FDA 批准药物的 ADME 基因相关药物基因组标签：与临床药物遗传学实施联盟（CPIC）证据水平的比较。

Medicines (Basel, Switzerland) Pub Date : 2024-02-20 DOI:10.3390/medicines11030006

Subrata Deb, Robert Hopefl, Anthony Allen Reeves, Dena Cvetkovic

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引用次数: 0

摘要

药物基因组学（PGx）可以促进向患者特异性用药方案的过渡，从而提高疗效并降低毒性。本研究旨在评估美国食品药品管理局（FDA）PGx标签和临床药理遗传学实施联盟（CPIC）数据库中与药物吸收、分布、代谢和消除（ADME）相关基因的PGx分类重叠情况。在 CPIC 数据库中确定了 FDA 批准的药物和 PGx 标签中的 ADME 基因。根据药物与 ADME（药代动力学）相关基因的关联、PGx FDA 标签类别和 CPIC 证据级别对药物进行筛选。在 CPIC 数据库中总共 442 对 ADME 和非 ADME 基因药物配对中，分别有 273 对、55 对和 48 对因缺乏 FDA 标签、混合 CPIC 证据级别临时分类和非 ADME 基因药物配对而被排除。这 66 对 ADME 基因-药物被分为以下几类：10对（15%）具有参考价值，49对（74%）具有可操作性，6对（9%）建议进行检测，1对（2%）需要进行检测。在 FDA PGx 标签中，CYP2D6 是最常见的基因。从具有 FDA 和 CPIC PGx 分类的 ADME 基因-药物配对来看，大多数药物用于抑郁症、癌症和止痛药。具有 FDA PGx 标签的 ADME 基因药物配对与 CPIC 分类有很大的重叠；但是，大量的 ADME 基因药物配对只有 CPIC 证据级别，而没有 FDA 分类。PGx 可操作标签是最常见的分类，CYP2D6 是 FDA PGx 标签中最常见的 ADME 基因。医疗专业人员可以通过分析和协调 FDA 标签和 CPIC 数据库，对药物遗传学干预的治疗效果产生影响。

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ADME Gene-Related Pharmacogenomic Labeling of FDA-Approved Drugs: Comparison with Clinical Pharmacogenetics Implementation Consortium (CPIC) Evidence Levels.

Pharmacogenomics (PGx) can facilitate the transition to patient-specific drug regimens and thus improve their efficacy and reduce toxicity. The aim of this study was to evaluate the overlap of PGx classification for drug absorption, distribution, metabolism, and elimination (ADME)-related genes in the U.S. Food and Drug Administration (FDA) PGx labeling and in the Clinical Pharmacogenetics Implementation Consortium (CPIC) database. FDA-approved drugs and PGx labeling for ADME genes were identified in the CPIC database. Drugs were filtered by their association with ADME (pharmacokinetics)-related genes, PGx FDA labeling class, and CPIC evidence level. FDA PGx labeling was classified as either actionable, informative, testing recommended, or testing required, and varying CPIC evidence levels as either A, B, C, or D. From a total of 442 ADME and non-ADME gene-drug pairs in the CPIC database, 273, 55, and 48 pairs were excluded for lack of FDA labeling, mixed CPIC evidence level provisional classification, and non-ADME gene-drug pairs, respectively. The 66 ADME gene-drug pairs were classified into the following categories: 10 (15%) informative, 49 (74%) actionable, 6 (9%) testing recommended, and 1 (2%) testing required. CYP2D6 was the most prevalent gene among the FDA PGx labeling. From the ADME gene-drug pairs with both FDA and CPIC PGx classification, the majority of the drugs were for depression, cancer, and pain medications. The ADME gene-drug pairs with FDA PGx labeling considerably overlap with CPIC classification; however, a large number of ADME gene-drug pairs have only CPIC evidence levels but not FDA classification. PGx actionable labeling was the most common classification, with CYP2D6 as the most prevalent ADME gene in the FDA PGx labeling. Health professionals can impact therapeutic outcomes via pharmacogenetic interventions by analyzing and reconciling the FDA labels and CPIC database.

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Medicines (Basel, Switzerland)

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6 weeks