Krembil Brain Institute, Toronto Western Hospital, Toronto, Ontario, Canada.
Department of Drug Design and Pharmacology, Faculty of Health and Medical Sciences, University of Copenhagen, Copenhagen, Denmark.
Crit Rev Clin Lab Sci. 2024 Dec;61(8):641-684. doi: 10.1080/10408363.2024.2358304. Epub 2024 Aug 9.
The field of pharmacogenetics, the investigation of the influence of one or more sequence variants on drug response phenotypes, is a special case of pharmacogenomics, a discipline that takes a genome-wide approach. Massively parallel, next generation sequencing (NGS), has allowed pharmacogenetics to be subsumed by pharmacogenomics with respect to the identification of variants associated with responders and non-responders, optimal drug response, and adverse drug reactions. A plethora of rare and common naturally-occurring GPCR variants must be considered in the context of signals from across the genome. Many fundamentals of pharmacogenetics were established for G protein-coupled receptor (GPCR) genes because they are primary targets for a large number of therapeutic drugs. Functional studies, demonstrating likely-pathogenic and pathogenic GPCR variants, have been integral to establishing models used for analysis. Variants in GPCR genes include both coding and non-coding single nucleotide variants and insertion or deletions (indels) that affect cell surface expression (trafficking, dimerization, and desensitization/downregulation), ligand binding and G protein coupling, and variants that result in alternate splicing encoding isoforms/variable expression. As the breadth of data on the GPCR genome increases, we may expect an increase in the use of drug labels that note variants that significantly impact the clinical use of GPCR-targeting agents. We discuss the implications of GPCR pharmacogenomic data derived from the genomes available from individuals who have been well-phenotyped for receptor structure and function and receptor-ligand interactions, and the potential benefits to patients of optimized drug selection. Examples discussed include the renin-angiotensin system in SARS-CoV-2 (COVID-19) infection, the probable role of chemokine receptors in the cytokine storm, and potential protease activating receptor (PAR) interventions. Resources dedicated to GPCRs, including publicly available computational tools, are also discussed.
药物遗传学领域研究一个或多个序列变异对药物反应表型的影响,是药物基因组学的一个特例,它采用全基因组方法。大规模平行的下一代测序(NGS)使得药物遗传学在识别与应答者和无应答者、最佳药物反应和药物不良反应相关的变异方面被纳入药物基因组学。在考虑来自整个基因组的信号时,必须考虑大量罕见和常见的天然存在的 GPCR 变异。许多药物遗传学的基本原则都是针对 G 蛋白偶联受体(GPCR)基因确立的,因为它们是大量治疗药物的主要靶点。功能研究证明了可能的致病性和致病性 GPCR 变异,对于建立用于分析的模型至关重要。GPCR 基因中的变异包括影响细胞表面表达(运输、二聚化和脱敏/下调)、配体结合和 G 蛋白偶联的编码和非编码单核苷酸变异和插入或缺失(indels),以及导致编码异构体/可变表达的交替剪接变异。随着关于 GPCR 基因组的数据范围的扩大,我们可能会期望增加使用药物标签来标记那些显著影响 GPCR 靶向药物临床应用的变异。我们讨论了从对受体结构和功能以及受体配体相互作用进行了充分表型分析的个体的基因组中获得的 GPCR 药物基因组学数据的影响,以及优化药物选择对患者的潜在益处。讨论的例子包括肾素-血管紧张素系统在 SARS-CoV-2(COVID-19)感染中的作用、趋化因子受体在细胞因子风暴中的可能作用以及潜在的蛋白酶激活受体(PAR)干预。还讨论了专门针对 GPCR 的资源,包括可公开获得的计算工具。
