Cyclin-dependent kinases in cancer: Role, regulation, and therapeutic targeting

细胞周期蛋白依赖激酶 细胞周期 癌症研究 帕博西利布 激酶 生物 细胞周期蛋白 癌变 细胞生物学 癌症 遗传学 乳腺癌 转移性乳腺癌
作者
Ashna Gupta,Gunjan Dagar,R. P. S. Chauhan,Hana Q. Sadida,Sara K. Almarzooqi,Sheema Hashem,Shahab Uddin,Muzafar A. Macha,Ammira S. Al-Shabeeb Akil,Tej K. Pandita,Ajaz A. Bhat,Mayank Singh
出处
期刊:Advances in protein chemistry and structural biology 卷期号:: 21-55 被引量:3
标识
DOI:10.1016/bs.apcsb.2023.02.001
摘要

Regulated cell division is one of the fundamental phenomena which is the basis of all life on earth. Even a single base pair mutation in DNA leads to the production of the dysregulated protein that can have catastrophic consequences. Cell division is tightly controlled and orchestrated by proteins called cyclins and cyclin-dependent kinase (CDKs), which serve as licensing factors during different phases of cell division. Dysregulated cell division is one of the most important hallmarks of cancer and is commonly associated with a mutation in cyclins and CDKs along with tumor suppressor proteins. Therefore, targeting the component of the cell cycle which leads to these characteristics would be an effective strategy for treating cancers. Specifically, Cyclin-dependent kinases (CDKs) involved in cell cycle regulation have been identified to be overexpressed in many cancers. Many studies indicate that oncogenesis occurs in cancerous cells by the overactivity of different CDKs, which impact cell cycle progression and checkpoint dysregulation which is responsible for development of tumor. The development of CDK inhibitors has emerged as a promising and novel approach for cancer treatment in both solid and hematological malignancies. Some of the novel CDK inhibitors have shown remarkable results in clinical trials, such as-Ribociclib®, Palbociclib® and Abemaciclib®, which are CDK4/6 inhibitors and have received FDA approval for the treatment of breast cancer. In this chapter, we discuss the molecular mechanism through which cyclins and CDKs regulate cell cycle progression and the emergence of cyclins and CDKs as rational targets in cancer. We also discuss recent advances in developing CDK inhibitors, which have emerged as a novel class of inhibitors, and their associated toxicities in recent years.
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