4.6 Review

Pharmacogenetics to guide cardiovascular drug therapy

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NATURE REVIEWS CARDIOLOGY
卷 18, 期 9, 页码 649-665

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NATURE PORTFOLIO
DOI: 10.1038/s41569-021-00549-w

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资金

  1. NIH grant NIH/NHGRI [U01 HG00729]
  2. NIH/NHLBI [R01 HL149752]
  3. NIH/NCATS [UL1TR001427]

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This Review examines the evidence supporting pharmacogenetic testing in cardiovascular medicine, including data from clinical trials, and provides examples of clinical implementation of genotype-guided cardiovascular therapies. Opportunities for future growth of the field are also discussed.
In this Review, Cavallari and colleagues examine the evidence supporting pharmacogenetic testing in cardiovascular medicine, describe guidelines for the use of cardiovascular pharmacogenetics and provide examples of the clinical implementation of genotype-guided therapies. Over the past decade, pharmacogenetic testing has emerged in clinical practice to guide selected cardiovascular therapies. The most common implementation in practice is CYP2C19 genotyping to predict clopidogrel response and assist in selecting antiplatelet therapy after percutaneous coronary intervention. Additional examples include genotyping to guide warfarin dosing and statin prescribing. Increasing evidence exists on outcomes with genotype-guided cardiovascular therapies from multiple randomized controlled trials and observational studies. Pharmacogenetic evidence is accumulating for additional cardiovascular medications. However, data for many of these medications are not yet sufficient to support the use of genotyping for drug prescribing. Ultimately, pharmacogenetics might provide a means to individualize drug regimens for complex diseases such as heart failure, in which the treatment armamentarium includes a growing list of medications shown to reduce morbidity and mortality. However, sophisticated analytical approaches are likely to be necessary to dissect the genetic underpinnings of responses to drug combinations. In this Review, we examine the evidence supporting pharmacogenetic testing in cardiovascular medicine, including that available from several clinical trials. In addition, we describe guidelines that support the use of cardiovascular pharmacogenetics, provide examples of clinical implementation of genotype-guided cardiovascular therapies and discuss opportunities for future growth of the field.

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