Important Compound Classes
Title
Substituted 6,7-Dihydro-5H-Benzo[7]annulene Compounds and Their Derivatives, Process for Their Preparation and Therapeutic Uses Thereof
Patent Publication Number
WO 2022/084280 A1
Publication Date
April 28, 2022
Priority Applications
EP 20306236.9 and EP 21306281.3
Priority Dates
October 19, 2020, and September 16, 2021
Inventors
Bernardelli, P.; Bianciotto, M.; Certal, V.; Da Rocha, A.; De Bruin, B.; El Ahmad, Y.; Halley, F.; Mougenot, P.; Nicolai, E.; Periers, A.-M.; Petit, F.; Slowinski, F.; Terrier, C.
Assignee Company
SANOFI, France
Disease Area
Cancer
Biological Target
Estrogen receptors
Summary
The estrogen receptors (ERs) belong to the steroid/nuclear receptor superfamily involved in the regulation of eukaryotic gene expression, cellular proliferation, and differentiation in target tissues. ERs are in two forms, the estrogen receptor alpha (ERα) and the estrogen receptor beta (ERβ), respectively encoded by the ESR1 and ESR2 genes. ERα and ERβ are ligand-activated transcription factors which are activated by the hormone estrogen.
ERα is mainly expressed in reproductive tissues such as uterine, ovarian, breast, bone, and white adipose tissue. Abnormal ERα leads to cancer, metabolic, cardiovascular, and neurodegenerative diseases. ERα is expressed in 50–80% of breast tumors. The etiological role of estrogen in breast cancer is well established, and modulation of ERα signaling remains the mainstay of breast cancer treatment. Although endocrine therapies have contributed enormously to reduction in breast cancer development, endocrine therapies display resistance. One of the new strategies to counterforce such resistance is to shut down the ERα signaling by removing ERα from the tumor cells using Selective Estrogen Receptor Degraders (SERDs).
The present application describes a series of novel substituted 6,7-dihydro-5H-benzo[7]annulene compounds as SERDs for the treatment of cancer. Further, the application discloses compounds, their preparation, use, and pharmaceutical composition, and treatment.
Definitions
R1 and R2 = H or D; R3 = H, COOH, or OH;
R3′ and R3″ = H, CH3, OCH3, Cl, F, or CN;
R4 and R5 = H, F, NH2, (C1–C3)alkyl, (C1–C3)alkoxy, or OH;
R6 = phenyl group, wherein phenyl group is optionally substituted by 1–3 substituents selected from halogen or (C1–C6)alkyl, and optionally substituted with CN or OH; (C1–C6)fluoroalkyl, (C3–C6)cycloalkyl, (C1–C6)alkoxy, (C1–C6)fluoroalkoxy, trifluoromethylsulfonyl, (C1–C4)alkylthio, (C1–C4)fluoroalkylthio, (C1–C4)alkylsulfonyl, or OH;
R8 = (C1–C3)alkyl, halogen, CN, (C1–C3)fluoroalkyl;
R7 = H, CH3, OH, or F; R9 = H or F; R10 and R10′ = H or F;
R11 = H or (C1–C3)alkyl; X = CH2, O, or S;
Y = −CH=, −N=, or −CR″=, where R″ = (C1–C3)alkyl, halogen, CN, or (C1–C3)fluoroalkyl; m = 0 or 1; and n = 0, 1, or 2.
Key Structures
Biological Assay
In vitro estrogen receptor degradation activity using a breast cancer cell ERα in cell western assay was performed. The compounds described in this application were tested for their ability to degrade estrogen receptor. The estrogen receptor degradation IC50 (nM) are shown in the table below.
Biological Data
The following table shows representative
compounds tested for estrogen receptor degradation and the biological
data obtained from testing representative examples.
Claims
Total claims: 33
Compound claims: 29
Pharmaceutical composition claims: 1
Method of preparation claims: 2
Medicament claims: 1
The author declares no competing financial interest.
Special Issue
Published as part of the ACS Medicinal Chemistry Letters virtual special issue “New Drug Modalities in Medicinal Chemistry, Pharmacology, and Translational Science”.
References
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