Discovery and Enzyme Kinetic Characterization of Novel CYP2D6 Variants

IF 3.7 3区 医学 Q2 CHEMISTRY, MEDICINAL Chemical Research in Toxicology Pub Date : 2024-10-21 DOI:10.1021/acs.chemrestox.4c0029810.1021/acs.chemrestox.4c00298
Yun-shan Zhong, Qi-hui Kong, Jing Wang, Feng Ye, Xin-yue Li, Li-qun Zhang, Da-peng Dai, Guo-xin Hu, Jian-ping Cai*, Jian-chang Qian* and Fu-sui Ji*, 
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Abstract

Cytochrome P450 2D6 (CYP2D6) exhibits rich genetic polymorphism, and functional changes caused by variations are the key reasons for differences in substrate drug systemic exposure. Discovering novel variants and defining their enzymatic kinetic characteristics can contribute to the personalized application of drugs. In this study, a data chain of variant-function-structure was established through population-based sequencing, baculovirus insect cell expression, in vitro enzymatic incubation, and ultrahigh performance liquid chromatography tandem mass spectrometry. Results revealed nine novel missense mutations in the exonic regions. After the corresponding microsomes were obtained, the kinetics of the variants were investigated using dextromethorphan as a probe substrate. It was found that the activities of CYP2D6.2, 10, 17, 35, 65, R28G, T76M, and E215K were significantly reduced, while D301V almost led to loss of enzyme function. Additionally, the relative clearance rate of R25Q was significantly increased. From the molecular structure perspective, the mutation sites are distributed outside the dextromethorphan binding pocket, suggesting that they primarily influence CYP2D6 activity via allosteric modulation. These research findings provide fundamental data for the precise application of CYP2D6 substrate drugs.

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新型 CYP2D6 变体的发现与酶动力学特性分析
细胞色素 P450 2D6(CYP2D6)具有丰富的遗传多态性,变异引起的功能变化是底物药物系统暴露差异的关键原因。发现新型变体并确定其酶动力学特征有助于药物的个性化应用。本研究通过群体测序、杆状病毒昆虫细胞表达、体外酶解孵育和超高效液相色谱串联质谱分析,建立了变异-功能-结构的数据链。结果发现外显子区有九个新的错义突变。在获得相应的微粒体后,以右美沙芬为探针底物研究了变体的动力学。结果发现,CYP2D6.2、10、17、35、65、R28G、T76M 和 E215K 的活性显著降低,而 D301V 几乎导致酶功能丧失。此外,R25Q 的相对清除率明显增加。从分子结构的角度来看,突变位点分布在右美沙芬结合口袋之外,表明它们主要通过异构调节影响 CYP2D6 的活性。这些研究成果为 CYP2D6 底物药物的精确应用提供了基础数据。
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来源期刊
CiteScore
7.90
自引率
7.30%
发文量
215
审稿时长
3.5 months
期刊介绍: Chemical Research in Toxicology publishes Articles, Rapid Reports, Chemical Profiles, Reviews, Perspectives, Letters to the Editor, and ToxWatch on a wide range of topics in Toxicology that inform a chemical and molecular understanding and capacity to predict biological outcomes on the basis of structures and processes. The overarching goal of activities reported in the Journal are to provide knowledge and innovative approaches needed to promote intelligent solutions for human safety and ecosystem preservation. The journal emphasizes insight concerning mechanisms of toxicity over phenomenological observations. It upholds rigorous chemical, physical and mathematical standards for characterization and application of modern techniques.
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