Integrating Pharmacogenomics into the Broader Construct of Genomic Medicine: Efforts by the ClinGen Pharmacogenomics Working Group (PGxWG)

药物基因组学 构造(python库) 群(周期表) 医学 基因组医学 心理学 计算生物学 药理学 生物 计算机科学 化学 有机化学 程序设计语言
作者
Li Gong,Clarissa Klein,Kelly E. Caudle,Ann M. Moyer,Stuart A. Scott,Michelle Whirl‐Carrillo,Teri E. Klein,Folefac Aminkeng,Sami S. Amr,Kristine Ashcraft,Brooke Bernhardt,Burns C Blaxwell,Zo Bly,Amber Cipriani,Neal Cody,Collet Dandara,Andria L. Del Tredici,Philip E. Empey,Elizabeth L. Fieg,Andrea Gaedigk,David Gregornik,Steven M. Harrison,Jennifer Hart,James M. Hoffman,Jessica Ezzell Hunter,Otito F. Iwuchukwu,Melissa Landrum,Kristofor K. Langlais,M T M Lee,Rongling Li,Adriana Malheiro,Howard L. McLeod,Andrew A. Monte,Joannella Morales,Hetanshi Naik,Aniwaa Owusu Obeng,Akinyemi Oni‐Orisan,Erin M. Ramos,Zhaoxia Ren,Marylyn D. Ritchie,Sara Rogers,Steven E. Scherer,Sherin Shaaban,Jesse J. Swen,Alex H. Wagner,Erica L. Woodahl,Joanne McIntyre,K.A. Merritt,Matt W. Wright
出处
期刊:Clinical Chemistry [Oxford University Press]
卷期号:71 (1): 36-44
标识
DOI:10.1093/clinchem/hvae181
摘要

Pharmacogenomics (PGx) is focused on the relationship between an individual's genetic makeup and their response to medications, with the overarching aim of guiding prescribing decisions to improve drug efficacy and reduce adverse events. The PGx and genomic medicine communities have worked independently for over 2 decades, developing separate standards and terminology, making implementation of PGx across all areas of genomic medicine difficult. To address this issue, the Clinical Genome Resource (ClinGen) Pharmacogenomics Working Group (PGxWG) was established by the National Institutes of Health (NIH)-funded ClinGen to initially create frameworks for evaluating gene-drug response clinical validity and actionability aligned with the ClinGen frameworks for evaluating monogenic gene-disease relationships, and a framework for classifying germline PGx variants similar to the American College of Medical Genetics (ACMG) and Association of Molecular Pathology (AMP) system for interpretation of disease-causing variants. These frameworks will leverage decades of work from well-established PGx resources facilitating buy-in among PGx stakeholders. In this report, we describe the background and major activities of the ClinGen PGxWG, and how this initiative will facilitate the critical inclusion of PGx into the larger context of genomic medicine.

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