(1-methyl-1H-pyrazol-4-yl)-3,4-di Hydroquinolin-1(2H)-yl)-N-methylisoindoline-2-carboxamide (50 mg, 105.95 ⁇ mol), XPhos Pd G3 (8.97 mg, 10.59 ⁇ mol) and K 3 PO 4 (67.47 mg , 317.84 ⁇ mol) was dissolved in THF (2 mL) and H 2 O (0.5 mL) and put into a microwave tube. Heat the microwave tube under microwave at 60°C for 1 hour. The mixture was extracted with EtOAc (10 mL) and washed with brine ( 5 mL % to 0%) to obtain yellow solid M001120 (3.66 mg, 7.13 ⁇ mol, 6.7% yield).
  • the reaction mixture was stirred at 60 °C under N for 2 h.
  • the mixture was quenched with water (50 mL) and extracted with ethyl acetate (80 mL ⁇ 2).
  • the combined organic phases were dried over sodium sulfate and filtered. The filtrate was concentrated under reduced pressure.
  • 22RV1 or vCap cells were cultured in RPMI-1640 medium (10% fetal calf serum was added to RPMI-1640, 100 units/chain per mL Mycin double-antibodies) and placed in a cell culture incubator at 37°C and 5% CO2 .
  • Cells in the logarithmic growth phase were seeded into a 96-well cell culture plate at 5x10 3 cells/100 ⁇ L/well and cultured overnight.
  • Different concentrations of active compound dissolved in DMSO were added, the final concentration was 0.5% DMSO, the positive control was 1% TweeN 2 0, and the negative control was 0.5% DMSO.
  • the X-axis is compound concentration ( ⁇ M) and the Y-axis is %Inhibition.
  • EP300 regulator biochemical activity test uses Ep300 Detection kit detection.
  • the assay principle is based on the enzymatic transfer of an acetyl group from acetyl-CoA to a specific lysine residue in a biotinylated peptide substrate.
  • Compounds are incubated with EP300, then with a combination of antibodies that specifically bind to the acetylated peptide and acceptor beads that bind the acetylated peptide, followed by incubation with streptavidin-labeled donor beads.
  • CBP preparation biochemical activity test uses CBP Detection kit detection.

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Abstract

本公开涉及一种式I所示的EP300/CBP调节剂及其制备方法和用途,所述式I结构如下。

Description

一种EP300/CBP调节剂及其制备方法和用途
本发明要求享有:
于2022年8月29日向中国国家知识产权局提交的,专利申请号为2022110436007,名称为“一种EP300/CBP抑制剂及其制备方法和用途”的在先申请的优先权;
于2022年9月13日向中国国家知识产权局提交的,专利申请号为2022111123014,名称为“一种EP300/CBP抑制剂及其制备方法和用途”的在先申请的优先权;
于2022年9月13日提交的美国临时申请US63/375,444,名称为“一种EP300/CBP抑制剂及其制备方法和用途”的在先申请的优先权;
于2023年8月18日向中国国家知识产权局提交的,专利申请号为2023110490720,名称为“一种EP300/CBP抑制剂及其制备方法和用途”的在先申请的优先权;
所述在先申请的全文通过引用的方式结合于本申请中。
技术领域
本公开属于医药领域,具体涉及一种EP300/CBP调节剂及其制备方法和用途。
背景技术
组蛋白乙酰转移酶(Histone acetyltransferase,HAT)和组蛋白去乙酰化酶(Histone deacetylase,HDAC)可以影响组蛋白的乙酰化,HAT和HDAC的募集和正常功能的发挥是基因表达和细胞周期的关键调控步骤,这些酶的功能性缺陷可能导致包括肿瘤在内的多种疾病。E1A结合蛋白EP300(EP300)及其紧密相关的类似物cAMP反应元件结合蛋白(CBP)结合蛋白是广泛表达的赖氨酸残基的乙酰化转移酶,能够将乙酰基从乙酰辅酶A转移到ε-N-乙酰赖氨酸来乙酰化组蛋白中保守的赖氨酸残基。
EP300/CBP也能够乙酰化非组蛋白,和转录因子形成转录复合物,发挥转录共激活的作用,像核受体和其他的转录因子来调控基因的表达。EP300和CBP是具有多个功能结构域的蛋白分子,调控很多蛋白之间的相互作用。EP300和CBP作为转录共激活因子通过和不同的转录因子结合,参与调控靶基因的表达,蛋白表达的变化影响了细胞的许多基本功能,包括增殖、细胞周期、细胞分化和DNA损伤反应等,进而影响了细胞的表型,在多种肿瘤的发生、发展中具有重要作用。目前研究表明,EP300/CBP在多种不同的肿瘤中高度表达和激活,EP300/CBP与多种肿瘤疾病密切相关,是极具应用前景的肿瘤治疗靶标,因此EP300/CBP调节剂越来越受到研究者的关注。
EP300/CBP的溴结构域是一个大约110氨基酸的结构域,可以识别乙酰化赖氨酸的残基,溴结构域是赖氨酸乙酰化的“readers”,负责转导由乙酰化赖氨酸残基携带的信号,同时将信号翻译成正常或异常的表型。EP300/CBP的溴结构域具有广泛的功能,范围从组蛋白乙酰化转移酶活性和染色质的重塑到介导转录共激活功能。目前已经有很多的证据证明,溴结构域在肿瘤的恶性进展中发挥重要作用,针对EP300/CBP特征性溴结构域的调节剂在多种肿瘤中具有重要的开发价值和临床意义。
但是,目前少数报道的EP300/CBP特征性溴结构域的调节剂多处于研发或临床早期,且存在活性较低、安全性不足等缺陷,远远不能满足临床需求。因此,研究出更多结构新颖、选择性更高、活性更好的EP300/CBP调节剂对于多种EP300/CBP相关肿瘤的治疗具有非常重要的意义。
发明内容
为解决现有技术存在的问题,第一方面,本公开提供了一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐:
其中:
n=0,1,2;
m=0,1,2,3;
p=0,1,2,3,4,5;
q=0,1,2;
X1,X2,X3,X4彼此独立地选自C或N;
每个R1相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R1a所取代的如下基团:C1-12烷基,C1-12烷氧基,-(C=O)R;
所述R选自C1-12烷基,C1-12烷氧基,NH2-,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C3-12环烷基;
每个R1a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1-12烷氧基;
每个R2相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1-12烷氧基;
R2’选自H,卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R2a所取代的如下基团:C6-14芳基,5-14元杂芳基,3-14元杂环基,C3-12环烷基,C1-12烷基;
每个R2a相同或不同,彼此独立地选自H、氧代(=O),卤素,COOH,OH,无取代或任选被1个、2个或更多个R2b所取代的如下基团:NH2,C1-12烷基,C1-12烷氧基,C1-12烷基硫基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基,C6-14芳基、5-14元杂芳基、3-14元杂环基、C3-12环烷基,C6-14芳基C(=O)-、5-14元杂芳基C(=O)-、3-14元杂环基C(=O)-、C3-12环烷基C(=O)-,C1-12烷基S(=O)2-、C1-12烷基S(=O)-、C1-12烷基S(=O)(=NH)-、C3-12环烷基S(=O)2-、C1-12烷基-C(=O)-NH-、C1-12烷基-S(=O)2-NH--;
每个R2b相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,;
R3选自H、卤素、CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R3a所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基-NHC(=O),N,N-二C1-12烷基氨基羰基,C6-14芳基,5-14元杂芳基,3-14元杂环基,C3-12环烷基;
每个R3a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R3b所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
每个R3b相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基;
R4选自H、卤素、CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R4a所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基-NHC(=O),N,N-二C1-12烷基氨基羰基,C6-14芳基,5-14元杂芳基,3-14元杂环基,C3-12环烷基;
每个R4a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R4b所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
每个R4b相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基;
每个R5相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R5a所取代的如下基团:C1-12烷基,C1-12烷氧基;
每个R5a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1-12烷氧基;
R6选自H、卤素、CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R6a所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基-NHC(=O),N,N-二C1-12烷基氨基羰基;
每个R6a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
R7选自H、卤素、CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R7a所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基-NHC(=O),N,N-二C1-12烷基氨基羰基;
每个R7a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
或R6与R7一起形成无取代或任选被1个、2个或更多个Rsa所取代的如下基团:5-14元杂芳基,3-14元杂环基;所述5-14元杂芳基,3-14元杂环基至少含有一个N原子;
每个Rsa相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个Rsb所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
每个Rsb相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基。
在一些实施方式中,X1,X2,X3,X4均选自C;
在一些实施方式中,X1,X2为N,X3,X4为C;
在一些实施方式中,
在一些实施方式中,式I中,部分选自如下结构:
所述结构上具有如前文所定义的R1、R2取代基。
在一些实施方式中,每个R1相同或不同,彼此独立地选自氧代(=O),C1-6烷基,C1-6烷氧基,-(C=O)R;所述R选自C1-6烷基,C1-6烷氧基,NH2-,C1-6烷基-NH-,C3-6环烷基;
在一些实施方式中,R1为环N原子上的取代基,示例性的,如(*代表所述R1取代位置)。
在一些实施方式中,R1为-(C=O)CH3
在一些实施方式中,每个R1相同或不同,彼此独立地选自=O,CH3,-C(=O)CH3,-C(=O)OCH3,-C(=O)OCH2CH3,CH3NHC(=O)-,CH3CH2NHC(=O)-,NH2C(=O)-,环丙基C(=O)-;
在一些实施方式中,R2’选自H、Cl、无取代或任选被1个、2个或更多个R2a所取代的C6-10芳基,5-9元杂芳基,3-12元杂环基,C3-8环烷基、C1-3烷基;所述杂环基含有1-4个(1个,2个,3个,4个)选自N,O,S的杂原子;
在一些实施方式中,R2’选自H、Cl、无取代或任选被1个、2个或更多个R2a所取代的如下结构:
在一些实施方式中,R2’选自如下结构:
在一些实施方式中,R2a选自H,卤素(如F),甲基,乙基,氧代(=O),甲氧基,OH,COOH,CH3C(=O)-,-CH2CHF2,-CH2CF3,-Cbz,-Boc,氨基,甲氨基,二甲氨基,甲硫基, -CH2CN,
在一些实施方式中,R2’选自如下结构:H,Cl,
在一些实施方式中,R3选自H、无取代或任选被1个、2个或更多个R3a所取代的如下基团:C1-6烷基,C1-6烷氧基,C3-8环烷基;每个R3a相同或不同,彼此独立地选自卤素,CN,NH2,COOH,OH;
在一些实施方式中,R3选自H、-CHF2
在一些实施方式中,R4选自无取代或任选被1个、2个或更多个R4a所取代的5-6元杂芳基(例如吡唑基);每个R4a相同或不同,彼此独立地选自无取代或任选被1个、2个或更多个R4b所取代的如下基团:C1-6烷基,C1-6烷氧基,N,N-二C1-6烷基氨基羰基;每个R4b相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-6烷基,C1-6烷氧基;
在一些实施方式中,R4选自
在一些实施方式中,每个R5相同或不同,彼此独立地选自H,卤素,C1-6烷基,C1-6烷氧基;
在一些实施方式中,R6选自H,卤素,C1-6烷基,C1-6烷氧基;
在一些实施方式中,R6选自H;
在一些实施方式中,R7选自H,卤素,C1-6烷基,C1-6烷氧基;
在一些实施方式中,R7选自F;
在一些实施方式中,R6与R7一起形成无取代或任选被1个、2个或更多个Rsa所取代的如下基团:5-6元杂芳基,5-6元杂环基。
在一些实施方式中,R6与R7一起形成无取代或任选被1个、2个或更多个Rsa所取代的如下结构:
在一些实施方式中,所述式I进一步选自如下式I-1所示结构:
其中,X1,X2,X3,X4,R1,R2,R2’,R3,R4,R5,R6,R7,R,n,m,p、q如式(I)中化合物所定义;
R1’具有R1所述的定义;
在一些实施方式中,R1’选自氧代(=O),C1-6烷基,C1-6烷氧基,-(C=O)R;所述R选自C1-6烷基,C1-6烷氧基,NH2-,C1-6烷基-NH-,C3-6环烷基;
在一些实施方式中,R1’选自H、CH3,-C(=O)CH3,-C(=O)OCH3,-C(=O)OCH2CH3,-C(=O)OCH(CH3)3,CH3NHC(=O)-,CH3CH2NHC(=O)-,NH2C(=O)-,环丙基-C(=O)-;
在一些实施方式中,R1’为-(C=O)CH3
在一些实施方式中,所述式I进一步选自如下式II、式III、式IV所示结构:

所述式II、式III、式IV中,X1,X2,X3,X4,R1,R2,R2’,R3,R4,R5,R6,R7,R,n,m,p,q如式(I)中化合物所定义。
在一些实施方式中,所述式I进一步选自如下式IIa、式IIIa所示结构:
所述式IIa、式IIIa,X1,X2,X3,X4,R1,R2,R2’,R3,R4,R5,R,n,m,p,q如式(I)中化合物所定义。
在一些实施方式中,式(I)所示化合物的示例性的具体化合物如下:














又一方面,本公开还提供了一种药物组合物,包括式I(包括式II、III、IV、IIa、IIIa)所示的化合物 及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐。
又一方面,本公开还提供了式I(包括式II、III、IV、IIa、IIIa)所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐以及包含其的药物组合物在制备预防和/或治疗CBP和/或EP300介导的疾病或病症的药物中的用途。
又一方面,本公开还提供了一种预防和/或治疗CBP和/或EP300介导的疾病或病症方法,其包括给予所需患者治疗有效量的式I(包括式II、III、IV、IIa、IIIa)所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐以及包含其的药物组合物。
本公开所述CBP和/或EP300介导的疾病或病症选自癌症,心脏病、代谢疾病、炎症疾病、纤维病变疾病及病毒感染。所述癌症包括但不限于前列腺癌,乳腺癌,膀胱癌,肺癌,黑色素瘤、结直肠癌、胃癌、卵巢癌、宫颈癌、膀胱癌、喉癌、多发性骨髓瘤、肝癌、淋巴瘤和白血病等。前列腺癌可以是例如对阉割有抗性的前列腺癌(CRPC)。肺癌可以是例如非小细胞肺癌或小细胞肺癌。所述淋巴瘤可选自非霍奇金淋巴瘤、漫大B细胞淋巴瘤等。
本公开的化合物可以与其他药物或其他疗法联合应用。
在一些实施方式中,本公开前文所述化合物与放射疗法联用。
在一些实施方式中,本发明还提供所述化合物与免疫调节剂联用用于治疗CBP和/或EP300介导的疾病或病症相关疾病(如多发性骨髓瘤)。
在一些实施方式中,所述免疫调节剂包括肿瘤坏死因子;干扰素α、β和γ;IL-2和其他细胞因子;F42K和其他细胞因子类似物;或MIP-1、MIP-1β、MCP-1、RANTES和其他趋化因子
在一些实施方式中,本公开前文所述化合物与第二治疗剂联用,所述第二治疗剂可选自常规用于治疗癌症,心脏病、代谢疾病、炎症疾病、纤维病变疾病及病毒感染的药物。在一些实施方案中,所述第二治疗剂的类别可以包括雄激素受体拮抗剂,例如恩杂鲁胺,和CYP17A1的抑制剂(17α-羟化酶/C17,20裂合酶),例如阿比特龙;细胞毒性化疗剂,例如多西他赛;用于治疗肺癌的治疗剂类别包括细胞毒素化疗剂,例如顺铂、卡铂、多西他赛;用于治疗膀胱癌的治疗剂类别包括细胞毒素化疗剂,例如吉西他滨、顺铂或免疫疗法,例如卡介苗(BCG)。所述第二治疗剂的类别还可以选自免疫检查点抑制剂,例如pembrolizumab,nivolumab,阿特珠单抗,伊匹木单抗;PARP(聚ADP核糖聚合酶)抑制剂比如奥拉帕尼;和CDK4/6(细胞周期蛋白-依赖性激酶4和6)抑制剂。在一些实施方案中,所述第二治疗剂可以选自与KRAS抑制剂等联合用药,用于肺癌,直肠癌,胰腺癌,肝癌,血液瘤等各种肿瘤的治疗。
因此,本公开提供了一种联用组合物,包含式I(包括式II、III、IV、IIa、IIIa)所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐和所述第二治疗剂;
本公开还提供了一种联合预防和/或治疗CBP和/或EP300介导的疾病或病症方法,其包括给予所需患者治疗有效量的式I(包括式II、III、IV、IIa、IIIa)所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐以及第二治疗剂。
本公开化合物的药学上可接受的盐可为无机盐或有机盐,如果这些化合物具有碱性中心,则其可以形成酸加成盐;如果这些化合物具有酸性中心,则其可以形成碱加成盐;如果这些化合物既包含酸性中心(例如羧基)又包含碱性中心(例如氨基),则其还可以形成内盐。
本公开化合物可以存在特定的几何或立体异构体形式。例如顺式和反式异构体、(-)-和(+)-对对映体、(R)-和(S)-对映体、非对映异构体、(D)-异构体、(L)-异构体,外消旋混合物和其他混合物,以及对映异构体或非对映体富集的混合物,所有这些混合物都属于本公开的范围之内。烷基等取代基中可存在另外的不对称碳原子。所有这些异构体以及它们的混合物,均包括在本公开的范围之内。
本公开的化合物和中间体还可以以不同的互变异构体形式存在,并且所有这样的形式包含于本公开的范围内。“互变异构体”是指可经由低能垒互变的不同能量的结构异构体。例如,质子互变异构体(也称为质子转移互变异构体)包括经由质子迁移的互变,如酮-烯醇异构化、亚胺-烯胺异构化和内酰胺-内酰亚胺异构化。本公开中的所有化合物的所有的互变异构形式均在本公开的范围内。用单一方式命名的化合物的名称不排除任何互变异构体。
本公开还包括一些与本文中记载的结构相同的,但一个或多个原子被原子量或质量数不同于自然中通常发现的原子量或质量数的原子置换的同位素标记的本公开化合物。可结合到本公开化合物的同位素的实 例包括氢、碳、氮、氧、磷、硫、氟、碘和氯的同位素,诸如分别为2H、3H、11C、13C、14C、13N、15N、15O、17O、18O、31P、32P、35S、18F、123I、125I和36Cl等。本公开的化合物的所有同位素组成的变换,无论放射性与否,都包括在本公开的范围之内。
除另有说明,当一个位置被特别地指定为氘(D)时,该位置应理解为具有大于氘的天然丰度(其为0.015%)至少1000倍的丰度的氘(即,至少10%的氘掺入)。示例中化合物的具有大于氘的天然丰度可以是至少1000倍的丰度的氘、至少2000倍的丰度的氘、至少3000倍的丰度的氘、至少4000倍的丰度的氘、至少5000倍的丰度的氘、至少6000倍的丰度的氘或更高丰度的氘。与碳原子连接的各个可用的氢原子可独立地被氘原子替换。本领域技术人员能够参考相关文献合成氘化形式的化合物。在制备氘代形式的化合物时可使用市售的氘代起始物质,或它们可使用常规技术采用氘代试剂合成,氘代试剂包括但不限于氘代硼烷、三氘代硼烷四氢呋喃溶液、氘代氢化锂铝、氘代碘乙烷和氘代碘甲烷等。
本公开所述术语“调节剂”指改变(即,增加或降低)靶生物分子例如酶的活性的化合物。一般来说,调节剂将是小分子。
术语“调节”是指化合物增加或降低靶标(诸如EP300或CBP)的功能和/或表达的能力,其中此类功能可包括转录调节活性和/或结合。调节可以在体外或体内进行。如本文所述,调节包括与EP300或CBP相关的功能或特征的直接或间接抑制、拮抗、部分拮抗、降解、活化、激动或部分激动,和/或表达EP300或CBP的直接或间接上调或下调。在另一实施方案中,调节是直接的。抑制剂或拮抗剂或降解剂是(例如结合以)部分或完全阻断刺激、降低、阻止、抑制、延迟活化、灭活、钝化或下调信号转导的化合物。活化剂或激动剂是(例如结合以)刺激、增加、打开、活化、促进、增强活化、活化、敏化或上调信号转导的化合物。因此,“EP300&CBP调节剂”可以进一步涵盖“EP300&CBP抑制剂”、“EP300&CBP降解剂”、“EP300&CBP激动剂”。
本公开所述术语“CBP和/或EP300介导的疾病或病症”是指以下疾病或病症,其中EP300、CBP或EP300和CBP两者的生物学功能影响疾病或病状的发展和/或病程,和/或其中EP300、CBP或EP300和CBP两者的调节改变发展、病程和/或症状。EP300或CBP介导的疾病或病状包括EP300抑制、CBP抑制或EP300和CBP抑制两者提供治疗益处的疾病或病状,例如其中用EP300或CBP抑制剂(包括本文所述的化合物)治疗为患有疾病或病状或处于疾病或病状风险中的受试者提供治疗益处。EP300或CBP介导的疾病或病状旨在包括具有CBP或EP300功能突变丧失的癌症,或存在EP300或CBP活化的癌症。EP300或CBP介导的疾病或病状也旨在包括表达雄激素受体的癌症。
本公开的“治疗有效量”是指研究人员、兽医、医师或其它临床医师等在组织、系统、动物、个体或人中寻找的引起生物学或医学反应的活性化合物或药物的量,它包括以下一项或多项:(1)预防疾病:例如在易感染疾病、紊乱或病症但尚未经历或出现疾病病理或症状的个体中预防疾病、紊乱或病症。(2)抑制疾病:例如在正经历或出现疾病、紊乱或病症的病理或症状的个体中抑制疾病、紊乱或病症(即阻止病理和/或症状的进一步发展)。(3)缓解疾病:例如在正经历或出现疾病、紊乱或病症的病理或症状的个体中缓解疾病、紊乱或病症(即逆转病理和/或症状)。针对药物或药理学活性剂而言,“治疗有效量”是指无毒的但能达到预期效果的药物或药剂的足够用量。有效量的确定因人而异,取决于受体的年龄和一般情况,也取决于具体的活性物质,个案中合适的有效量可以由本领域技术人员根据常规试验确定。
有益效果
本公开提供了一类具有式(I)所示结构的新颖化合物,具有良好的EP300/CBP调节活性(如抑制活性)和药用前景。
术语定义与说明
除非有相反陈述,否则在说明书和权利要求书中使用的术语具有下述含义。
术语“烷基”指饱和脂肪族烃基团,其为包含1至12个碳原子(例如1、2、3、4、5、6、7、8、9、10、11和12个)的直链或支链基团,优选含有1至6个碳原子的烷基(C1-6烷基)。烷基的非限制性实例包括甲基、乙基、正丙基、异丙基、正丁基、异丁基、叔丁基、仲丁基、正戊基、1,1-二甲基丙基、1,2-二甲基丙基、2,2-二甲基丙基、1-乙基丙基、2-甲基丁基、3-甲基丁基、正己基、1-乙基-2-甲基丙基、1,1,2-三甲基丙基、1,1-二甲基丁基、1,2-二甲基丁基、2,2-二甲基丁基、1,3-二甲基丁基、2-乙基丁基、2-甲基戊基、3-甲基戊基、4-甲基戊基、2,3-二甲基丁基,及其各种支链异构体等。烷基可以是取代的或未取代的。
术语“烷氧基”指-O-(烷基),其中烷基的定义如本文中所述。烷氧基的非限制性实例包括:甲氧基、乙氧基、丙氧基和丁氧基。烷氧基可以是取代的或未取代的。
术语“环烷基”指饱和或部分不饱和单环或多环环状烃取代基,环烷基环优选包含3至12个或3至8个(例 如3、4、5、6、7和8个)碳原子,更优选包含3至6个碳原子。单环环烷基的非限制性实例包括环丙基、环丁基、环戊基、环戊烯基、环己基、环己烯基、环己二烯基、环庚基、环庚三烯基、环辛基等;多环环烷基包括螺环、稠环和桥环的环烷基。
术语“螺环烷基”指系统中的每个单环之间共用一个碳原子(称螺原子)的多环基团,其可以含有一个或多个双键。优选为6至12元,更优选为7至10元(例如7、8、9或10元)。根据环与环之间共用螺原子的数目将螺环烷基分为单螺环烷基、双螺环烷基或多螺环烷基,优选为单螺环烷基和双螺环烷基。更优选为3元/5元、3元/6元、4元/4元、4元/5元、4元/6元、5元/5元或5元/6元单螺环烷基。螺环烷基的非限制性实例包括:
术语“稠环烷基”指系统中的每个环与体系中的其他环共享毗邻的一对碳原子的全碳多环基团,其中一个或多个环可以含有一个或多个双键。优选为6至12元,更优选为7至10元(例如7、8、9或10元)。根据组成环的数目可以分为双环、三环、四环或多环稠环烷基,优选为双环或三环,更优选为3元/4元、3元/5元、3元/6元、4元/4元、4元/5元、4元/6元、5元/4元、5元/5元、5元/6元、6元/3元、6元/4元、6元/5元和6元/6元的双环烷基。稠环烷基的非限制性实例包括:
术语“桥环烷基”指任意两个环共用两个不直接连接的碳原子的全碳多环基团,其可以含有一个或多个双键。优选为6至12元,更优选为7至10元(例如7、8、9或10元)。根据组成环的数目可以分为双环、三环、四环或多环桥环烷基,优选为双环、三环或四环,更优选为双环或三环。桥环烷基的非限制性实例包括:
所述环烷基环包括如本文中所述的环烷基(包括单环、螺环、稠环和桥环)稠合于芳基、杂芳基或杂环烷基环上,其中与母体结构连接在一起的环为环烷基,非限制性实例包括 等;优选所述环烷基可以是取代的或未取代的。
术语“杂环基”指饱和或部分不饱和单环或多环环状取代基,其包含3至14个环原子,其中一个或多个环原子为选自氮、氧和硫的杂原子,所述的硫可任选被氧代(即形成亚砜或砜),但不包括-O-O-、-O-S-或-S-S-的环部分,其余环原子为碳。优选包含3至12个(例如3、4、5、6、7、8、9、10、11和12个)环原子,其中1~4个(例如1、2、3和4个)是杂原子;更优选包含3至8个环原子(例如3、4、5、6、7和8个),其中1-3个(例如1、2和3个)是杂原子;更优选包含3至6个环原子,其中1-3个是杂原子;最优选包含5或6个环原子,其中1-3个是杂原子。单环杂环基的非限制性实例包括吡咯烷基、四氢吡喃基、1,2,3,6-四氢吡啶基、哌啶基、哌嗪基、吗啉基、硫代吗啉基、高哌嗪基等。多环杂环基包括螺环、稠环和桥环的杂环基。
术语“螺杂环基”指系统中的每个单环之间共用一个原子(称螺原子)的多环杂环基团,其中一个或多个 环原子为选自氮、氧和硫的杂原子,所述的硫可任选被氧代(即形成亚砜或砜),其余环原子为碳。其可以含有一个或多个双键。优选为6至14元,更优选为7至10元(例如7、8、9或10元)。根据环与环之间共用螺原子的数目将螺杂环基分为单螺杂环基、双螺杂环基或多螺杂环基,优选为单螺杂环基和双螺杂环基。更优选为3元/5元、3元/6元、4元/4元、4元/5元、4元/6元、5元/5元或5元/6元单螺杂环基。螺杂环基的非限制性实例包括:
术语“稠杂环基”指系统中的每个环与体系中的其他环共享毗邻的一对原子的多环杂环基团,一个或多个环可以含有一个或多个双键,其中一个或多个环原子为选自氮、氧和硫的杂原子,所述的硫可任选被氧代(即形成亚砜或砜),其余环原子为碳。优选为6至14元,更优选为7至10元(例如7、8、9或10元)。根据组成环的数目可以分为双环、三环、四环或多环稠杂环基,优选为双环或三环,更优选为3元/4元、3元/5元、3元/6元、4元/4元、4元/5元、4元/6元、5元/4元、5元/5元、5元/6元、6元/3元、6元/4元、6元/5元和6元/6元双环稠杂环基。稠杂环基的非限制性实例包括:
术语“桥杂环基”指任意两个环共用两个不直接连接的原子的多环杂环基团,其可以含有一个或多个双键,其中一个或多个环原子为选自氮、氧和硫的杂原子,所述的硫可任选被氧代(即形成亚砜或砜),其余环原子为碳。优选为6至14元,更优选为7至10元(例如7、8、9或10元)。根据组成环的数目可以分为双环、三环、四环或多环桥杂环基,优选为双环、三环或四环,更优选为双环或三环。桥杂环基的非限制性实例包括:
所述杂环基环包括如本文中所述的杂环基(包括单环、螺杂环、稠杂环和桥杂环)稠合于芳基、杂芳基或环烷基环上,其中与母体结构连接在一起的环为杂环基,其非限制性实例包括:
等。所述杂环基可以是取代的或未取代的。
术语“芳基”指具有共轭的π电子体系的6至14元全碳单环或稠合多环(稠合多环是共享毗邻碳原子对的环)基团,优选为6至10元,例如苯基和萘基。所述芳基环包括如本文中所述的芳基环稠合于杂芳基、杂环基或环烷基环上,其中与母体结构连接在一起的环为芳基环,其非限制性实例包括:
芳基可以是取代的或未取代的。
术语“杂芳基”指包含1至4个(例如1、2、3和4个)杂原子、5至14个环原子的杂芳族体系,其中杂原子选自氧、硫和氮。杂芳基优选为5至10元(例如5、6、7、8、9或10元),更优选为5元或6元,例如呋喃基、噻吩基、吡啶基、吡咯基、N-烷基吡咯基、嘧啶基、吡嗪基、哒嗪基、咪唑基、吡唑基、三唑基、四唑基等。所述杂芳基环包括如本文中所述的杂芳基稠合于芳基、杂环基或环烷基环上,其中与母体结构连接在一起的环为杂芳基环,其非限制性实例包括:
杂芳基可以是取代的或未取代的。
本领域技术人员可以理解,所述环烷基、杂环基、芳基和杂芳基等包括从母体环原子上除去一个氢原子所衍生的残基,或从母体的相同或两个不同的环原子上除去两个氢原子所衍生的残基,即“二价环烷基”、“二价杂环基”、“亚芳基”、“亚杂芳基”。
术语“卤素”指F、Cl、Br或I。
“任选”或“任选地”意味着随后所描述地事件或环境可以但不必发生,该说明包括该事件或环境发生或不发生地场合。例如,“任选被烷基取代的杂环烷基团”意味着烷基可以但不必须存在,该说明包括杂环烷基团被烷基取代的情形和杂环烷基团不被烷基取代的情形。
术语“更多个”包括3个,4个,5个以及更多。
具体实施方式
下文将结合具体实施例对本公开的技术方案做更进一步的详细说明。应当理解,下列实施例仅为示例性地说明和解释本公开,而不应被解释为对本公开保护范围的限制。凡基于本公开上述内容所实现的技术均涵盖在本公开旨在保护的范围内。
除非另有说明,以下实施例中使用的原料和试剂均为市售商品,或者可以通过已知方法制备。
实施例1
7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-1,2,3,4-四氢喹啉合成:
6-溴-7-(二氟甲基)-1,2,3,4-四氢喹啉的合成:
向7-(二氟甲基)-1,2,3,4-四氢喹啉(18g,98.2mmol,1eq)的DCM(180ml)溶液中于0℃下加入NBS(17.5g,98.2mmol,1eq)。将混合物在25℃下搅拌16小时。通过添加冰H2O(200mL)使反应混合物骤冷,并用DCM(150mL*2)萃取,用Na2SO4干燥,过滤并减压浓缩。残余物通过柱色谱法纯化(石油醚/乙酸乙酯=0至10%),得到黄色固体形式的化合物2(16g,61.1mmol,62.1%产率)。
MS(ESI):C10H11F2N;found 262.6(M+H)+.
1H NMR(400MHz,CDCl3)δ=7.18(s,1H),7.04(s,1H),6.63(s,1H),4.09-3.82(m,1H),3.28-3.18(m,2H),2.66(br t,J=6.3Hz,2H),1.88-1.79(m,2H)
7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-1,2,3,4-四氢喹啉合成:
6-溴-7-(二氟甲基)-1,2,3,4-四氢喹啉(11g,41.9mmol,1eq)、1-甲基-4-(4,4,5,5-四甲基-1,3,2-二氧苯并呋喃-2-基)吡唑(8.7g,41-9mmol,1eq)、环戊基(二苯基)膦的混合物;二氯钯;铁(3.0g,4.2mmol,0.1eq)、K2CO3(11.6g,83.9mmol,2eq)在二氧六环(80mL)和H2O(20mL)中的混合物在110℃下,在N2气下搅拌12小时。减压浓缩反应混合物。残余物通过柱色谱法纯化(石油醚/乙酸乙酯=0至40%),得到int-9(10g,37.9mmol,90.5%产率),为棕色固体。
MS(ESI):C14H15F2N3;found 263.9(M+H)+.
1H NMR(400MHz,DMSO-d6)δ=7.68(s,1H),7.43(s,1H),6.90(s,1H),6.73(s,1H),6.01(s,1H),3.84(s, 3H),3.24-3.14(m,2H),2.68(br t,J=6.0Hz,2H),1.79(quin,J=5.9Hz,2H)
实施例2
1-(6-氯-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚-2-基)乙烷-1-酮的合成:
5-氯-3-碘-2-甲基苯甲酸的合成:
向化合物1(50g,293.1mmol,1eq)的浓硫酸(350mL)溶液中,在0℃滴加NIS(76g,331mmol,98%纯度,1.13eq)的硫酸溶液(30ml)。将混合物在25℃下搅拌16小时。将反应物倒入冰水(500ml)中搅拌30分钟,然后过滤得到棕色固体形式的化合物2(68.5g,231mmol,78.8%产率)。
MS(ESI):C8H6ClIO2;found 294.8(M-H)+.
5-氯-3-碘-2-甲基苯甲酸甲酯的合成:
向化合物2(68.5g,231mmol,1eq)的MeOH(350mL)溶液中加入浓H2SO4(12mL)。将混合物在60℃下搅拌16小时。在减压下浓缩反应混合物。残余物用DCM(300mL)稀释,合并的有机相用NaHCO3水溶液(200mL)和盐水(200mL)洗涤。用无水Na2SO4干燥,过滤并真空浓缩,得到黄色油状化合物3(58.5g,188.4mmol,81.5%产率)。
1H NMR(400MHz,CHLOROFORM-d)δ=7.98(d,J=2.0Hz,1H),7.76(d,J=1.8Hz,1H),3.92(s,4H),2.64(s,3H).
2-(溴甲基)-5-氯-3-碘苯甲酸甲酯的合成:
向5-氯-3-碘-2-甲基苯甲酸甲酯(55g,177.12mmol,1eq)的CCl4(350ml)溶液中加入NBS(33g,185.41mmol,1.05eq)和BPO(4.5g,18.58mmol,1e-1eq)。将混合物在80℃下搅拌17小时。过滤反应混合物并减压浓缩。残余物通过柱色谱法纯化(石油醚/乙酸乙酯=100/0至10/1),得到无色油状化合物4(40g,103.1mmol,57%产率)。
1H NMR(400MHz,CHLOROFORM-d)δ=7.97(d,J=2.2Hz,1H),7.84(d,J=2.2Hz,1H),5.01(s,2H),3.89(s,3H).
2-(溴甲基)-5-氯-3-碘苯甲酸甲酯的合成:
化合物4(40g,102.5mmol,1eq)加入NH3/MeOH(150ml)溶液中。将混合物在60℃下搅拌2.5小时。在减压下浓缩反应混合物以除去MeOH。残余物用EA(150mL)洗涤3次,得到白色固体形式的化合物5(20.6g,70.4mmol,68.5%产率)。
MS(ESI):C8H6ClINO;found 295.8(M+H)+.
1H NMR(400MHz,DMSO-d6)δ=8.96(br s,1H),8.09(s,1H),7.71(s,1H),4.18(s,2H)
6-氯-4-碘异吲哚的合成:
向化合物5(17g,57.92mmol,1eq)的DCM(150mL)溶液中,在氮气下于0℃下逐滴添加DIBALH(1M,202.73mL,3.5eq)。将混合物在45℃下搅拌54小时。通过在0℃添加15%NaOH 100mL来猝灭反应混合物,然后过滤并用EtOAc洗涤。用盐水(200ml)洗涤滤液,用Na2SO4干燥,过滤并减压浓缩。残余物通过快速硅胶色谱法(硅胶快速柱,0~10%MeOH/DCM洗脱液)纯化,得到棕色固体形式的化合物6(5.5g,19.6mmol,33.9%)。
1H NMR(400MHz,DMSO-d6)δ=7.64(s,1H),7.37(s,1H),4.20(s,2H),3.93(s,2H).
1-(6-氯-4-碘代异吲哚-2-基)乙烷-1-酮的合成:
向化合物6(4.5g,16.1mmol,1eq)和TEA(4.1g,40.3mmol,5.6mL,2.5eq)的DCM(80mL)溶液中,在0℃的N2气下滴加醋酸酐(2.46g,24.1毫摩,2.26mL,1.5eq)。将混合物在25℃下搅拌16小时。残余物用H2O(100mL)稀释并用DCM(40mL*2)提取。合并的有机层用NaCl(40ml*2)洗涤, 用Na2SO4干燥,过滤并减压浓缩。残留物通过快速硅胶色谱法(0~100%乙酸乙酯/石油醚梯度洗脱液)纯化,得到棕色固体形式的化合物7(3.25g,8.2mmol,51%产率,70%纯度)。
MS(ESI):C10H9ClINO;found 322.3(M+H)+.
1-(6-氯-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚-2-基)乙烷-1-酮的合成:
将化合物7(1.15g,3.58mmol,1eq)、7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-1,2,3,4-四氢喹啉(941.6mg,3.58mmol,1eq)、NaOBu-t(859.2mg,8.94mmol,2.5eq)和Cphos-Pd G3(288.4mg,357.6μmol,0.1eq)放入二氧六环(10ml)中的微波管中。在微波下将密封管在110℃下加热50分钟。将反应混合物用H2O(20ml)稀释并用EtOAc(20ml*3)萃取。合并的有机层用盐水(50ml)洗涤,用Na2SO4干燥,过滤并减压浓缩。残留物通过快速硅胶色谱法纯化得到棕色固体形式的化合物8(700mg,1.53mmol,42.8%产率)。
MS(ESI):C24H23ClF2N4O;found 457.0(M+H)+.
5,6-并环(异吲哚)类的化合物可参照此方法合成。
实施例3
M001014(8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-6-吗啉-3,4-二氢异喹啉-2(1H)-甲酰胺)的合成:
8-溴-6-氯-1,2,3,4-四氢异喹啉的合成:
将8-溴-6-氯异喹啉(8.6g,35.46mmol)在AcOH(80mL)中的溶液冷却至0℃,然后分批加入NaBH4(2.68g,70.93mmol),将混合物在25℃下搅拌0.5小时。将混合物倒入H2O中以猝灭反应,然后用NH4Cl调节pH=8,用EtOAc(200ml)提取得到黄色固体形式的化合物2(8.48g,34.40mmol,97.0%产率,粗品),并通过HNMR确认。
1H NMR(400MHz,CD3Cl)δ7.42(s,1H),7.09(s,1H),4.00(s,2H),3.15-3.18(m,2H),2.85-2.88(m,2H).
8-溴-6-氯-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯的合成:
向8-溴-6-氯-1,2,3,4-四氢异喹啉(8.48g,34.40mmol)的DCM(100mL)溶液中加入TEA(6.96g,68.79mmol)和Boc2O(11.26g,51.60mmol)。将混合物在25℃下搅拌12小时。用盐水(50mL x 2)洗涤混合物,得到粗品,通过硅胶柱色谱法(石油醚/乙酸乙酯100%至70%)纯化,得到黄色油状化合物3(6.7g,19.33mmol,56.2%产率),并通过核磁共振进行确认。
1H NMR(400MHz,CD3Cl)δ7.42(s,1H),7.10(s,1H),4.49(s,2H),3.61-3.63(m,2H),2.80-2.82(m,2H),1.50(s,9H).
6-氯-8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-3.4-二羟基异喹啉-2(1H)-甲酸叔丁酯的合成:
8-溴-6-氯-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(29.3g,84.52mmol,29.3mg,84.52mmol),7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-1.2,3.3,4-四氢喹啉啉(13.35g,50.71mmol),tBuONa(24.37g,253.57mmol),CPHOS PD G3(6.82g,8.45mmol)和二氧六环(300mL)的混合物。脱气并用N2置换3次,-然后将混合物在100℃下在N2气下搅拌2小时。混合物用EtOAc(200ml)提取得到粗品,用硅胶柱色谱法纯化(石油醚/乙酸乙酯100%至70%),得到黄色油状化合物5(22.6g,42.72mmol,50.5%)。
LCMS(ESI+):m/z 529.3(M+H)+,Rt:2.38min.
8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-吗啉-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯的合成:
6-氯-8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-3.4-二羟基异喹啉-2(1H)-甲酸叔丁酯(200mg,378.06μmol)、吗啉(164.68mg,1.89mmol)、XPhos(36.05mg,75.61μmol)、Pd2(dba)3(34.62mg,37.81μmol)和t-BuONa(72.67mg,756.12μmol)溶于二氧六环(5ml),脱气并用N2置换3次,然后将混合物在100℃下在N2气下搅拌2小时。用EtOAc(10ml)提取混合物,并用盐水(5ml x 2)洗涤。残余物通过硅胶柱色谱法(石油醚/乙酸乙酯从100%至35%)纯化,得到黄色胶状化合物6(70mg,118.34μmol,31.3%),并通过LCMS检查。
LCMS(ESI+):m/z 580.4(M+H)+,Rt:1.77min.
4-(8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-1,2,3,4四氢异喹啉-6-基)吗啉的合成:
向8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-吗啉-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(60mg,103.51μmol)的DCM(5ml)溶液中添加TFA(27.01mmol,2ml)。将混合物在25℃下搅拌0.5小时。将混合物浓缩,得到黄色固体形式的化合物7(60mg,101.08μmol,97.7%产率,TFA盐粗)。
LCMS(ESI+):m/z 480.2(M+H)+,Rt:1.12min.
8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-6-吗啉-3,4-二氢异喹啉-2(1H)-甲酰胺的合成:
向4-(8-(7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-1,2,3,4-四氢异喹啉-6-基)吗啉(60mg,101.08μmol,TFA)的DCM(2mL)溶液中加入TEA(30.68mg,303.24μmol)和甲氨基甲酸盐(11.34mg,121.30μmol),并在55℃下搅拌16小时。混合物用DCM(10mL)萃取并用盐水(5mL)洗涤。有机层在Na2SO4上干燥,过滤并浓缩以获得粗品,通过prep-HPLC(FA)纯化以获得灰色固体形式的M001014(28.12mg,52.40μmol,51.8%产率)。
LCMS(ESI+):m/z 559.4(M+Na)+,Rt:1.75min,
1H NMR(400MHz,CD3Cl)δ7.53(s,1H),7.40(s,1H),7.05(s,1H),6.67(d,J=3.9Hz,2H),6.62-6.24(m,2H),4.46(d,J=15.9Hz,1H),4.36-4.27(m,1H),4.16-4.06(m,1H),3.95(s,3H),3.85(t,J=4.8Hz,4H),3.78-3.68(m,1H),3.63-3.43(m,3H),3.20-3.09(m,4H),3.01-2.83(m,4H),2.79(d,J=4.6Hz,3H),2.24-2.03(m,2H).
6,6-并环(二氢异喹啉)类的化合物可参照此方法合成。
实施例4
8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-6-(1-甲基-2-氧哌啶-4-基)-3,4-二氢异喹啉-2(1H)-甲酰胺的合成(M001124):
1-甲基-4-(4,4,5,5-四甲基-1,3,2-二氧杂硼烷-2-基)吡啶-2(1H)-酮的合成:
向4-溴-1-甲基吡啶-2-酮(500mg,2.66mmol)的1,4-二氧六环(10.0ml)溶液中加入Bis(pinacolato)diboron(1350mg,5.31mmol)、AcOK(783mg,7.97mmol)和Pd(dppf)Cl2(113mg,0.132mmol)。将反应溶液加热至100℃并在该温度下在,N2下搅拌2小时。将混合物冷却至25℃并减压浓缩。残余物通过硅胶色谱纯化,在15分钟内用MeOH/DCM(MeOH从0到10%)洗脱,得到黄色油状1-甲基-4-(4,4,5,5-四甲基-1,3,2-二氧苯并呋喃-2-基)吡啶-2(1H)-酮(500mg,产率62%)。
8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(1-甲基-2-氧代-1,2-二氢吡啶-4-基)-3,3-二氢异喹啉-2(1H)-甲酸叔丁酯的合成:
向6-氯-8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-3.4-二羟基异喹啉-2(1H)-甲酸叔丁酯(450mg,0.849mmol)的THF(10.0mL)和H2O(1.0mL)溶液中添加1-甲基-4-(4,4,5,5,4-四甲基-1,3,2-二氧杂环戊醇-2(2H)-1(400)。三磷酸钾(360mg,1.69mmol)和X-磷G3(72.0mg,0.084mmol)。将反应溶液加热至60℃并在该温度下,N2下搅拌3小时。将混合物冷却至25℃并减压浓缩。残余物通过硅胶色谱纯化,在10分钟内用MeOH/DCM洗脱(MeOH从0到5%),以黄色油的形式提供8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑基-吡唑基-4-基)-3,4-二氢喹啉-1(2H)-基)-3.4-二羟基喹啉-2(2H)-6-(2-甲基-2-氧基-1,2-二氢吡啶-4-甲酸叔丁酯(460mg,产率85%)。
4-(8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-1,2,3,4-四氢异喹啉-6-基)-1-甲基吡啶-2(1H)-酮的合成:
向8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(2-甲基-2-氧代-1,2-二氢吡啶-4-基)-3,4H-二氢异喹啉-2(1H)-甲酸叔丁酯(450mg,0.746mmol)的DCM(10.0ml)溶液中加入TFA(3.0ml)。将溶液在25℃下搅拌1小时。减压下浓缩混合物。残留物无需纯化直接用于下一步。
8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-6-(1-甲基-2-氧代-1,2-二氢吡啶-4-基)-3-四氢异喹啉-2(1H)-甲酰胺的合成:
向4-(8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-1,2,3,4-四氢异喹啉-6-基)-1-甲基吡啶-2(1H)-酮(450mg,0.897mmol)的DCM(10.0mL)溶液中添加Et3N(454mg,4.486mmol)和N-甲基氨甲酰氯(252mg,2.69mmol)。将反应溶液在25℃下搅拌1小时。减压下浓缩混合物。残余物通过Prep HPLC纯化(CH3CN在7分钟内从35%至65%),以黄色固体形式提供8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-6-(1-甲基-2-氧代-1,2-二氢吡啶-4-基)-3,4-二氢异喹啉-2(1H)-甲酰胺(320mg,产率64%)。
8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-6-(1-甲基-2-氧哌啶-4-基)-3,4-二氢异喹啉-2(1H)-甲酰胺的合成:
向8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-6-(1-甲基-2-氧代-1,2-二氢吡啶-4-基)-3,4-二氢异喹啉-2(1H)-甲酰胺(200mg,0.358mmol)的MeOH(10.0ml)溶液中添加PtO2(81.0mg,0.358mmol)。将溶液在25℃下在H2下搅拌12小时。过滤混合物以除去固体并浓缩。残余物通过Prep HPLC纯化(CH3CN在8分钟内从25%至50%),以黄色固体的形式提供8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-6-(1-甲基-2-氧哌啶-4-基)-3,4-二氢异喹啉-2(1H)-甲酰胺(90.0mg,41%产率)。
1H NMR(400MHz,DMSO-d6)δ7.72(s,1H),7.47(s,1H),7.06(m,3H),6.70(m,1H),6.48(d,J=4.0Hz,1H),6.17(s,1H),4.43(d,J=16.0Hz,1H),4.16–4.08(m,1H),3.86(s,3H),3.59–3.41(m,4H),3.28–3.22(m,1H),3.05(s,1H),2.81(m,7H),2.54(d,J=4.0Hz,3H),2.43–2.30(m,2H),2.18–1.81(m,5H).
实施例5
在20℃下向2,4-二氯-7,8-二氢吡啶并[4,3-d]嘧啶-6(5H)-甲酸叔丁酯(化合物1,432mg,1.64mmol,1.0eq),7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-1,2,3,4-四氢喹啉(化合物int-1,1.0g,3.29mmol,2.0eq)的混合物中加入DIEA(637mg,4.93mmol,858μL,3.0eq)。将混合物在150℃下搅拌4小时。LC-MS显示化合物1被完全消耗。所得混合物用乙酸乙酯(100mL)萃取,用盐水(10mL*3)洗涤,用Na2SO4(25g)干燥并浓缩。通过prep-HPLC(Phenomenex luna C18 100×40mm×3μm;流动相:[水-ACN];B%:40%-60%,12min)纯化残余物,获得2-氯-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-7,8-二氢吡啶并[4,3-d]嘧啶-6(5H)-甲酸叔丁酯(化合物2,100mg,粗品),为黄色油状物。经过H NMR确认。
在90℃下,向化合物2(100mg,188μmol,1.0eq)和2-(3,6-二氢-2H-吡喃-4-基)-4,4,5-5-四甲基-1,3,2-二氧杂硼烷(化合物3,79.1mg,376μmol,2.0eq)的二氧六环(4.0mL)、H2O(1.0mL)中的混合物中一次性加入Ruphos Pd G3(31.5mg,37.6μmol,0.2eq)和Cs2CO3(184mg,564μmol,3.0eq)。将混合物加热至90℃并搅拌16小时。LC-MS显示检测到32%的所需化合物。反应液减压下浓缩,残留物通过快速硅胶色谱法(25g硅胶快速柱,20~30%乙酸乙酯/石油醚梯度洗脱液@50mL/min)纯化。TLC(石油醚∶乙酸乙酯=3∶1,Rf=0.48)。得到黄色油状4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-2-(3,6-二氢-2H-吡喃-4-基)-7,8-二氢吡啶并[4,3-d]嘧啶-6(5H)-甲酸叔丁酯(化合物4,50.0mg,86.4μmol,45.9%产率)。
在20℃下,向化合物4(50.0mg,86.4μmol,1.0eq)的THF(5.0mL)混合物中一次性加入H2和Pd/C(20.0mg,10%纯度)(15psi)。将混合物加热至20℃并搅拌16小时。LC-MS显示检测到46.5%的所需化合物。反应液减压下浓缩,得到黄色油状4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-2-(四氢-2H-吡喃-4-基)-7,8-二氢吡啶并[4,3-d]嘧啶-6(5H)-甲酸叔丁酯(化合物5,50.0mg,粗品)。
在20℃、N2下,向化合物5(50.0mg,86.1μmol,1.0eq)的DCM(3.0mL)中一次性加入TFA(85.6mg,751μmol,55.6μL,8.72eq)。将混合物在20℃下搅拌16小时。LC-MS显示化合物5被完全消耗。将反应混合物在水(20.0mL)和乙酸乙酯(20.0mL)之间分配。有机层用Na2SO4干燥并浓缩以得到所需产物。得到黄色油状4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-2-(四氢-2H-吡喃-4-基)-5,6,7,8-四氢吡啶并[4,3-d]嘧啶(化合物6,50.0mg,粗品)。
在20℃,N2下,向N-甲基-1H-咪唑-1-甲酰胺(化合物7,26.0mg,208μmol,2.0eq)的DCM(5.0mL)中的混合物中一次性加入TEA(63.1mg,624μmol,86.8μL,6.0eq)和化合物6(50.0mg,104μmol,1.0eq)。将混合物在20℃下搅拌16小时。LC-MS显示化合物6被完全消耗。将反应混合物在水(20.0mL)和乙酸乙酯(20.0mL)之间分配。有机层用Na2SO4干燥并浓缩以得到所需产物。残留物通过制备HPLC柱纯化:PhenomenexGemini-NXC1875*30mm*3um;流动相:[水(0.05%NH3H2O+10mM NH4HCO3)-ACN];B%:22%-62%,11分钟。获得黄色油状4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-2-(四氢-2H-吡喃-4-基)-7,8-二氢吡啶并[4,3-d]嘧啶-6(5H)-甲酰胺(化合物M001245,34mg,62.4μmol,60.0%产率,98.7%纯度)。
M001245:
1H NMR(400MHz,DMSO-d6)δ7.74(s,1H),7.60(s,1H),7.30(s,1H),6.84–6.82(m,1H),6.82–6.53(m,1H),4.62(s,1H),4.07(s,3H),4.04(d,J=2.0Hz,1H),3.97(s,3H),3.92(t,J=6.0Hz,2H),3.68(t,J=6.4Hz,2H),3.58(dt,J=2.4,11.8Hz,2H),3.06–2.90(m,5H),2.68(s,3H),2.18–2.10(m,2H),2.07–1.96(m,2H),1.94–1.87(m,2H).
实施例6
向6-氯-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-2-甲酸叔丁酯(700mg,1.36mmol)的二氧六环(5.0mL)和H2O(0.5ml)的溶液中加入4-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)环己-3-烯-1-醇(609.2mg,2.72mmol)、K2CO3(563.6mg,4.0 8mmol)和XPhos Pd G3(114.9mg、0.14mmol)。然后将混合物在100℃下搅拌2小时。LCMS显示消耗了原料并检测到所需产物。残留物用快速柱色谱法纯化,用EtOAc在PE中洗脱0-50%,然后用快速柱层析法用MeOH在DCM中洗脱0-5%,得到黄色固体4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-羟基环己-1-烯-1-基)异吲哚啉-2-甲酸叔丁酯。
向4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-羟基环己-1-烯-1-基)异吲哚啉-2-甲酸叔丁酯(700mg,1.21mmol)的DCM(3.0mL)溶液中加入TFA(1.0mL)。将混合物减压浓缩,得到黄色固体4-(7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己-3-烯-1-醇(600mg,98%产率)。
向4-(7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己-3-烯-1-醇(600mg,1.3mmol)的DCM(4.0mL)溶液中加入25%的TEA(382.2mg,3.8mmol)和乙酰氯(197.7mg,2.5mmol)。加入水(50mL)使反应猝灭,用EtOAc(50mL×3)萃取。合并的有机层用盐水(50mL×3)洗涤,用无水Na2SO4干燥。残留物通过用EtOAc在PE中洗脱0-50%的快速柱色谱法纯化,然后通过用甲醇在DCM中洗脱0-5%的快速柱层析法纯化,得到黄色固体1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-羟基环己-1-烯-1-基)异吲哚啉-2-基)乙-1-酮(600mg,产率92%)。
在25℃,H2气氛(15PSI)下,向1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-羟基环己-1-烯-1-基)异吲哚啉-2-基)乙-1-酮(600mg,1.2mmol)的THF(4.0mL)溶液中,添加Pd/C(60%在油中)(123.1mg,1.2mol)。过滤后,在减压下浓缩滤液,得到黄色固体1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-羟基环己基)异吲哚啉-2-基)乙-1-酮(600mg,99%产率)。
在25℃下,向1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-羟基环己基)异吲哚啉-2-基)乙-1-酮(130mg,0.25mmol)的DCM(2.0mL)溶液中加入DessMartin(158.9mg,0.37mmol)。然后将混合物在25℃下搅拌2小时。加入饱和NaHCO3水溶液(20mL)淬灭混合物,并用DCM(3×20mL)萃取。将合并的有机层用Na2SO4干燥。过滤后,滤液通过快速柱色谱纯 化,用EtOAc在PE中从0%到50%洗脱,然后通过快速柱色谱纯化,用甲醇在二氯甲烷中从0%到5%洗脱,得到白色固体4-(2-乙酰基-7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己-1-酮(100mg,产率77%)。
在25℃下,向4-(2-乙酰基-7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己-1-酮(200mg,0.39mmol)的MeOH(3.0mL)溶液中加入碳酸铵(74.1mg,0.77mmol)。将混合物在25℃下搅拌1小时。然后向该混合物中加入NaCNBH3(48.5mg,0.77mmol)。将混合物在25℃下搅拌1小时。LCMS显示消耗了起始材料并检测到所需产物。粗产物通过制备HPLC纯化,用CH3CN在0.1%FA/水中洗脱,在8分钟内从38%至45%,得到白色固体1-(6-(4-氨基环己基)-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-2-基)乙-1-酮(30.4mg,15%产率)。
M001301:
1H NMR(400MHz,DMSO-d6)δ8.40(s,1H),7.74(s,1H),7.49(s,1H),7.16–7.10(m,2H),6.74(t,J=55.2Hz,1H),6.40(d,J=28.0Hz,1H),4.85(s,1H),4.64(s,1H),4.60(s,1H),4.28(s,1H),3.86(s,3H),3.57–3.48(m,4H),2.98–2.94(m,1H),2.87–2.80(m,2H),2.64–2.53(m,1H),2.47–2.42(m,1H),2.19–1.96(m,6H),1.87–1.81(s,2H),1.62–1.47(m,2H),1.43–1.36(m,2H).
M001301作为原料进一步制备得到M001320和M001321
在25℃下,向1-(6-(4-氨基环己基)-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-2-基)乙烷-1-酮(215mg,0.414mmol)和Boc2O(181mg,0.828mol)的DCM(6mL)溶液中加入TEA(41.9mg,1.24mmol)。将反应混合物在25℃下在N2下搅拌1小时。将混合物在减压下浓缩。残留物通过SFC纯化(Daicel CHIRALCEL IB-N,250mm×30mm I.D.,10μm;流动相CO2/MeOH[0.2%NH3(7M MeOH溶液)]=50/40;80g/min;35℃),得到白色固体((1s,4s)-4-(2-乙酰基-7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己基)氨基甲酸叔丁酯(37.2mg,14.5%产率)和((1r,4r)-4-(2-乙酰基-7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己基)氨基甲酸叔丁酯(105.3mg,41%)。
在25℃下,向(1s,4s)-4-(2-乙酰基-7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己基)氨基甲酸叔丁酯(37.2mg,0.0601mmol)的二氧六环(5mL)溶 液中加入在二恶环(4N,5mL)的HCl。将反应混合物在25℃下搅拌1小时。通过冷冻干燥将水中溶液干燥,得到28.5mg(84%)白色固体的1-(6-((1s,4s)-4-氨基环己基)-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-2-基)乙-1-酮盐酸盐。
在25℃下,向(1r,4r)-4-(2-乙酰基-7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己基)氨基甲酸叔丁酯(105.3mg,0.170mmol)的二氧六环(5mL)溶液中加入在二恶环(4N,5mL)的HCl。将反应混合物在25℃下搅拌1小时。通过冷冻干燥将水中溶液干燥,得到白色固体的1-(6-((1r,4r)-4-氨基环己基)-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-2-基)乙-1-酮盐酸盐(93.2mg,98%产率)。
M001320:
1H NMR(400MHz,DMSO-d6)δ7.98(s,3H),7.75(s,1H),7.49(s,1H),7.19–7.10(m,3H),6.74(t,J=55.2Hz,1H),6.45–6.35(m,1H),4.92–7.80(m,1H),4.71–4.50(m,2H),4.36–4.20(m,1H),3.86(s,3H),3.56–3.49(m,2H),3.14–3.00(m,1H),2.93–2.83(m,2H),2.61–2.52(m,1H),2.07–1.96(m,7H),1.92–1.80(m,2H),1.62–1.40(m,4H).
M001321:
1H NMR(400MHz,DMSO-d6)δ7.99(s,3H),7.75(s,1H),7.49(s,1H),7.28–7.18(m,2H),7.13(s,1H),6.74(t,J=55.2Hz,1H),6.46–6.34(m,1H),4.92–4.81(m,1H),4.74–4.52(m,2H),4.45–4.22(m,1H),3.86(s,3H),3.62–3.51(m,2H),3.45–3.42(m,1H),2.92–2.84(m,2H),2.65–2.55(m,1H),2.05–1.98(m,5H),1.89–1.72(m,6H),1.69–1.58(m,2H).
实施例7
在0℃下,向1-(6-(4-氨基环己基)-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-2-基)乙-1-酮(60mg,0.12mmol)的DCM(2.0mL)和THF(1.0mL)溶液中添加TEA(23.4mg,0.23mmol)和乙酰氯(13.6mg,0.17mmol。将混合物在25℃下搅拌0.5小时。LCMS显示消耗了起始材料并检测到所需产物。粗产物通过制备HPLC纯化,用CH3CN在H2O(0.1%NH3)中洗脱,在7分钟内从33%洗脱至43%,得到白色固体N-((1s,4s)-4-(2-乙酰基-7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己基)乙酰胺(2.8mg,4%产率)和N-((1r,4r)-4(2-乙酰基-7-(7-[二氟甲基]-6-(1-乙基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚啉-5-基)环己基)乙酰胺(11.7mg、18%产率)。
M001304
1H NMR(400MHz,DMSO-d6)δ7.76–7.73(m,2H),7.49(s,1H),7.17(s,1H),7.15–7.07(m,2H),6.74(t,J=55.1Hz,1H),6.40(d,J=28.8Hz,1H),4.85(s,1H),4.64(s,1H),4.61(s,1H),4.28(s,1H),3.86(s,3H),3.58–3.52(m,3H),2.90–2.86(m,2H),2.60–2.53(m,1H),2.10–1.96(m,5H),1.91–1.81(m,4H),1.79–1.77(m,3H),1.59–1.49(m,2H),1.32–1.24(m,2H).
M001308
1H NMR(400MHz,DMSO-d6)δ7.83(d,J=8.0Hz,1H),7.74(s,1H),7.49(s,1H),7.19(d,J=11.2Hz,1H),7.17–7.08(m,2H),6.74(t,J=55.2Hz,1H),6.40(d,J=27.2Hz,1H),4.86(s,1H),4.66(s,1H),4.62(s,1H),4.29(s,1H),4.00-3.96(m,1H),3.86(s,3H),3.67–3.48(m,2H),2.90–2.87(m,2H),2.63–2.54(m,1H),2.13–1.92(m,5H),1.85–1.83(m,3H),1.82–1.76(m,2H),1.69–1.65(m,2H),1.61–1.56(m,4H).
实施例8
向4-甲磺酰基环己-1-酮(0.6g,0.0034mol)的DCM(10mL)溶液中加入Tf2O(1.92g,0.0068mol)和2,6-二叔丁基-4-甲基吡啶(1.54g,0.00748mol)。将反应混合物在40℃下搅拌16小时。TLC显示形成了所需的产物。反应混合物用DCM稀释,用HCl(1N)洗涤并用DCM萃取。有机层用无水Na2SO4干燥,过滤并真空浓缩。残留物通过快速柱色谱法纯化,用DCM在PE中洗脱0%至100%,得到白色固体4-甲磺酰基环己-1-烯-1-基三氟甲磺酸酯(490mg,47%)。
向4-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)-1,3-二氢异吲哚-2-甲酸叔丁酯(325mg,0.5359mmol)的1,4-二氧六环(6mL)和H2O(1mL)溶液中加入4-甲磺酰基环己-1-烯-1-基三氟甲磺酸酯(165mg,0.5359mmol),XPhos Pd G3(45mg,0.05359mmol)和K2CO3(2mg,1.6077mmol)。将反应溶液加热至100℃,并在该温度下在N2下搅拌4小时。LCMS显示形成了所需的产物。将混合物冷却至25℃,并在减压下浓缩。残留物通过硅胶色谱法纯化,用MeOH在DCM中从0%至5%洗脱,得到黄色油状4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲基磺酰基)环己-1-烯-1-基)异吲哚啉-2-甲酸叔丁酯(225mg,66%)。
向4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲基磺酰基)环己-1-烯-1-基)异吲哚啉-2-甲酸叔丁酯(225mg,0.3522mmol)的DCM(3mL)溶液中加入TFA(1mL)。将反应混合物在25℃下搅拌30分钟。LCMS显示形成了所需的产物。在减压下除去溶剂,得到黄色油状7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-1-(6-(4-(甲基磺酰基)环己-1-烯-1-基)异吲哚啉-4-基)-1,2,3,4-四氢喹啉(185mg,粗品)。
向7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-1-(6-(4-(甲基磺酰基)环己-1-烯-1-基)异吲哚啉-4-基)-1,2,3,4-四氢喹啉(185mg,0.3434mmol)的DCM(1mL)溶液中加入TEA(695mg,6.868mmol)和乙酰氯(270mg,3.434mmol)。将反应混合物在25℃下搅拌50分钟。LCMS显示形成了所需的产物。 减压除去溶剂,残留物通过硅胶色谱法纯化,用MeOH在DCM中从0%至10%洗脱,得到黄色固体1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲基磺酰基)环己-1-烯-1-基)异吲哚啉-2-基)乙-1-酮(90mg,45%)。
向1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲基磺酰基)环己-1-烯-1-基)异吲哚啉-2-基)乙-1-酮(90mg,0.1550mmol)的MeOH(30mL)溶液中加入10%Pd/C(49mg,0.0465mmol)。将反应混合物在25℃下搅拌16小时。LCMS显示形成了所需的产物。过滤反应混合物,真空浓缩,残留物通过Pre-HPLC(色谱柱:-Xbridge-C18 150x19x19mm,5um流动相:ACN-H2O(0.1%FA))纯化,得到1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲基磺酰基)环己基)异吲哚啉-2-基)乙-1-酮(30mg,33%)。
采用高效液相色谱法(Daicel CHIRALCEL IB-N,250mm)纯化1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲基磺酰基)环己基)异吲哚啉-2-基)乙-1-酮(30mg,0.0515mmol)内径30毫米,10微米;流动相:CO2/MeOH[0.2%NH3(7M MeOH溶液)]=50/40;80g/分钟;35℃)得到1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-((1s,4s)4-(甲基磺酰基)环己基)异吲哚啉-2-基)乙-1-酮(6.4mg,21%),为黄色固体;和1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-((1r,4r)4-(甲基磺酰基)环己基)异吲哚啉-2-基)乙-1-酮(14.0mg,47%)。
M001299:
1H NMR(400MHz,DMSO-d6)δ7.75(s,1H),7.49(s,1H),7.13(t,J=12.8Hz,3H),6.88(s,0.25H),6.74(s,0.5H),6.60(s,0.25H),6.44-6.37(m,1H),4.87–4.25(m,4H),3.86(s,3H),3.55(d,J=4.8Hz,2H),3.11(s,1H),2.93(d,J=4.4Hz,3H),2.88(s,2H),2.61(s,1H),2.18(s,2H),2.04–1.94(m,7H),1.60–1.50(m,4H).
M001310:
1H NMR(400MHz,DMSO-d6)δ7.75(s,1H),7.49(s,1H),7.17–7.06(m,3H),6.87(s,0.25H),6.74(s,0.5H),6.60(s,0.25H),6.44–6.37(m,1H),4.87–4.29(m,4H),3.86(s,3H),3.55(d,J=4.8Hz,2H),3.31–3.26(m,1H),2.97(d,J=4.8Hz,3H),2.88(s,2H),2.82–2.72(m,1H),2.15(d,J=12.8Hz,2H),2.09–1.97(m,7H),1.91–1.83(m,2H),1.73–1.67(m,2H).
实施例9
向6-氯-3,4-二氢-2H-萘-1-酮(5.00g,0.027mol)的MeOH(50.0mL)溶液中加入吡啶(2.63g,0.033mol)和O-甲基羟胺盐酸盐(2.78g,0.03mol)。将反应溶液在25℃下在N2下搅拌12小时。将混合物在减压下浓缩。残留物通过硅胶色谱法在10分钟内用EA/PE(EA为0-5%)洗脱进行纯化,得到白色油状的(E)-6-氯-3,4-二氢萘-1(2H)-酮O-甲基肟(5.60g,92%产率)。
向(E)-6-氯-3,4-二氢萘-1(2H)-酮O-甲基肟(5.6g,0.026mol)的AcOH(50.0mL)溶液中加入N-溴代琥珀酰亚胺(4.75g,0.026mol)和Pd(OAc)2(0.60g,0.003mol)。将反应溶液在90℃下在微波辐射下搅拌0.5小时。将混合物浓缩,残留物用NaHCO3溶液(100mL)洗涤,并用DCM(60mL×2)萃取。合并的有机层用盐水(50mL)洗涤并用Na2SO4干燥,过滤并浓缩至干。残留物通过硅胶色谱法在10分钟内用EA/PE(EA为0-5%)洗脱进行纯化,得到黄色油状的(E)-8-溴-6-氯-3,4-二氢萘-1(2H)-酮O-甲基肟(6.50g,80%产率)。
在微波辐射下,将(E)-8-溴-6-氯-3,4-二氢萘-1(2H)-酮O-甲基肟(6.50g,0.022mol)的1,4-二氧六环(15.0mL)和6N HCl(70.0mL)溶液在120℃下搅拌2小时。将混合物浓缩,残留物用NaHCO3溶液(100mL)洗涤,并用DCM(60mL×2)萃取。合并的有机层用盐水(50mL)洗涤并用Na2SO4干燥,过滤并浓缩至干。残留物通过硅胶色谱法纯化,用EA/PE(EA为0-5%)在10分钟内洗脱为黄色油状的8-溴-6-氯-3,4-二氢萘-1(2H)-酮(5.10g,83%产率)。
向8-溴-6-氯-3,4-二氢萘-1(2H)-酮(5.10g,0.019mol)的EtOH(50.0mL)和吡啶(10.0mL)溶液中加入盐酸羟胺(2.05g,0.029mol)。将反应溶液在100℃下在微波辐射下搅拌1小时。过滤混合物并收集残留物得到白色固体(E)-8-溴-6-氯-3,4-二氢萘-1(2H)-酮肟(4.60g,81%产率)。
在0℃下,向(E)-8-溴-6-氯-3,4-二氢萘-1(2H)-酮肟(4.60g,0.016mol)的DMF(50.0mL)溶液中加入NaH(2.02g,0.050mol)。然后将整个混合物在0℃下搅拌0.5小时,并加入4-甲基苯磺酰氯 (3.84g,0.020mol)。将混合物在25℃下搅拌0.5小时。将混合物倒入水中,并用DCM(100mL×2)萃取整个混合物。将合并的有机相用盐水(50mL)洗涤。将合并的有机相用硫酸钠干燥并过滤。滤液在减压下浓缩。残留物通过硅胶色谱法纯化,用THF在PE中从0%至10%洗脱,得到黄色固体(E)-8-溴-6-氯-3,4-二氢萘-1(2H)-酮O-甲苯磺酰基肟(2.30g,27%产率)
将(E)-8-溴-6-氯-3,4-二氢萘-1(2H)-酮O-甲苯磺酰基肟(2.30g,0.005mol)在TFA(30.0mL)中的溶液在25℃下搅拌1小时。减压浓缩混合物。残留物通过硅胶色谱法在15分钟内用THF/PE(THF为0-50%)洗脱进行纯化,得到黄色油状的9-溴-7-氯-2,3,4,5-四氢-1H-苯并[c]氮杂卓-1-酮(0.91g,57%产率)。
在25℃下,向BH3(1M THF,66.3mL)溶液中加入9-溴-7-氯-2,3,4,5-四氢-1H-苯并[c]氮杂卓-1-酮(910mg,3.32m mol)。将反应混合物加热至65℃,并在65℃,N2下搅拌25小时。将反应混合物冷却至环境温度并用MeOH淬灭,直到气泡停止。然后加入4N HCl的水溶液,将混合物在80℃下加热1小时。将混合物冷却至室温。反应混合物用乙酸乙酯(50mL×2)萃取。加入水相5N KOH将pH调节至8,并用DCM(50mL×2)萃取。将混合物减压浓缩,得到黄色油状的9-溴-7-氯-2,3,4,5-四氢-1H-2-苯并氮杂卓(850mg,产率89%)。
在25℃下,向9-溴-7-氯-2,3,4,5-四氢-1H-2-苯并氮(850mg,3.26mmol)的THF(20.0mL)和H2O(10.0mL)溶液中加入NaHCO3(822mg,9.79mmol)和二碳酸二叔丁酯(783mg,3.59mmol。将反应混合物在25℃下搅拌16小时。用乙酸乙酯(20mL×2)萃取混合物。将合并的有机相用硫酸钠干燥并过滤。滤液在减压下浓缩。残留物通过硅胶色谱法纯化,用石油中的EtOAc从0%至5%洗脱,得到无色油状的9-溴-7-氯-1,3,4,5-四氢-2-苯并氮杂卓-2-甲酸叔丁酯(1000mg,77%产率)。
向9-溴-7-氯-1,3,4,5-四氢-2-苯并氮杂-2-甲酸叔丁酯(300mg,0.831mmol)的1,4-二氧六环(10.0mL)溶液中加入7-(二氟甲基)-6-(1-甲基吡唑-4-基)-1,2,3,4-四氢喹啉(219mg,0.831mmol),Cphos-Pd G3(67.0mg,0.083mmol)和LHMDS(418mg,2.495mmol)。将反应溶液加热至100℃,并在N2下搅拌12小时。将混合物冷却至25℃并减压浓缩。残余物通过硅胶色谱纯化,用MeOH/DCM(MeOH从0到10%)洗脱10分钟,得到7-氯-9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-1,3,4,5-四氢-2H-苯并[c]氮杂卓-2-甲酸叔丁酯(220mg,产率22%),为黄色固体。
向7-氯-9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-1,3,4,4,5-四氢-2H-苯并[c]氮杂卓-2-甲酸叔丁酯(200mg,0.368mmol)的1,4-二氧六环(10.0mL)溶液中加入4,4,5,5-四甲基-2-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)-1,3,2-二氧杂硼杂环戊烷(187mg,0736mmol),AcOK(72.0mg,0.736mmol)和XPhos Pd G3(31.0mg,0.036mmol)。将反应溶液加热至100℃,并在N2下搅拌2小时。将混合物冷却至25℃,并在减压下浓缩,得到黑色固体的9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-7-(4,4,5,5-四甲基-1,3,2-二氧杂硼烷-2-基)-1,3,4,5-四氢-2H-苯并[c]氮杂卓-2-甲酸叔丁酯(300mg,产率64%)。
向9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-1-(4,4,4,5,5-四甲基-1,3,3,4,5-四甲基-1,3,4,5-四氢-2H-苯并[c]氮杂卓-2-甲酸叔丁酯(200mg,0.315mmol)的1,4-二氧六环(6.0mL)和H2O(1.1.0mL)溶液中加入4-溴-1-乙基吡啶-2-酮(191mg,0.945mmol)、K2CO3(87.0mg,0.630mmol)和XPhos Pd G3(27.0mg,0.031mmol)。将反应溶液加热至100℃,并在N2下搅拌3小时。将混合物冷却至25℃并在减压下浓缩。残留物通过硅胶色谱法用MeOH/DCM(用0至5%的MeOH)在10分钟内洗脱来纯化,得到黄色固体9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-7-(1-乙基-2-氧代-1,2-二氢吡啶-4-基)-1,3,4,5-四氢-2H-苯并[c]氮杂-2-甲酸叔丁酯。
向9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-7-(1-乙基-2-氧代-1,2-二氢吡啶-4-基)-1,3,4,5-四氢-2H-苯并[c]氮杂卓-2-甲酸叔丁酯(120mg,0.190mmol)的MeOH(10.0mL)溶液中加入PtO2(43.0mg,0mmol)。将溶液在25℃下在H2下搅拌12小时。过滤混合物以除去固体并浓缩。残留物通过硅胶色谱法在10分钟内用MeOH/DCM(MeOH为0-5%)洗脱进行纯化,得到黄色固体9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-7-(1-乙基-2-氧代哌啶-4-基)-1,3,4,5-四氢-2H-苯并[c]氮杂卓-2-甲酸叔丁酯(114mg,产率90%)。
将9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-7-(1-乙基-2-氧代哌啶-4-基)-1,3,4,5-四氢-2H-苯并[c]氮杂卓-2-甲酸叔丁酯(114mg,0.179mmol)的DCM(5.0mL)和TFA(2.0mL)中的溶液在25℃下搅拌1小时。混合物在减压下浓缩,得到黄色油状的4-(9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-2,3,4,5-四氢-1H-苯并[c]氮杂卓-7-基)-1-乙基哌啶-2-酮(90.0mg,产率84%)。
向4-(9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-2,3,4,5-四氢-1H-苯并[c]氮杂卓-7-基)-1-乙基哌啶-2-酮(25.0mg,0.046mmol)的DCM(5.0mL)溶液中加入Et3N(14.0mg, 0.0mg,0.140mmol)和氯(甲氧基)甲酮(13.0mg,0.140mmol)。将反应溶液在25℃下搅拌1小时。在减压下浓缩混合物,残留物通过制备HPLC(用CH3CN在8分钟内从50%到80%)纯化,得到白色固体9-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-7-(1-乙基-2-氧代哌啶-4-基)-1,3,4,5-四氢-2H-苯并[c]氮杂卓-2-甲酸甲酯(4.4mg,16%产率)。
M001260:
1H NMR(400MHz,DMSO-d6)δ7.71(s,1H),7.47(s,1H),7.09(d,J=8.0Hz,2H),7.02(d,J=8.0Hz,1H),6.86–6.53(m,1H),6.09(d,J=48.0Hz,1H),4.85–3.91(m,2H),3.85(s,3H),3.69(s,1H),3.54(d,J=28.0Hz,3H),3.39–3.34(m,2H),3.31–3.19(m,5H),3.02–2.88(m,5H),2.49–2.30(m,2H),2.16–1.98(m,3H),1.91–1.58(m,3H),1.03–0.96(m,3H).
实施例10
-10℃下,将5-氯-2-甲基苯甲酸(20g,117.24mmol)加入到冷却的浓H2SO4(135mL)中。搅拌10分钟后,在-10℃下滴加浓HNO3(16.47g,261.44mmol)和浓H2SO4(22mL)的混合溶液。将混合物在-10℃下搅拌12小时后倒在冰水中,过滤沉淀的固体,用水洗涤直到滤液的pH为7左右,并在真空下干燥,得到灰白色固体5-氯-2-甲基-3-硝基-苯甲酸(15.5g,粗品)。
在0℃下,向5-氯-2-甲基-3-硝基-苯甲酸(15.5g,71.90mmol)的DCM(150mL)溶液中滴加草酰氯(18.25g,143.79mmol)和DMF(525.49mg,7.19mmol。将混合物在25℃下搅拌3小时。真空浓缩反应,得到黄色固体的5-氯-2-甲基-3-硝基-苯甲酰氯(15.8g,67.51mmol,粗品)。
在0℃和N2下,向5-氯-2-甲基-3-硝基-苯甲酰氯(15.8g,67.51mmol)的THF(150mL)溶液中滴加三甲基硅烷化重氮甲烷(2M,135.02mL)。将混合物在25℃下搅拌12小时。将反应物在真空中浓缩,得到黄色胶状物的1-(5-氯-2-甲基-3-硝基-苯基)-2-重氮基-乙酮(16g,粗品)。
在0℃搅拌下向TEA(33.78g,3.87mmol)和苯甲酸银(9.17g,40.06mmol)的MeOH(60mL)溶液中,然后逐滴加入溶解在MeOH中的1-(5-氯-2-甲基-3-硝基-苯基)-2-重氮基-乙酮(16g,66.77mmol)。将反应混合物在25℃下搅拌1小时。混合物用饱和HCl水溶液(1M)(500mL)洗涤,然后用EA(600mL X 3)萃取。有机层用无水Na2SO4干燥,过滤并在减压下浓缩,得到残留物。粗品通过FCC纯化(40g二氧化硅柱,0~10%乙酸乙酯/石油醚梯度洗脱液@50mL/min),石油醚/乙酸乙酯=3:1,Rf=0.7),得到黄色固体2-(5-氯-2-甲基-3-硝基-苯基)乙酸甲酯(12.1g,49.66mmol,74.37%产率)。
向2-(5-氯-2-甲基-3-硝基-苯基)乙酸甲酯(12.1g,49.66mmol)的EtOH(100mL)溶液中加入DIBAH(25.94g,148.99mmol)在90℃下溶解在H2O(30mL)中。将混合物在90℃下搅拌10分钟。用饱和H2O(400mL)洗涤混合物,然后用EA(600mL×3)萃取。有机层用无水Na2SO4干燥,过滤并在减压下浓缩,得到残留物。粗品通过FCC(40g二氧化硅柱,0~20%乙酸乙酯/石油醚梯度洗脱液@40mL/min),石油醚/乙酸乙酯=3:1,Rf=0.4)纯化,得到白色固体的2-(3-氨基-5-氯-2-甲基-苯基)乙酸甲酯(3.2g,14.98mmol,30.16%产率)。
将NaNO2(1.14g,16.47mmol)在H2O(15mL)中的溶液加入2-(3-氨基-5-氯-2-甲基苯基)乙酸甲 酯(3.2g,14.98mmol)的HCl(2M,14.98mL)溶液中,并将ACN(10mL)冷却至5℃以下。在0℃下搅拌45分钟后,逐滴倒入KI(3.73g,22.47mmol)在H2O(15mL)中的溶液。使所得混合物达到25℃并搅拌4小时。将混合物倒入150mL水中,用EA(300mL×3)萃取,浓缩合并的有机层,得到粗产物。粗品经FCC(20g二氧化硅柱,0~10%乙酸乙酯/石油醚梯度洗脱液40mL/min)。TLC:石油:乙酸乙酯=3:1,Rf=0.8),得到白色固体2-(5-氯-3-碘-2-甲基-苯基)乙酸甲酯(3.8g,11.71mmol,78.18%产率)。
在0℃下搅拌2-(5-氯-3-碘-2-甲基-苯基)乙酸甲酯(3.8g,11.71mmol)、NBS(2.50g,14.05mmol)在CCl4(38mL)中的混合物。然后向混合物中加入BPO(567.24mg,2.34mmol)。将残留物脱气并用N2置换3次,然后将混合物在85℃下在N2气氛下搅拌3小时。将混合物倒入水(500mL)中,用DCM(500mL×3)萃取,浓缩合并的有机层,得到粗产物。通过FCC(40g二氧化硅柱,0~10%乙酸乙酯/石油醚梯度洗脱液40mL/min)纯化粗产物,得到呈灰白色液体的2-[2-(溴甲基)-5-氯-3-碘代-苯基]乙酸甲酯(4.1g,10.16mmol,86.79%收率)。
在25℃下向2-[2-(溴甲基)-5-氯-3-碘代-苯基]乙酸甲酯(4.1g,10.16mmol)的EtOH(5mL)溶液中加入MeNH2(10.52g,101.63mmol)。将混合物在25℃下搅拌2小时。反应物在真空中浓缩后粗品通过FCC(40g二氧化硅柱,0~30%乙酸乙酯/石油醚梯度洗脱液40mL/min)纯化。TLC:石油醚:乙酸乙酯=0∶1,Rf=0.5),得到灰白色固体6-氯-8-碘-2-甲基-1,4-二氢异喹啉-3-酮(2.32g,7.22mmol,71.00%产率)。
向6-氯-8-碘-2-甲基-1,4-二氢异喹啉-3-酮(500mg,1.56mmol)、7-(二氟甲基)-6-(1-甲基吡唑-4-基)-1,2,3,4-四氢喹啉(409.41mg,1.56mmol)、Cs2CO3(1.52g,4.67mmol)和甲苯(5mL)脱气并用N2置换3次,然后加入Cphos Pd G3(125.39mg,0.156mmol),并将混合物在110℃下在N2下搅拌1小时。反应物在真空中浓缩。将混合物倒入50mL水中,用EA(100mL×3)萃取,浓缩合并的有机层,得到粗产物。残留物通过快速硅胶色谱法(12g二氧化硅柱,洗脱液为0~5%MeOH/DCM梯度@30mL/min),得到黄色油状的6-氯-8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-2-甲基-1,4-二氢异喹啉-3-酮(160mg,0.350mmol,22.52%产率)。
6-氯-8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-2-甲基-1,4-二氢异喹啉-3-酮(50mg,0109mmol)、1-甲基-4-(4,4,5,5-四甲基-1,3,2-二氧杂硼烷-2-基)-3,6-二氢-2H-吡啶(24,42mg,将K3PO4(69.69mg,0.328mmol)和XPhos Pd G3(18.53mg,0.0219mmol)的THF/H2O(V:V=5:1)(1mL)中的溶液放入微波管中,并将混合物在60℃下在微波下搅拌0.5小时。将反应混合物在减压下浓缩,得到残留物。残留物通过制备TLC(SiO2,PE:EA=1∶1)纯化,得到8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-2-甲基-6-(1-乙基-3,6-二氢-2-吡啶-4-基)-1,4-二氢异喹啉-3-酮(35mg,0.0676mmol,61.79%产率),为黄色胶状物。
将8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-2-甲基-6-(1-甲基-3,6-二氢-1H-吡啶-4-基)-1,4-二氢异喹啉-3-酮(35mg,0.0676mmol)、Pd/C(30mg,10%纯度)的MeOH(1mL)中的混合物脱气并用H2置换3次,然后将混合物在25℃下在H2(15Psi)气氛下搅拌0.5小时。将反应混合物过滤并在减压下浓缩,得到残留物。然后通过制备的HPLC(Welch Xtimate C18150*25mm*5mm,流动相A:水(FA),流动相B:乙腈,流速:25ml/min,梯度条件为5%B至50%)进一步纯化产物。收集纯级分,并在真空下除去挥发物。残留物在乙腈(2mL)和水(10mL)之间分配。将该溶液冻干,得到8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-2-甲基-6-(1-甲基-4-哌啶基)-1,4-二氢异喹啉-3-酮(1.07mg,0.00192mmol,2.83%产率,93%纯度),为黄色胶状物。
M001028:
1H NMR(400MHz,METHANOL-d4)δ8.49(br s,1H)7.62(s,1H)7.49(s,1H)7.10-7.16(m,3H)6.50(t,J=55.41Hz,1H)6.30(s,1H)4.54-4.63(m,1H)4.28-4.51(m,2H)3.93(s,3H)3.60-3.72(m,3H)3.46-3.55(m,3H)3.02-3.05(m,1H)3.00(s,3H)2.94-2.99(m,2H)2.86-2.93(m,1H)2.83(s,3H)2.07-2.20(m,4H)1.87-2.00(m,2H).
实施例11
将2-溴-6-碘苯腈(3.9g,0.012mol),丙炔酸甲酯(1.1g,0.012mmol),Pd(PPh3)2Cl2(0.90g,0.0012mol)和CuI(0.49g,0.0025mol)在DMF(20mL)和TEA(20mL)中的混合物在25℃,N2下搅拌。将混合物加热至50℃并在此温度下搅拌2小时。将反应混合物冷却至25℃,用水(100mL)稀释并用EtOAc(100mL×2)萃取。将合并的有机相用Na2SO4干燥并过滤。滤液在减压下浓缩。通过硅胶色谱法纯化残余物,用EtOAc/石油醚洗脱,EtOAc在15分钟内从0%洗脱至100%,得到3-(3-溴-2-氰基苯基)丙酸甲酯(1.5g,50%收率),为黄色固体。
向3-(3-溴-2-氰基苯基)丙炔酸甲酯(2g,7.57mmol)的EtOH(20mL)和THF(20mL)溶液中依次加入PtO2(171mg,0.75mmol)。将反应混合物在25℃的氢气氛(气球)下搅拌2小时。将反应混合物通过硅藻土垫过滤,然后将滤液减压浓缩,得到黄色固体3-(3-溴-2-氰基苯基)丙酸甲酯(1.5g,产率66%)。
将3-(3-溴-2-氰基苯基)丙酸甲酯(400mg,1.49mmol),7-(二氟甲基)-6-(1-甲基吡唑-4-基)-1,2,3,4-四氢喹啉(314mg,1.19mmol),Cs2CO3(1458mg,4.4757mmol),Pd2(dba)3(136mg,0.14mmol)和Xantphos(172mg,0.29mmol)在二氧六环(10mL)中的混合物在25℃,N2下搅拌。将混合物加热至100℃并在此温度下搅拌10小时。将反应混合物冷却至25℃,用水(10mL)稀释并用EtOAc(30mL×2)萃取。将合并的有机相用Na2SO4干燥并过滤。滤液在减压下浓缩。残余物通过硅胶色谱纯化,用EtOAc/石油醚洗脱,EtOAc在15分钟内从0%洗脱至100%,得到3-{2-氰基-3-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]苯基}丙酸甲酯(300mg,产率40%),为黄色固体。
在25℃下,向3-{2-氰基-3-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]苯基}丙酸甲酯(150mg,0.33mmol)的MeOH(4mL)溶液中加入Raney Ni(19mg,0.33mmol)。加入后,将混合物在25℃下在H2下搅拌2小时。将反应混合物通过硅藻土垫过滤,然后减压浓缩滤液。通过制备HPLC(CH3CN在10分钟内从10%至70%)纯化残余物,得到白色固体9-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,2,4,5-四氢-2-苯并氮杂卓-3-酮(10mg,产率7%)。
M001215:
1H NMR(400MHz,DMSO-d6)δ7.87–7.84(m,1H),7.72(s,1H),7.47(s,1H),7.35–7.30(m,1H),7.25–7.20(m,1H),7.15–7.05(m,2H),6.80–6.55(m,1H),6.16(s,1H),4.30–4.13(m,2H),3.88(s,3H),3.50–3.45(m,1H),3.25–3.15(m,1H),3.02–2.80(m,3H),2.72–2.60(m,1H),2.54–2.50(m,2H),2.13–2.03(m,2H).
实施例12
向7-(二氟甲基)-6-(1-甲基吡唑-4-基)-1,2,3,4-四氢喹啉(100mg,0.380mmol)和9-溴-1,3,4,5-四 氢-1-苯并氮杂卓-2-酮(109mg,0.456mmol)的1,4-二氧六环(15mL)溶液中加入t-BuONa(73.0mg,0.760mmol)和Cphos-Pd G3(30.6mg,0.0379mmol)。将反应混合物在90℃下搅拌16小时。将反应混合物加入水中(20mL)。水相用乙酸乙酯(30mL×2)萃取。将合并的有机相用硫酸钠干燥并过滤。滤液在减压下浓缩。通过制备HPLC(CH3CN为45%至75%)在9分钟内纯化残余物,得到白色固体9-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3,4,5-四氢-1-苯并氮杂卓-2-酮(2.40mg,产率1.5%)。
M001236:
1H NMR(400MHz,DMSO-d6)δ8.90(s,1H),7.71(s,1H),7.46(s,1H),7.24(s,3H),7.08(s,1H),6.70(t,J=55.2Hz,1H),6.19(s,1H),3.85(s,3H),3.60–3.46(m,2H),2.90–2.83(m,2H),2.77–2.71(m,2H),2.25–1.97(m,6H).
实施例13
在25℃下,向6-氯-4-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-2-甲酸叔丁酯(400mg,0.777mmol)的二氧六环(20mL)溶液中加入2-氰基乙酸乙酯(351mg,3.11mmol),K3PO4(495mg,2.33mmol)和Xhos-Pd G3(65.7mg,0.0776mmol)。将反应混合物在25℃,N2下搅拌2小时。将反应混合物加入水中(20mL),水相用乙酸乙酯(50×2mL)萃取,合并的有机相用NaCl水溶液(10mL×2)洗涤,用Na2SO4干燥,过滤,减压浓缩。残余物通过硅胶色谱纯化,用EtOAc在石油中从0%至50%洗脱,得到6-(1-氰基-2-乙氧基-2-氧乙基)-4-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-2-甲酸叔丁酯(440mg,纯度95%,收率91%),为黄色固体。
在25℃下,向6-(1-氰基-2-乙氧基-2-氧乙基)-4-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基)-1,3-二氢异吲哚-2-甲酸叔丁酯(230mg,0.389mol)的THF(35mL)溶液中加入硼烷-四氢呋喃复合物(1M,23mL)。将反应混合物加热至60℃,并在氮气下于60℃搅拌5小时。将反应混合物冷却至环境温度并用MeOH淬灭直至停止鼓泡。混合物在减压下浓缩。滤液用水(50mL)淬灭,然后用DCM(30mL×2)萃取。将合并的有机相用硫酸钠干燥并过滤,得到白色固体6-(1-氨基-3-羟基丙烷-2-基)-4-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-2-甲酸叔丁酯(180mg,产率75%)。
向6-(1-氨基-3-羟基丙烷-2-基)-4-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-2-甲酸叔丁酯(180mg,0.0361mmol)的DCM(60mL)溶液中加入三光气(145mg,0.488mmol)。将反应混合物在25℃,N2下搅拌5小时。将混合物用水(30mL)淬灭,然后用DCM(30mL×2)萃取。将合并的有机相用硫酸钠干燥并过滤,得到4-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(2-氧代-1,3-恶嗪-5-基)-1,3-二氢异吲哚-2-甲酸叔丁酯(105mg,50%收率),为黄色固体。
在25℃下,向4-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(2-氧代-1,3-恶嗪-5-基)-1,3-二氢异吲哚-2-甲酸叔丁酯(105mg,0.181mmol)的DCM(6.0mL)溶液中加入TFA(2.0mL)。将反应混合物在25℃下搅拌0.5小时。将滤液减压浓缩,得到5-{7-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-2,3-二氢-1H-异吲哚-5-基}-1,3-恶嗪-2-酮(100mg,粗品),作为黄色油状物直接用于下一步,无需进一步纯化。
向5-{7-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-2,3-二氢-1H-异吲哚-5-基}-1,3-恶嗪-2-酮(107mg,0.223mmol)的DCM(10mL)溶液中加入TEA(67.7mg,0.670mmol)。将混合物在25℃下搅拌10分钟。将混合物减压浓缩。残余物通过Prep-HPLC纯化(CH3CN在9分钟内从28%至58%),得到白色固体的5-{2-乙酰基-7-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-5-基}-1,3-恶嗪-2-酮(8.70mg,产率7.5%)。
M001246:
1H NMR(400MHz,DMSO-d6)δ7.75(s,1H),7.50(s,1H),7.42–7.35(m,1H),7.29–7.22(m,2H),7.14(s,1H),6.75(t,J=55.2Hz,1H),6.44–6.35(m,1H),4.90–4.84(m,1H),4.76–4.45(m,2H),4.40–4.23(m,3H),3.86(s,3H),3.60–3.51(m,2H),3.44–3.37(m,3H),2.91–2.83(s,2H),2.05–1.96(m,5H).
向5-{2-乙酰基-7-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-5-基}-1,3-恶嗪-2-酮(20.0mg,0.0383mmol)的THF(6.0mL)溶液中滴加KHMDS(1M在THF中,0.1mL,0.0766mmol),温度为-60℃,N2气氛。搅拌10分钟后,在-30℃,N2气氛下滴加碘甲烷(8.15mg,0.0574mmol)的THF(0.5mL)溶液。在10℃下再搅拌20分钟后,将混合物用NH4Cl溶液(20mL)淬灭,然后用乙酸乙酯(20mL×2)萃取。将合并的有机相用硫酸钠干燥并过滤。滤液在减压下浓缩。将混合物减压浓缩,残余物通过Prep-HPLC纯化(CH3CN在8分钟内从35%至45%),得到5-{2-乙酰基-7-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-5-基}-3-甲基-1,3-恶嗪-2-酮(5.00mg,产率23%),为黄色固体。
M001238:
1H NMR(400MHz,DMSO-d6)δ7.75(s,1H),7.50(s,1H),7.30–7.22(m,2H),7.14(s,1H),6.75(t,J=55.0Hz,1H),6.45–6.33(m,1H),4.89–4.85(m,1H),4.69–4.54(m,2H),4.38–4.25(m,3H),3.86(s,3H),3.60–3.47(m,5H),2.91–2.84(m,5H),2.04(s,3H),2.01–1.93(m,2H).
实施例14
将1-甲氧基哌啶-4-酮(500mg,3.87mmol)的THF(15mL)溶液冷却至-78℃,并在N2下加入LDA(2M,2.5mL,5.03mmol)。将所得混合物在相同温度下搅拌30分钟,并加入1,1,1-三氟-N-苯基-N-(三氟甲烷)磺酰基甲磺酰胺(1.80g,5.03mmol)的THF(15mL)溶液处理。将反应混合物再搅拌30分钟并使其升温至25℃。将混合物用水(50mL)淬灭,然后用乙酸乙酯(60mL×2)萃取。将合并的有机相用硫酸钠干燥并过滤。滤液在减压下浓缩。通过硅胶色谱法纯化残余物,用0%至5%的四氢呋喃石油溶液洗脱,得到1-甲氧基-3,6-二氢-2H-吡啶-4-基三氟甲磺酸酯(687mg,纯度90%,收率61%),为无色油状物。
在25℃下,向8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)-3,4-二氢-1H-异喹啉-2-甲酸叔丁酯(234mg,0.377mmol)和1-甲氧基-3,6- 二氢-2H-吡啶-4-基三氟甲磺酸酯(197mg,0.754mmol)的二氧六环(8.0mL)和H2O(0.8mL)溶液中加入K2CO3(156mg,1.13mmol)和XPhos Pd G3(32.0mg,0.0377mmol)。将反应混合物加热至100℃,并在氮气下于100℃搅拌2小时。将混合物减压浓缩。残余物通过硅胶色谱纯化,用甲醇在DCM中从0%至5%洗脱,得到8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(1-甲氧基-3,6-二氢-2H-吡啶-4-基)-3,4-二氢-1H-异喹啉-2-甲酸叔丁酯(210mg,纯度90%,收率83%),为棕色固体。
向8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(1-甲氧基-3,6-二氢-2H-吡啶-4-基)-3,4-二氢-1H-异喹啉-2-甲酸叔丁酯(120mg,0.198mmol)的MeOH(10mL)溶液中加入Pd/C(21.1mg,0.198mmol)。将混合物在25℃的H2气球压力下搅拌16小时。过滤混合物以除去固体并浓缩。残余物通过Prep-HPLC纯化(CH3CN在9分钟内从70%至95%),得到8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(1-甲氧基哌啶-4-基)-3,4-二氢-1H-异喹啉-2-甲酸叔丁酯(70mg,产率57%),为白色固体。
M001274:
1H NMR(400MHz,DMSO-d6)δ7.71(s,1H),7.46(s,1H),7.11–7.00(m,3H),6.69(t,J=55.2Hz,1H),6.16(s,1H),4.44–4.32(m,1H),4.28–4.06(m,1H),3.86(s,3H),3.59–3.48(m,3H),3.44–3.40(3,3H),3.39–3.35(m,2H),2.95–2.79(m,4H),2.45–2.30(m,2H),2.07–1.99(m,2H),1.90–1.76(m,2H),1.75–1.59(m,2H),1.49–1.17(m,11H).
在25℃下,向8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(1-甲氧基哌啶-4-基)-3,4-二氢-1H-异喹啉-2-甲酸叔丁酯(76.0mg,0.125mmol)的DCM(6.0mL)溶液中加入TFA(2.0mL)。将反应混合物在25℃下搅拌0.5小时。将混合物减压浓缩,得到7-(二氟甲基)-1-[6-(1-甲氧基哌啶-4-基)-1,2,3,4-四氢异喹啉-8-基]-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉(65mg,产率97%),为黄色油状物,直接用于下一步,无需进一步纯化。
在25℃下,向7-(二氟甲基)-1-[6-(1-甲氧基哌啶-4-基)-1,2,3,4-四氢异喹啉-8-基]-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉(64.0mg,0.126mmol)的DCM(6.0mL)溶液中加入TEA(38.3mg,0.378mmol)和N-甲基氨基甲酰氯(17.7mg,0.189mmol)。将混合物在25℃下搅拌10分钟。将混合物用水(10mL)淬灭,然后用乙酸乙酯(20mL x 2)萃取。将合并的有机相用硫酸钠干燥并过滤。残余物通过Prep-HPLC纯化(CH3CN在9分钟内从50%至60%),得到白色固体8-[7-(二氟甲基)-6-(1H-吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(1-甲氧基哌啶-4-基)-N-甲基-3,4-二氢-1H-异喹啉-2-甲酰胺(26.9mg,产率38%)。
M001268:
1H NMR(400MHz,DMSO-d6)δ7.72(s,1H),7.47(s,1H),7.08(s,1H),7.04(s,1H),6.99(s,1H),6.69(t,J=55.2Hz,1H),6.51–6.42(m,1H),6.18(s,1H),4.46–4.36(m,1H),4.17–4.05(m,1H),3.86(s,3H),3.57–3.35(m,9H),3.03–2.70(m,5H),2.54(d,J=4.0Hz,3H),2.42–2.28(m,2H),2.10–1.99(m,2H),1.90–1.76(m,2H),1.74–1.56(m,2H).
实施例15
在25℃下,向8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-N-甲基-6-(哌啶-4-基)-3,4-二氢-1H-异喹啉-2-甲酰胺(50.0mg,0.0935mmol)的THF(2.0mL)溶液中,加入过氧化苯甲酰(34.0mg,0.140mmol)。将反应混合物在25℃下搅拌2小时。通过制备TLC(PE/THF=3:7)纯化反应混合物,得到4-{8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-2-(甲基氨基甲酰基)-3,4-二氢-1H-异喹啉-6-基}哌啶-1-基苯甲酸酯(20.0mg,产率29%),为白色固体。
在25℃下,向4-{8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-2-(甲基氨基甲酰基)-3,4-二氢-1H-异喹啉-6-基}哌啶-1-基苯甲酸酯(20.0mg,0.0305mmol)的MeOH(2mL)溶液中加入K2CO3(12.7mg,0.0915mmol)。将反应混合物在25℃下搅拌1小时。将混合物用水(10mL)淬灭, 然后用乙酸乙酯(20mL x 2)萃取。将合并的有机相用硫酸钠干燥并过滤。滤液在减压下浓缩。通过Prep-HPLC(CH3CN为20%至50%)在10分钟内纯化残余物,得到白色固体的8-[7-(二氟甲基)-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-(1-羟基哌啶-4-基)-N-甲基-3,4-二氢-1H-异喹啉-2-甲酰胺(4.00mg,产率24%)。
M001276:
1H NMR(400MHz,DMSO-d6)δ7.93(s,1H),7.71(s,1H),7.47(s,1H),7.08(s,1H),7.04(s,1H),6.99(s,1H),6.83–6.45(m,2H),6.18(s,1H),4.46–4.38(m,1H),4.15–4.06(m,1H),3.86(s,3H),3.55–3.41(m,4H),3.25–3.05(m,2H),3.00–2.77(m,5H),2.54(d,J=4.2Hz,3H),2.45–2.33(m,2H),2.10–2.00(m,2H),1.85–1.40(m,4H).
实施例16
在0℃下,向4-溴-1H-吡啶-2-酮(200mg,1.15mmol)的THF(8.0mL)溶液中加入t-BuOK(1M的THF溶液,1.8mL,1.8mmol)。将混合物在0℃下搅拌0.5小时。然后在0℃下将1-(2-甲氧基-5-甲基苯基)-2,6-二氧代哌啶-3-基三氟甲磺酸酯(526.0mg,1.4mmol)的THF(2.0mL)溶液加入反应混合物中。将混合物在0℃下搅拌0.5小时。将反应物减压浓缩,并通过硅胶色谱纯化,用EtOAc在PE中从0%至50%洗脱,得到3-(4-溴-2-氧代吡啶-1(2H)-基)-1-(4-甲氧基苄基)哌啶-2,6-二酮(300mg,产率64%),为黄色固体。
向6-氯-8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(300mg,0.57mmol)的二氧六环(4.0mL)溶液中加入4,4,5,5-四甲基-2-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)-1,3,2-二氧杂硼杂环戊烷(288.0mg,1.13mmol),AcOK(167.0mg,1.70mmol)和XPhos Pd G3(95.9mg,0.11mmol)。然后将混合物在100℃下搅拌2小时。LCMS显示原料被消耗并且检测到所需产物。过滤后,将滤液减压浓缩,得到8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(300mg,产率85%),为黄色油状物。
向8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(298.6mg,0.48mmol)的二氧六环(5.0mL)和H2O(0.5mL)溶液中加入3-(4-溴-2-氧代吡啶-1(2H)-基)-1-(4-甲氧基苄基)哌啶-2,6- 二酮(130.0mg,0.32mmol),K3PO4(204.3mg,0.96mmol)和XPhos Pd G3(54.3mg,0.06mmol)。然后将混合物在100℃下搅拌2小时。LCMS显示原料被消耗并且检测到所需产物。残留物通过快速柱色谱法纯化,用EtOAc在PE中从0%洗脱至50%,然后通过快速柱色谱纯化,用甲醇在DCM中从0%至5%洗脱,得到8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(1-(4-甲氧基苄基)-2,6-二氧代哌啶-3-基)-2-氧代-1,2-二氢吡啶-4-基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(160mg,收率91%),为黄色固体。
向8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(1-(1-(4-甲氧基苄基)-2,6-二氧代哌啶-3-基)-2-氧代-1,2-二氢吡啶-4-基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(300mg,0.37mmol)的DCM(6.0mL)溶液中加入TFA(2.0mL)。然后将混合物在25℃下搅拌0.5小时。LCMS显示原料被消耗并且检测到所需产物。将所得混合物减压浓缩,得到黄色固体3-(4-(8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-1,2,3,4-四氢异喹啉-6-基)-2-氧代吡啶-1(2H)-基)-1-(4-甲氧基苄基)哌啶-2,6-二酮(250mg,95%收率)。
向3-(4-(8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-1,2,3,4-四氢异喹啉-6-基)-2-氧代吡啶-1(2H)-基)-1-(4-甲氧基苄基)哌啶-2,6-二酮(200mg,0.42mmol)的DCM(2.0mL)溶液中加入TEA(126.7mg,1.3mmol)和N-甲基氨基甲酰氯(78.1mg,0.83mmol))在25℃。然后将混合物在25℃下搅拌0.5小时。加入水(50mL)淬灭反应,用DCM(50mL×3)萃取,用无水Na2SO4干燥。过滤后,将滤液减压浓缩,得到黄色固体的8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(1-(4-甲氧基苄基)-2,6-二氧代哌啶-3-基)-2-氧代-1,2-二氢吡啶-4-基)-N-甲基-3,4-二氢异喹啉-2(1H)-甲酰胺(130mg,产率60%)。
在25℃,H2气氛(15PSI)下,向8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(1-(4-甲氧基苄基)-2,6-二氧代哌啶-3-基)-2-氧代-1,2-二氢吡啶-4-基)-N-甲基-3,4-二氢异喹啉-2(1H)-甲酰胺(50mg,0.06mmol)的THF(1.0mL)溶液中加入PtO2(14.6mg,0.06mmol)。然后将混合物在25℃下搅拌12小时。LCMS显示原料被消耗并且检测到所需产物。过滤后,将滤液减压浓缩,得到黄色固体的8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(1’-(4-甲氧基苄基)-2,2’,6’-三氧基-[1,3’-联哌啶]-4-基)-N-甲基-3,4-二氢异喹啉-2(1H)-甲酰胺(40mg,产率80%)。
向8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(1’-(4-甲氧基苄基)-2,2’,6’-三氧基-[1,3’-联哌啶]-4-基)-N-甲基-3,4-二氢异喹啉-2(1H)-甲酰胺(50mg,0.06mmol)的TFA(2.0mL)溶液中加入TfOH(0.2mL)。然后将混合物在60℃下搅拌6小时。通过制备HPLC纯化反应,用0.1%FA/水中的CH 3 CN在7分钟内从27%洗脱至57%,得到8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基-6-(2,2',6'-三氧基-[1,3'-联吡啶]-4-基)-3,4-二氢异喹啉-2(1H)-甲酰胺(0.9mg,收率3%),为白色固体。
M001287:
1H NMR(400MHz,DMSO-d6)δ10.80(s,1H),7.71(s,1H),7.47(s,1H),7.10(d,J=11.2Hz,3H),6.70(t,J=55.2Hz,1H),6.48–6.45(m,1H),6.18(s,1H),4.44(d,J=16.8Hz,2H),4.40–4.29(m,1H),4.11(d,J=16.8Hz,2H),3.86(s,3H),3.57–3.51(m,2H),3.50–3.42(m,2H),3.40–3.35(m,2H),3.30–3.16(m,2H),3.16–3.05(m,2H),2.97–2.77(m,5H),2.55(d,J=4.4Hz,3H),2.14–1.87(m,4H).
向8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(1-(4-甲氧基苄基)-2,6-二氧代哌啶-3-基)-2-氧代-1,2-二氢吡啶-4-基)-N-甲基-3,4-二氢异喹啉-2(1H)-甲酰胺(50mg,0.06mmol)的TFA(2.0mL)溶液中加入TfOH(0.2mL)。然后将混合物在60℃下搅拌6小时。通过制备HPLC纯化反应,用0.1%FA/水中的CH3CN在7分钟内从26%洗脱至56%,得到白色的8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(1-(2,6-二氧代哌啶-3-基)-2-氧代-1,2-二氢吡啶-4-基)-N-甲基-3,4-二氢异喹啉-2(1H)-甲酰胺(5.3mg,产率13%)固体。
M001300:
1H NMR(400MHz,DMSO-d6)δ11.03(s,1H),7.73–7.70(m,2H),7.59(s,1H),7.55(s,1H),7.48(s,1H),7.12(s,1H),6.76(t,J=55.1Hz,1H),6.73(s,1H),6.69–6.63(m,1H),6.57–6.51(m,1H),6.21(s,1H),4.52(d,J=17.2Hz,2H),4.17(d,J=17.2Hz,2H),3.86(s,3H),3.69–3.54(m,2H),3.54–3.41(m,2H),3.04–2.82(m,4H),2.61(s,1H),2.56(d,J=4.4Hz,3H),2.10–2.00(m,4H).
实施例17
向1,4-二氧杂螺[4.5]癸-8-醇(10g,0.063mol),4-DMAP(0.77g,0.0063mol)和TEA(19g,0.19mol)的DCM(200mL)溶液中加入TsCl(18g,0.095mol)。将反应混合物在25℃下搅拌16小时。LCMS显示形成了所需的产物。减压除去溶剂。通过快速色谱法纯化残余物,用EtOAc在PE中从0%至30%洗脱,得到白色固体的1,4-二氧杂螺[4.5]癸-8-基4-甲基苯磺酸盐(10g,48%)。
向1,4-二氧杂螺[4.5]癸-8-基4-甲基苯磺酸盐(5.0g,0.02mol)的EtOH(50mL)溶液中加入甲硫酸钠(2.2g,0.032mol)。将反应混合物在80℃下搅拌30分钟。减压除去溶剂。将固体溶于水中并用EtOAc(200mL×2)萃取,将合并的有机层用Na2SO4干燥,过滤并减压浓缩。通过快速色谱法纯化残余物,用EA在PE中从0%至20%洗脱,得到8-(甲硫基)-1,4-二氧杂螺[4.5]癸烷(2.2g,55%),为黄色油状物。
向8-(甲基磺酰基)-1,4-二氧杂螺[4.5]癸烷(2.2g,5.9mmol)的H2O(5.0mL)溶液中加入PTSA(2.2g,11.6mmol)。将反应混合物在100℃下搅拌16小时。反应用EtOAc(200mL)萃取。将有机层用Na2SO4干燥,过滤并减压浓缩。通过快速色谱法纯化残余物,用EA在PE中从0%至20%洗脱,得到4-(甲硫基)环己烷-1-酮(1.2g,78%),为黄色油状物。
在-78℃下,向4-(甲硫基)环己烷-1-酮(1.2g,8.4mmol)的THF(15mL)溶液中加入LDA(4.5mL,2M的THF,9.0mmol)。将反应混合物在相同温度下搅拌1.0小时,然后加入1,1,1-三氟-N-苯基-N-((三氟甲基)磺酰基)甲磺酰胺(3.2g,9.0mmol)。将反应混合物在25℃下搅拌16小时。将反应混合物用NH 4Cl(aq)淬灭并用EA(200mL×2)萃取,将合并的有机层用Na2SO4干燥,过滤并减压浓缩。通过快速色谱法纯化残余物,用EA在PE中从0%洗脱至3%,得到4-(甲硫基)环己-1-烯-1-基三氟甲磺酸酯(0.8g,35%),为淡黄色油状物。
向4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)异吲哚啉-2-甲酸叔丁酯(1.0g,1.6mmol)和4-(甲硫基)环己-1-烯-1-基三氟甲磺酸叔丁酯(0.46g,1.6mmol)的二氧六环(20.0mL)和H2O(3mL)溶液中加入Xphos 1 Pd G3(0.13g,0.16mmol)和K2CO3(0.34g,2.5mmol)。将反应混合物在100℃下搅拌2.0小时。减压除去溶剂。残余物通过快速色谱纯化,用EtOAc在PE中从0%至60%洗脱,得到4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲硫基)环己-1-烯-1-基)异吲哚啉-2-甲酸叔丁酯(0.50g,50%),为浅黄色固体。
将4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲硫基)环己-1-烯-1-基)异吲哚啉-2-甲酸叔丁酯(0.50g,0.80mmol)在HCl(3.0ml,4M EA)中的溶液在25℃下搅拌30分钟。LCM显示目标产物形成。减压除去固体,得到白色固体的7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-1-(6-(4-(甲硫基)环己-1-烯-1-基)异吲哚-4-基)-1,2,3,4-四氢喹啉(0.46g,粗品)。
向7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-1-(6-(4-(甲硫基)环己-1-烯-1-基)异吲哚-4-基)-1,2,3,4-四氢喹啉(0.46g,0.92mmol)和TEA(0.28g,2.7mmol)的DCM(5.0mL)溶液中加入乙酰氯(0.14g,12.2mmol),将反应混合物在25℃下搅拌30分钟。用水淬灭反应并用DCM(100mL)萃取。将有机层用Na2SO4干燥,过滤并减压浓缩,得到白色固体的1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲硫基)环己-1-烯-1-基)异吲哚啉-2-基)乙-1-酮(0.42g, 86%)。
向1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲硫基)环己-1-烯-1-基)异吲哚-2-基)乙-1-酮(0.42g,0.77mmol)的MeOH(5.0mL)溶液中加入PtO2(0.42g)。将反应混合物在25℃下在H2气氛下搅拌48小时。滤出PtO2,减压除去溶剂,残余物通过预HPLC纯化(CH3CN在2分钟内从33%至43%),得到1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲硫基)环己基)异吲哚-2-基)乙烷-1-酮(0.1g,24%),为白色固体。
M001315:
1H NMR(400MHz,DMSO-d6)δ7.74(s,1H),7.49(s,1H),7.15–7.07(m,3H),6.87(s,0.25H),6.74(s,0.50H),6.60(s,0.25H),6.45–6.33(m,1H),4.90–4.50(m,3H),4.28(s,1H),3.86(s,3H),3.54(d,J=4.8Hz,2H),2.87(s,2H),2.64–2.53(m,2H),2.10–1.96(m,10H),1.87(d,J=11.6Hz,2H),1.60–1.47(m,2H),1.38(d,J=9.6Hz,2H).
向1-(4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-6-(4-(甲硫基)环己基)异吲哚-2-基)乙-1-酮(90mg,0.17mmol)和氨基甲酸铵(19mg,0.25mmol)的MeOH(3.0mL)溶液中加入PIDA(113mg,0.35mmol)。将反应混合物在0℃下搅拌30分钟。LCMS显示目标产物形成。用水淬灭反应并用EA(10mL×3)萃取,将合并的有机层用Na2SO4干燥,过滤并减压浓缩。通过预HPLC(CH3CN在3分钟内从20%至35%)纯化残余物,得到(4-(2-乙酰基-7-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)异吲哚-5-基)环己基)(亚氨基)(甲基)-l6-磺胺酮(16mg,17%),为浅黄色固体。
M001297:
1H NMR(400MHz,DMSO)δ7.74(s,1H),7.49(s,1H),7.13(d,J=6.0Hz,3H),6.88(s,0.25H),6.74(s,0.50H),6.61(s,0.25H),6.46–6.34(m,1H),4.95–4.55(m,3H),4.29(s,1H),3.86(s,3H),3.54(s,3H),2.98(s,1H),2.88(s,2H),2.83(d,J=4.0Hz,3H),2.58(s,1H),2.21(s,2H),2.05–1.90(m,7H),1.65–1.45(m,4H).
实施例18
向6-氯-8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(120mg,226.83μmol)的DCM(4mL)溶液中加入TFA(1.54g,13.51mmol)。将混合物在25℃下搅拌0.5小时。浓缩混合物,得到黄色固体形式的化合物2(120mg,221.02μmol,97.4%收率,TFA)。
向1-((8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-1,2,3,4-四氢异喹啉-6-基)甲基)哌啶-3-甲酸甲酯(50mg,75.34μmol,TFA)的DCM(3mL)溶液中加入TEA(22.87mg,226.01μmol)和甲氨基甲酰氯(17.61mg,188.34μmol)。将混合物在15℃下搅拌16小时。混合物用DCM(10mL)萃取并用盐水(5mL)洗涤,有机层用Na2SO4干燥,过滤并浓缩,得到化合物4(40mg,65.93μmol,87.5%收率),为黄色油状物。
6-氯-8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(0.7g,1.32mmol),乙烯三氟硼酸钾(265.86mg,1.98mmol),Pd2(dba)3(121.17mg,132.32μmol),s-Phos(108.64mg,264.64μmol)和t-BuONa(381.49mg,3.97mmol)的二氧六环(10mL)溶液脱气并用N2置换3次,然后将混合物在N2气氛下于100℃搅拌16小时。将混合物用EtOAc(20mL)萃取并用盐水(10mL)洗涤,将有机层用Na2SO4干燥,过滤并浓缩得到粗品,将其通过硅胶柱色谱法纯化(石油醚/乙酸乙酯从100%至70%),得到化合物6(593mg,1.14mmol,产率86.3%),为黄色油状物。
向8-(7-(二氟甲基)-6-(1-甲基-1H-吡咯-3-基)-3,4-二氢喹啉-1(2H)-基)-6-乙烯基-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(593mg,1.14mmol)的H2O(2mL)和THF(8mL)溶液中加入K2OsO4(21.71mg,114.12μmol),将混合物冷却至0℃,然后加入NaIO4(488.19mg,2.28mmol,126.47μL,2eq),然后加热至15℃并搅拌16小时。混合物用EtOAc(20mL)萃取并用盐水(10mL)洗涤,有机层用Na2SO4干燥,过滤并浓缩得到粗品,通过硅胶柱色谱法(石油醚/乙酸乙酯从100%至30%)纯化,得到化合物7(451mg,864.65μmol,75.8%收率),为黄色油状物。
向1-((8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-1,2,3,4-四氢异喹啉-6-基)甲基)哌啶-3-甲酸甲酯(50mg,75.34μmol,TFA)的DCM(3mL)溶液中加入TEA(22.87mg,226.01μmol)和甲氨基甲酰氯(17.61mg,188.34μmol)。将混合物在15℃下搅拌16小时。混合物用DCM(10mL)萃取并用盐水(5mL)洗涤,有机层用Na2SO4干燥,过滤并浓缩,得到化合物6(40mg,65.93μmol,87.5%收率,粗品),为黄色油状物。
向1-((8-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-2-(甲基氨基甲酰基)-1,2,3,4-四氢异喹啉-6-基)甲基)哌啶-3-甲酸甲酯(40mg,65.93μmol)的MeOH(2mL)和H2O(1mL)溶液中加入LiOH(4.74mg,197.79μmol)。将混合物在15℃下搅拌0.5小时。将混合物浓缩得到粗品,并通过prep-HPLC(FA)纯化,得到灰色固体M001015(3.25mg,5.48μmol,8.3%收率)。
M001015:
1H NMR(400MHz,CD3Cl)δ8.23(br s,1H),7.72(s,1H),7.47(s,1H),7.34-6.96(m,3H),6.88-6.09(m,1H),6.18(s,1H),4.56-4.07(m,3H),3.85(s,3H),3.01-2.63(m,8H),2.59-2.53(m,6H),2.42-2.28(m,2H),2.18-1.89(m,4H),1.83-1.51(m,2H),1.45-1.30(m,1H).
实施例19
将苯硼酸(19.38mg,158.92μmol),6-氯-4-(7-(二氟甲基)-6-(1-甲基-1H-吡唑-4-基)-3,4-二氢喹啉-1(2H)-基)-N-甲基异吲哚啉-2-甲酰胺(50mg,105.95μmol),XPhos Pd G3(8.97mg,10.59μmol)和K3PO4(67.47mg,317.84μmol)溶于THF(2mL)和H2O(0.5mL)后放入微波管中。将微波管在微波下在60℃加热1小时。将混合物用EtOAc(10mL)萃取并用盐水(5mL x 2)洗涤,将有机层用Na2SO4干燥,过滤并浓缩得到粗品,将其通过硅胶柱色谱法纯化(石油醚/乙酸乙酯从100%至0%),得到黄色固体M001120(3.66mg,7.13μmol,6.7%收率)。
M001120:
1H NMR(400MHz,DMSO-d6)δ7.75(s,1H),7.69(br d,J=7.70Hz,2H),7.56(s,1H),7.48-7.51(m,2H),7.44-7.47(m,1H),7.33-7.41(m,1H),7.14(s,1H),6.60-6.91(m,1H),6.29-6.46(m,2H),4.68(br s,2H),4.26-4.47(m,2H),3.85(s,3H),3.63(br s,1H),2.86-2.93(m,2H),2.55-2.63(m,4H),1.98-2.09(m,2H)
实施例20
向6-溴-7-(二氟甲基)-1,2,3,4-四氢喹啉(600mg,2.30mmol)和3-(甲氧基甲基)-1-甲基-4-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)吡唑(635mg,2.52mmol)的二氧六环(20mL)和H2O(2.0mL)溶液中加入K2CO3(949mg,6.87mmol)和Pd(dppf)Cl2(168mg,0.230mmol)。将反应混合物在100℃,N2下搅拌2小时。将混合物用水(50mL)淬灭,然后用乙酸乙酯(80mL x 2)萃取。合并的有机相用NaCl水溶液(10mL×2)洗涤,用Na2SO4干燥,过滤,减压浓缩。滤液在减压下浓缩。残余物通过硅胶色谱纯化,用EtOAc在石油中从0%至30%洗脱,得到7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-1,2,3,4-四氢喹啉(700mg,产率85%),为黄色油状物。
在25℃下,向7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-1,2,3,4-四氢喹啉(797mg,2.59mmol)和(6-氯-4-碘-1,3-二氢异吲哚-2-基)甲酸叔丁酯(1974mg,5.19mmol)的二氧六环(60mL)溶液中加入t-BuONa(748mg,7.78mmol)和XPhos Pd G3(219mg,0.259mmol)。将反应混合物在90℃下搅拌16小时。将混合物用水(50mL)淬灭,然后用乙酸乙酯(80mL×2)萃取。将合并的有机相用硫酸钠干燥并过滤。滤液在减压下浓缩。残余物通过硅胶色谱纯化,用THF在PE中从0%至25%洗脱,得到{6-氯-4-[7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-2-基}甲酸叔丁酯(1.01g,产率66%),为棕色固体。
向{6-氯-4-[7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-2-基}甲酸叔丁酯(200mg,0.357mmol)和2-(1-甲基苯氧基)-4-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)吡啶(167mg,0.536mmol)的THF/H2O=10:1(11mL)溶液中:在25℃下加入K3PO4(227mg,1.07mmol)和XPhos Pd G3(60.4mg,0.0714mmol)℃。将反应混合物在60℃,N2下搅拌2小时。将混合物用水(50mL)淬灭,然后用乙酸乙酯(80mL×2)萃取。将合并的有机相用硫酸钠干燥并过滤。滤液在减压下浓缩。残余物通过硅胶色谱纯化,用石油中的THF从0%至60%洗脱,得到{4-[7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-3,4-二氢-2H-喹啉-1-基]-6-[2-(1-甲基苯氧基)吡啶-4-基]-1,3-二氢异吲哚-2-基}甲酸叔丁酯(113mg,产率44%),为棕色固体。
在25℃下,向{4-[7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-3,4-二氢-2H-喹啉-1-基]-6-[2-(1-甲基苯氧基)吡啶-4-基]-1,3-二氢异吲哚-2-基}甲酸叔丁酯(113mg,0.159mmol)的DCM(6.0mL)溶液中加入TFA(2.0mL)。将反应混合物在25℃下搅拌0.5小时。将混合物减压浓缩,得到7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-1-{6-[2-(1-甲基苯氧基)吡啶-4-基]-2,3-二氢-1H-异吲哚-4-基}-3,4-二氢-2H-喹啉(120mg,产率92%),为棕色油状物,直接用于下一步,无需进一步纯化。
向7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-1-{6-[2-(1-甲基苯氧基)吡啶-4-基]-2,3-二氢-1H-异吲哚-4-基}-3,4-二氢-2H-喹啉(97.0mg,0.159mmol)的DCM(5.0mL)溶液中加入TEA(48.4mg,0.478mmol)和乙酰氯(18.8mg,0.239mmol)。将反应混合物在25℃下搅拌10分钟。将混合物用水(20mL)淬灭,然后用乙酸乙酯(50mL×2)萃取。将合并的有机相用硫酸钠干燥并过滤。滤液在减压下浓缩。残余物通过硅胶色谱纯化,用甲醇在DCM中从0%至5%洗脱,得到1-{4-[7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-3,4-二氢-2H-喹啉-1-基]-6-[2-(1-甲基苯氧基)吡啶-4-基]-1,3-二氢异吲哚-2-基}乙酮(71.0mg,产率62%),为黄色固体。
向1-{4-[7-(二氟甲基)-6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-3,4-二氢-2H-喹啉-1-基]-6-[2-(1-甲基苯氧基)吡啶-4-基]-1,3-二氢异吲哚-2-基}乙烯(99.0mg,0.155mmol)的MEOH(8.0mL)溶液中加入PtO2(34.5mg,0.152mmol)。将混合物在25℃,H2气球压力下搅拌16小时。过滤混合物以除去固体并浓缩。残余物通过Prep-HPLC纯化(CH3CN在10分钟内从40%至70%),得到4-{2-乙酰基-7-[7-(二氟甲基)- 6-[3-(甲氧基甲基)-1-甲基吡唑-4-基]-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-5-基}哌啶-2-酮(15.1mg,产率18%),为白色固体。
M001206:
1H NMR(400MHz,DMSO-d6)δ7.63–7.52(m,2H),7.25–7.14(m,2H),7.09–7.03(m,1H),6.65(d,J=55.4Hz,1H),6.45–6.35(m,1H),4.90–4.84(m,1H),4.74–4.50(m,2H),4.37–4.27(m,1H),4.18(s,2H),3.84(s,3H),3.62–3.54(m,2H),3.22–3.17(m,4H),3.14–3.02(m,2H),2.90–2.84(m,2H),2.37–2.30(m,2H),2.05–1.87(m,7H).
实施例21
向7-溴-1,2,3,4-四氢喹啉(2.0g,0.0094mol)和环丙基硼炔二醇(1.6g,0.019mol)的甲苯/水(11ml)溶液中加入K3PO4(6.0g,0.028mol),三环己基膦(0.3g,0.0009mol)和Pd(OAc)2(0.2g,0.0009mol)。将混合物在100℃下搅拌5小时。将混合物减压浓缩。通过硅胶色谱法纯化残余物,用EtOAc/石油醚洗脱,
EtOAc在15分钟内从0%洗脱至20%,得到7-环丙基-1,2,3,4-四氢喹啉(1.2g,产率66%),为黄色胶状物。
在0℃下,向7-环丙基-1,2,3,4-四氢喹啉(1.1g,0.0062mol)的ACN(20ml)溶液中加入N-溴代琥珀酰亚胺(1.2g,0.0065mol)。将混合物在25℃下搅拌1小时。将混合物减压浓缩。通过硅胶色谱纯化残余物,用EtOAc/石油醚洗脱,EtOAc在20分钟内从0%洗脱至30%,得到6-溴-7-环丙基-1,2,3,4-四氢喹啉(1.3g,74%收率),为黄色液体。
向6-溴-7-环丙基-1,2,3,4-四氢喹啉(0.9g,0.0054mol)和1-甲基-4-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)吡唑(1.1g,0.0054mmol)的二氧六环/水(22mL)溶液中加入K2CO3(1.5g,0.011mol)和Pd(dppf)Cl2(0.3g,0.0003mmol)。将混合物在90℃下搅拌5小时。将混合物减压浓缩。通过硅胶色谱纯化残余物,用EtOAc/石油醚洗脱,EtOAc在20分钟内从0%洗脱至50%,得到7-环丙基-6-(1-甲基吡唑-4-基)-1,2,3,4-四氢喹啉(0.7g,产率64%),为黄色胶状物。
向7-环丙基-6-(1-甲基吡唑-4-基)-1,2,3,4-四氢喹啉(300mg,3.2mmol)和(6-氯-4-碘-1,3-二氢异吲哚-2-基)甲酸叔丁酯(1322mg,3.5mmol)的二氧六环(30ml)溶液中加入Cphos-Pd G3(509mg,0.63mmol)和t-BuONa(607mg,6.3mmol)。将混合物在90℃下搅拌2小时。将混合物减压浓缩。残余物通过硅胶色谱法纯化,用EtOAc/石油醚洗脱,EtOAc在15分钟内从0%洗脱至50%,得到{6-氯-4-[7-环丙基-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-2-基}甲酸叔丁酯(400mg,产率23%),为黄色胶状物。
向{6-氯-4-[7-环丙基-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-2-基}甲酸叔丁酯(200mg,0.40mmol)和2-(1-甲基苯氧基)-4-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)吡啶(247mg,0.79mmol)的二氧六环/水(11ml)溶液中加入K2CO3(252mg,1.2mmol)和X-Phos Pd G3(67mg,0.079mmol)。将混合物在90℃下搅拌2小时。将混合物减压浓缩。残余物通过硅胶色谱纯化,用EtOAc/石油醚洗脱,EtOAc在15分钟内从0%洗脱至50%,得到{4-[7-环丙基-6-(1-甲基吡唑-4-基)-3,4- 二氢-2H-喹啉-1-基]-6-[2-(1-甲基苯氧基)吡啶-4-基]-1,3-二氢异吲哚-2-基}甲酸叔丁酯(100mg,产率35%),为黄色胶状物。
将{4-[7-环丙基-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-[2-(1-甲基苯氧基)吡啶-4-基]-1,3-二氢异吲哚-2-基}甲酸叔丁酯(100mg,0.15mmol)的DCM/TFA(6ml)中的混合物在25℃下搅拌0.1小时。将混合物减压浓缩,得到7-环丙基-1-{6-[2-(1-甲基苯氧基)吡啶-4-基]-2,3-二氢-1H-异吲哚-4-基}-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉(80mg,产率85%),为黄色胶状物。
向7-环丙基-1-{6-[2-(1-甲基苯氧基)吡啶-4-基]-2,3-二氢-1H-异吲哚-4-基}-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉(80mg,0.14mmol)和TEA(44mg,0.43mmol)的DCM(10ml)溶液中加入乙酰氯(23mg,0.29mmol)。将混合物在25℃下搅拌0.1小时,将混合物减压浓缩。残余物通过硅胶色谱纯化,用EtOAc/石油醚洗脱,EtOAc在10分钟内从0%洗脱至50%,得到1-{4-[7-环丙基-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-[2-(1-甲基苯氧基)吡啶-4-基]-1,3-二氢异吲哚-2-基}乙烯酮(70mg,产率73%),为黄色胶状物。
向1-{4-[7-环丙基-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-6-[2-(1-甲基苯氧基)吡啶-4-基]-1,3-二氢异吲哚-2-基}乙烯(70mg,0.12mmol)的MeOH(5ml)溶液中加入PtO2(27mg,0.12mmol)。将混合物在25℃下搅拌16小时。将混合物过滤并减压浓缩。通过预HPLC纯化残余物,用含有40%至50%CH3CN的水中的CH3CN在10分钟内洗脱,得到白色固体的4-{2-乙酰基-7-[7-环丙基-6-(1-甲基吡唑-4-基)-3,4-二氢-2H-喹啉-1-基]-1,3-二氢异吲哚-5-基}哌啶-2-酮(30mg,产率49%)。
M001219:
1H NMR(400MHz,DMSO-d6)δ7.84(s,1H),7.60(s,1H),7.56(s,1H),7.14-7.01(m,2H),7.02(s,1H),5.88-5.82(m,,1H),4.85(s,1H),4.64(s,1H),4.59(s,1H),4.26(s,1H),3.85(s,3H),3.49(d,J=5.2Hz,2H),3.20(s,2H),3.07(s,1H),2.79-2.78(m,2H),2.36–2.29(m,2H),2.04(d,J=5.2Hz,1H),2.00–1.92(m,4H),1.87-1.84(m,3H),0.77–0.69(m,2H),0.21–0.13(m,2H).
实施例22
向搅拌的2-溴-4-氟苯甲醛(5.0g,0.024mol)的H2SO4(30.0mL)溶液中,在0℃下加入硝酸(1.71g,0.027mol)。将反应混合物加热至25℃并在该温度下搅拌2小时。将反应混合物用水(200mL)淬灭,然 后用EtOAc(50mL×2)萃取。将合并的有机相用Na2SO4干燥,然后过滤。将滤液减压浓缩,得到黄色固体的2-溴-4-氟-5-硝基苯甲醛(5.6g,产率78%)。
在0℃下,向2-溴-4-氟-5-硝基苯甲醛(1.5g,0.006mol)的DCM(20.0mL)搅拌溶液中加入DAST(1.93g,0.012mol)。将反应混合物加热至25℃并在该温度下搅拌12小时。将反应混合物用水(200mL)淬灭,然后用EtOAc(50mL×2)萃取。将合并的有机相用Na2SO4干燥,过滤并浓缩。通过硅胶色谱法纯化残余物,在10分钟内用EtOAc/PE(EtOAc从0%到5%)洗脱,得到1-溴-2-(二氟甲基)-5-氟-4-硝基苯(1.4g,78%收率),为黄色固体。
向1-溴-2-(二氟甲基)-5-氟-4-硝基苯甲酸酯(1.4g,0.005mol)的EtOH(20.0mL)和H2O(5.0mL)溶液中加入Fe(1.45g,0.026mol)和NH4Cl(2.78g,0.052mol)。将反应溶液加热至90℃并在该温度下搅拌2小时。将混合物冷却至25℃并过滤以除去固体并浓缩。通过硅胶色谱法纯化残余物,在10分钟内用EtOAc/PE(EtOAc从0%到5%)洗脱,得到4-溴-5-(二氟甲基)-2-氟苯胺(0.85g,62%收率),为白色固体。
向4-溴-5-(二氟甲基)-2-氟苯胺(850mg,3.54mmol)的1,4-二氧六环(15.0mL)和H2O(2.0mL)溶液中加入1-甲基-4-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)吡唑(884mg,4.24mmol),K2CO3(979mg,7.08mmol)和Pd(dppf)Cl2(259mg,0.354mmol)。将反应溶液加热至100℃并在该温度下在N2下搅拌10小时。将混合物冷却至25℃并减压浓缩。残余物通过硅胶色谱纯化,用EtOAc/PE(EtOAc从0%到20%)在10分钟内洗脱,得到5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯胺(790mg,产率88%),为白色固体。
向5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯胺(500mg,2.07mmol)的1,4-二氧六环(10.0mL)溶液中加入8-溴-6-氯-3,4-二氢-1H-异喹啉-2-甲酸叔丁酯(719mg,2.07mmol),t-BuONa(398mg,4.14mmol)和Cphos-Pd G3(167mg,0.207mmol)。将反应溶液加热至90℃并在该温度下在N2下搅拌12小时。将混合物冷却至25℃并减压浓缩。残余物通过硅胶色谱纯化,用MeOH/DCM(MeOH从0到10%)在10分钟内洗脱,得到6-氯-8-((5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯基)氨基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(780mg,产率45%),为黄色固体。
向6-氯-8-(5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯基)氨基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(150mg,0.295mmol)的THF(6.0mL)和H2O(1.0mL)溶液中加入1-甲基-5-(4,4,5,5-四甲基-1,3,2-二氧杂硼杂环戊烷-2-基)吡啶-2-酮(139mg,0.591mmol),K3PO4(188mg,0.887mmol)和XPhos Pd G3(25.0mg,0.029mmol)。将反应溶液加热至80℃并在该温度下在N2下搅拌12小时。将混合物冷却至25℃并减压浓缩。残余物通过硅胶色谱纯化,用MeOH/DCM(MeOH从0到10%)洗脱10分钟,得到8-((5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯基)氨基)-6-(1-甲基-6-氧代-1,6-二氢吡啶-3-基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(150mg,产率83%),为黄色固体。
向8-((5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯基)氨基)-6-(1-甲基-6-氧代-1,6-二氢吡啶-3-基)-3,4-二氢异喹啉-2(1H)-甲酸叔丁酯(150mg,0.258mmol)的DCM(5.0mL)溶液中加入TFA(1.0mL)。将溶液在25℃下搅拌1小时。将混合物减压浓缩至5-(8-((5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯基)氨基)-1,2,3,4-四氢异喹啉-6-基)-1-甲基吡啶-2(1H)-酮(110mg,产率84%),为黄色油状物。
向5-(8-((5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯基)氨基)-1,2,3,4-四氢异喹啉-6-基)-1-甲基吡啶-2(1H)-酮(110mg,0.229mmol)的DCM(5.0mL)溶液中加入Et3N(70.0mg,0.688mmol)和N-甲基氨基甲酰氯(64.0mg,0.688mmol)。将反应溶液在25℃下搅拌1小时。将混合物减压浓缩。通过Prep-HPLC(在8分钟内将CH3CN从25%纯化至55%)纯化残余物,得到白色固体c(80.0mg,产率65%)。
M001239:
1H NMR(400MHz,DMSO-d6)δ8.03(d,J=2.0Hz,1H),7.87(s,1H),7.71–7.68(m,1H),7.61(d,J=8.0Hz,2H),7.34(d,J=12.0Hz,1H),7.14(d,J=8.0Hz,2H),7.06–6.75(m,2H),6.48–6.43(m,2H),4.43(s,2H),3.88(s,3H),3.55–3.52(m,2H),3.47(s,3H),2.84(s,2H),2.59(d,J=4.0Hz,3H).
向8-((5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯基)氨基)-N-甲基-6-(1-甲基-6-氧代-1,6-二氢吡啶-3-基)-3,4-二氢异喹啉-2(1H)-甲酰胺(70mg,0.130mmol)的MeOH(6.0mL)溶液中加入PtO2(30.0mg,0.130mmol)。将溶液在25℃,H2下搅拌12小时。过滤混合物以除去固体并浓缩。通过Prep-HPLC(CH3CN在9分钟内从25%至55%)纯化残余物,得到8-((5-(二氟甲基)-2-氟-4-(1-甲基-1H-吡唑-4-基)苯基)氨基)-N-甲基-6-(1-甲基-6-氧代哌啶-3-基)-3,4-二氢异喹啉-2(1H)-甲酰胺 (42.5mg,50%收率),为白色固体。
M001232:
1H NMR(400MHz,DMSO-d6)δ7.87(s,1H),7.62(s,1H),7.50(s,1H),7.34(d,J=12.0Hz,1H),7.15(d,J=8.0Hz,1H),7.05–6.76(m,3H),6.49–6.41(m,1H),4.39(s,2H),3.89(s,3H),3.52–3.49(m,2H),3.32–3.24(m,2H),3.05–2.99(m,1H),2.79–2.76(m,5H),2.59(d,J=4.0Hz,3H),2.36–2.22(m,2H),1.97–1.82(m,2H).
















































生物活性实施例1
将22RV1或vCap细胞培养于RPMI-1640培养基(RPMI-1640中加入10%胎牛血清,每mL100单位青/链 霉素双抗),置于37℃,5%CO2的细胞培养箱。将对数生长期的细胞以5x103细胞/100μL/孔接种于96孔细胞培养板,培养过夜。加入不同浓度的溶于DMSO的活性化合物,终浓度为0.5%DMSO,阳性对照为1%TweeN20,阴性对照为0.5%DMSO。培养72h后,每孔加入等体积CellTiter-Glo,震荡混匀2min,室温静置10min,用酶标仪读取荧光信号值。使用Prism 7.0分析数据并生成图形。所示值为平均值±SEM(N=2)。阴性对照组为0%抑制组(0%Inhibition),阳性对照组为100%抑制组(100%Inhibition)。抑制率计算公式如下:%抑制率=(Icompound-IZPE)/(IHPE-IZPE)×100;Icompound为化合物组信号值;IHPE为100%抑制组信号值;IZPE为阴性对照信号值。X轴为化合物浓度(μM),Y轴为%Inhibition。
注:A<1μM,1μM<B





EP300调节剂生化活性测试采用Ep300检测试剂盒检测。该测定原理是基于乙酰基从乙酰辅酶A到特定赖氨酸的酶促转移生物素化肽底物中的残基。将化合物与EP300孵育后,再与特异性结合乙酰化肽的抗体和结合乙酰化肽的受体珠的组合抗体孵育,随后与链霉亲和素标记的供体珠孵育读取Alpha计数并使用Prism 7.0分析数据并计算IC50,所示值为平均值±SEM(N=2)。
CBP制剂生化活性测试采用CBP检测试剂盒检测。该检测原理是基于CBP溴结构域与乙酰化组蛋白底物的结合。将化合物与CBP和生物素化的底物一起孵育30min,随后添加受体珠子孵育15min再添加供体珠子孵育15min后读取Alpha计数并使用Prism 7.0分析数据并计算IC50,所示值为平均值±SEM(N=2)。
A<10nM,B>10nM
以上对本公开技术方案的实施方式进行了示例性的说明。应当理解,本公开的保护范围不拘囿于上述实施方式。凡在本公开的精神和原则之内,本领域技术人员所做的任何修改、等同替换、改进等,均应包含在权利要求书的保护范围之内。

Claims (11)

  1. 一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐:
    其中:
    n=0,1,2;
    m=0,1,2,3;
    p=0,1,2,3,4,5;
    q=0,1,2;
    X1,X2,X3,X4彼此独立地选自C或N;
    每个R1相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R1a所取代的如下基团:C1-12烷基,C1-12烷氧基,-(C=O)R;
    所述R选自C1-12烷基,C1-12烷氧基,NH2-,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C3-12环烷基;
    每个R1a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基;
    每个R2相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1-12烷氧基;
    R2’选自H、卤素、CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R2a所取代的如下基团:C6-14芳基,5-14元杂芳基,3-14元杂环基,C3-12环烷基,C1-12烷基;
    每个R2a相同或不同,彼此独立地选自H、氧代(=O),卤素,COOH,OH,无取代或任选被1个、2个或更多个R2b所取代的如下基团:NH2,C1-12烷基,C1-12烷氧基,C1-12烷基硫基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基,C6-14芳基、5-14元杂芳基、3-14元杂环基、C3-12环烷基,C6-14芳基C(=O)-、5-14元杂芳基C(=O)-、3-14元杂环基C(=O)-、C3-12环烷基C(=O)-,C1-12烷基S(=O)2-、C1-12烷基S(=O)-、C1-12烷基S(=O)(=NH)-、C3-12环烷基S(=O)2-、C1-12烷基-C(=O)-NH-、C1-12烷基-S(=O)2-NH-;
    每个R2b相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,;
    R3选自H、卤素、CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R3a所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基-NHC(=O),N,N-二C1-12烷基氨基羰基,C6-14芳基,5-14元杂芳基,3-14元杂环基,C3-12环烷基;
    每个R3a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R3b所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
    每个R3b相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基;
    R4选自H、卤素、CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R4a所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基-NHC(=O),N,N-二C1-12烷基氨基羰基,C6-14芳基,5-14元杂芳基,3-14元杂环基,C3-12环烷基;
    每个R4a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R4b所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
    每个R4b相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基;
    每个R5相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R5a所取代的如下基团:C1-12烷基,C1-12烷氧基;
    每个R5a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基;
    R6选自H、卤素、CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R6a所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基-NHC(=O),N,N-二C1-12烷基氨基羰基;
    每个R6a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
    R7选自H、卤素、CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个R7a所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基-NHC(=O),N,N-二C1-12烷基氨基羰基;
    每个R7a相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
    或R6与R7一起形成无取代或任选被1个、2个或更多个Rsa所取代的如下基团:5-14元杂芳基,3-14元杂环基;所述5-14元杂芳基,3-14元杂环基至少含有一个N原子;
    每个Rsa相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,无取代或任选被1个、2个或更多个Rsb所取代的如下基团:C1-12烷基,C1-12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基,C1-12烷基C(=O)-,C1-12烷氧基C(=O)-,C1-12烷基-NHC(=O)-,N,N-二C1-12烷基氨基羰基;
    每个Rsb相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-12烷基,C1- 12烷氧基,C1-12烷基-NH-,N,N-二C1-12烷基氨基。
  2. 根据权利要求1所述的一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐,其特征在于,所述式I中,部分选自如下结构:
  3. 根据权利要求1或2所述的一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐,其特征在于,每个R1相同或不同,彼此独立地选自氧代(=O),C1-6烷基,C1-6烷氧基,-(C=O)R;所述R选自C1- 6烷基,C1-6烷氧基,NH2-,C1-6烷基-NH-,C3-6环烷基。
  4. 根据权利要求1-3任一项所述的一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐,其特征在于,R2’选自H、Cl、无取代或任选被1个、2个或更多个R2a所取代的C6-10芳基,5-9元杂芳基,3-12元杂环基,C3-8环烷基、C1-3烷基;所述杂环基含有1-4个选自N,O,S的杂原子;
    优选的,R2’选自H、Cl、无取代或任选被1个、2个或更多个R2a所取代的如下结构:

    更优选的,R2’选自如下结构:
    优选地,R2a选自H,卤素(如F),甲基,乙基,氧代(=O),甲氧基,OH,COOH,CH3C(=O)-,-CH2CHF2,-CH2CF3,-Cbz,-Boc,氨基,甲氨基,二甲氨基,甲硫基, -CH2CN,
  5. 根据权利要求1-4任一项所述的一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐,其特征在于,
    R3选自H、无取代或任选被1个、2个或更多个R3a所取代的如下基团:C1-6烷基,C1-6烷氧基,C3-8环烷基;每个R3a相同或不同,彼此独立地选自卤素,CN,NH2,COOH,OH;
    R4选自无取代或任选被1个、2个或更多个R4a所取代的5-6元杂芳基(例如吡唑基);每个R4a相同或不同,彼此独立地选自无取代或任选被1个、2个或更多个R4b所取代的如下基团:C1-6烷基,C1-6烷氧基,N,N-二C1-6烷基氨基羰基;每个R4b相同或不同,彼此独立地选自氧代(=O),卤素,CN,NH2,COOH,OH,C1-6烷基,C1-6烷氧基;
    优选的,R4选自
    每个R5相同或不同,彼此独立地选自H,卤素,C1-6烷基,C1-6烷氧基;
    优选的,R6选自H,卤素,C1-6烷基,C1-6烷氧基;优选地,R6选自H;
    优选的,R7选自H,卤素,C1-6烷基,C1-6烷氧基;优选地,R7选自F;
    更优选的,R6与R7一起形成无取代或任选被1个、2个或更多个Rsa所取代的如下基团:5-6元杂芳基,5-6元杂环基;
    最优选的,R6与R7一起形成无取代或任选被1个、2个或更多个Rsa所取代的如下结构:
  6. 根据权利要求1-5任一项所述的一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐,其特征在于,所述式I进一步选自如下式I-1所示结构:
    其中,X1,X2,X3,X4,R1,R2,R2’,R3,R4,R5,R6,R7,R,n,m,p、q如权利要求1-5任一项所定义;
    R1’具有R1所述的定义;
    优选地,R1’选自氧代(=O),C1-6烷基,C1-6烷氧基,-(C=O)R;所述R选自C1-6烷基,C1-6烷氧基,NH2-,C1-6烷基-NH-,C3-6环烷基;
    优选地,R1’选自H、CH3,-C(=O)CH3,-C(=O)OCH3,-C(=O)OCH2CH3,-C(=O)OCH(CH3)3,CH3NHC(=O)-,CH3CH2NHC(=O)-,NH2C(=O)-,环丙基-C(=O)-;
    优选地,R1’为-(C=O)CH3
    优选地,所述式I进一步选自如下式II、式III、式IV所示结构:
    所述式II、式III、式IV中,X1,X2,X3,X4,R1,R2,R2’,R3,R4,R5,R6,R7,R,n,m,p,q如权利要求1-5任一项所定义;
    优选的,所述式I进一步选自如下式IIa、式IIIa所示结构:
    所述式IIa、式IIIa,X1,X2,X3,X4,R1,R2,R2’,R3,R4,R5,R,n,m,p,q如式(I)中化合物所定义。
  7. 根据权利要求1-6任一项所述的一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐,其特征在于,式(I)所示化合物的示例性的具体化合物如下:















  8. 一种药物组合物,其特征在于,所述药物组合物包括权利要求1-7任一项所述的一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐。
  9. 根据权利要求8所述的药物组合物,其特征在于,所述药物组合物包含第二治疗剂,所述第二治疗剂可选自常规用于治疗癌症,心脏病、代谢疾病、炎症疾病、纤维病变疾病及病毒感染的药物;优选的,所述第二治疗剂的类别可以包括雄激素受体拮抗剂,例如恩杂鲁胺,和CYP17A1的抑制剂(17α-羟化酶/C17,20裂合酶),例如阿比特龙;细胞毒性化疗剂,例如多西他赛;用于治疗肺癌的治疗剂类别包括细胞毒素化疗剂,例如顺铂、卡铂、多西他赛;用于治疗膀胱癌的治疗剂类别包括细胞毒素化疗剂,例如吉西他滨、顺铂或免疫疗法,例如卡介苗(BCG);所述第二治疗剂的类别还可以选自免疫检查点抑制剂,例如pembrolizumab,nivolumab,阿特珠单抗,伊匹木单抗;PARP(聚ADP核糖聚合酶)抑制剂比如奥拉帕尼;和CDK4/6(细胞周期蛋白-依赖性激酶4和6)抑制剂;优选的,所述第二治疗剂可以选自与KRAS抑制剂等联合用药。
  10. 根据权利要求1-7任一项所述的一种式I所示的化合物及其消旋体、立体异构体、互变异构体、同位素衍生物、氮氧化物、溶剂化物、多晶型物、代谢产物、酯、前药或其药学上可接受的盐或根据权利要求8-9任一项所述的药物组合物在制备预防和/或治疗CBP和/或EP300介导的疾病或病症的药物中的用途。
  11. 根据权利要求10所述的用途,其特征在于,所述CBP和/或EP300介导的疾病或病症选自癌症,心脏病、代谢疾病、炎症疾病、纤维病变疾病及病毒感染;所述癌症包括但不限于前列腺癌,乳腺癌,膀胱癌,肺癌,黑色素瘤、结直肠癌、胃癌、卵巢癌、宫颈癌、膀胱癌、喉癌、多发性骨髓瘤、肝癌、淋巴瘤和白血病等;前列腺癌可以是例如对阉割有抗性的前列腺癌(CRPC);肺癌可以是例如非小细胞肺癌或小细胞肺癌;所述淋巴瘤可选自非霍奇金淋巴瘤、漫大B细胞淋巴瘤等。
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