Centre for Clinical Pharmacology, University College London, London, United Kingdom.
PLoS One. 2009 Dec 2;4(12):e7960. doi: 10.1371/journal.pone.0007960.
Studies of the genetic basis of drug response could help clarify mechanisms of drug action/metabolism, and facilitate development of genotype-based predictive tests of efficacy or toxicity (pharmacogenetics).
We conducted a systematic review and field synopsis of pharmacogenetic studies to quantify the scope and quality of available evidence in this field in order to inform future research.
Original research articles were identified in Medline, reference lists from 24 meta-analyses/systematic reviews/review articles and U.S. Food and Drug Administration website of approved pharmacogenetic tests. STUDY ELIGIBILITY CRITERIA, PARTICIPANTS, AND INTERVENTION CRITERIA: We included any study in which either intended or adverse response to drug therapy was examined in relation to genetic variation in the germline or cancer cells in humans.
Study characteristics and data reported in abstracts were recorded. We further analysed full text from a random 10% subset of articles spanning the different subclasses of study.
From 102,264 Medline hits and 1,641 articles from other sources, we identified 1,668 primary research articles (1987 to 2007, inclusive). A high proportion of remaining articles were reviews/commentaries (ratio of reviews to primary research approximately 25 ratio 1). The majority of studies (81.8%) were set in Europe and North America focussing on cancer, cardiovascular disease and neurology/psychiatry. There was predominantly a candidate gene approach using common alleles, which despite small sample sizes (median 93 [IQR 40-222]) with no trend to an increase over time, generated a high proportion (74.5%) of nominally significant (p<0.05) reported associations suggesting the possibility of significance-chasing bias. Despite 136 examples of gene/drug interventions being the subject of >or=4 studies, only 31 meta-analyses were identified. The majority (69.4%) of end-points were continuous and likely surrogate rather than hard (binary) clinical end-points.
The high expectation but limited translation of pharmacogenetic research thus far may be explained by the preponderance of reviews over primary research, small sample sizes, a mainly candidate gene approach, surrogate markers, an excess of nominally positive to truly positive associations and paucity of meta-analyses. Recommendations based on these findings should inform future study design to help realise the goal of personalised medicines. SYSTEMATIC REVIEW REGISTRATION NUMBER: Not Registered.
药物反应遗传基础的研究有助于阐明药物作用/代谢的机制,并促进基于基因型的疗效或毒性预测测试(药物遗传学)的发展。
我们进行了一项系统评价和领域综述,对药物遗传学研究进行量化,以了解该领域现有证据的范围和质量,从而为未来的研究提供信息。
在 Medline、24 项荟萃分析/系统评价/综述文章的参考文献列表以及美国食品和药物管理局批准的药物遗传学测试网站中确定了原始研究文章。
研究入选标准、参与者和干预措施标准:我们纳入了任何研究,其中药物治疗的预期或不良反应与人类生殖系或癌细胞中的遗传变异有关。
记录了研究特征和摘要中报告的数据。我们进一步分析了来自不同研究子类的随机 10%子集的文章的全文。
从 102,264 篇 Medline 命中和其他来源的 1,641 篇文章中,我们确定了 1,668 篇原发性研究文章(1987 年至 2007 年,包括在内)。剩余的文章大部分是评论/评论(评论与原始研究的比例约为 25 比 1)。大多数研究(81.8%)集中在欧洲和北美,专注于癌症、心血管疾病和神经病/精神病学。主要采用常见等位基因的候选基因方法,尽管样本量较小(中位数为 93 [IQR 40-222]),且没有随时间增加的趋势,但产生了高比例(74.5%)的名义上显著(p<0.05)报告关联,表明存在意义追逐偏见的可能性。尽管有 136 个基因/药物干预的例子是>或=4 项研究的主题,但只确定了 31 项荟萃分析。大多数(69.4%)终点是连续的,更可能是替代而不是硬(二进制)临床终点。
药物遗传学研究迄今为止的高期望但有限的转化可以用评论多于原始研究、样本量小、主要候选基因方法、替代标志物、名义上阳性到真正阳性关联的过多以及荟萃分析的缺乏来解释。基于这些发现的建议应该为未来的研究设计提供信息,以帮助实现个性化药物的目标。
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