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Therapeutic targeting of CDK12: a medicinal chemistry perspective.

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Bioorganic & medicinal chemistry 📖 저널 OA 5.3% 2024: 0/3 OA 2025: 0/27 OA 2026: 4/43 OA 2024~2026 2026 Vol.135() p. 118552 Cancer-related Molecular Pathways
TL;DR A detailed review of various types of CDK12 small-molecule inhibitors/degraders is provided, primarily based on key structural frameworks, aiming to offer a comprehensive perspective for developing highly selective CDK12-targeted inhibitors/degraders and providing valuable insights for future novel drug development.
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PubMed DOI OpenAlex Semantic 마지막 보강 2026-05-01
OpenAlex 토픽 · Cancer-related Molecular Pathways Advanced Breast Cancer Therapies Epigenetics and DNA Methylation

Wang F, Dai H, Wan K, Wang M

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A detailed review of various types of CDK12 small-molecule inhibitors/degraders is provided, primarily based on key structural frameworks, aiming to offer a comprehensive perspective for developing hi

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APA Feifei Wang, Hongxue Dai, et al. (2026). Therapeutic targeting of CDK12: a medicinal chemistry perspective.. Bioorganic & medicinal chemistry, 135, 118552. https://doi.org/10.1016/j.bmc.2026.118552
MLA Feifei Wang, et al.. "Therapeutic targeting of CDK12: a medicinal chemistry perspective.." Bioorganic & medicinal chemistry, vol. 135, 2026, pp. 118552.
PMID 41544426 ↗

Abstract

CDK12 (Cyclin-dependent kinase 12) is a cyclin-dependent kinase that regulates gene transcription by phosphorylating the C-terminal domain of RNA polymerase II, playing a crucial role in maintaining genomic stability. Mutations or alterations in the CDK12 genome can trigger tumorigenesis and progression. Inhibiting the overexpression of CDK12 suppresses tumor growth and proliferation, indicating that it serves both as a biomarker for tumorigenesis and a potential therapeutic target for cancer treatment. In recent years, the structure and biological functions of CDK12 have been progressively elucidated, attracting significant research attention. Currently, the CDK12/13 inhibitor CT7439 is undergoing Phase I/II clinical trials. This paper provides a detailed review of various types of CDK12 small-molecule inhibitors/degraders, primarily based on key structural frameworks. It focuses on exploring the existing structure-activity relationships, aiming to offer a comprehensive perspective for developing highly selective CDK12-targeted inhibitors/degraders and providing valuable insights for future novel drug development.

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