2017
DOI: 10.1002/cpt.663
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Are Evidence Standards Different for Genomic‐ vs. Clinical‐Based Precision Medicine? A Quantitative Analysis of Individualized Warfarin Therapy

Abstract: Evidence requirements for implementation of precision medicine (PM), whether informed by genomic or clinical data, are not well defined. Evidence requirements are driven by uncertainty and its attendant consequences; these aspects can be quantified by a novel technique in health economics, value of information analysis (VOI). We utilized VOI analysis to compare the evidence levels over time for warfarin dosing based on pharmacogenomic- vs. amiodarone-warfarin drug-drug interaction information. The primary outc… Show more

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Cited by 8 publications
(4 citation statements)
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“…There is also no clear and specific guidance on "how to evaluate a PGx test" for clinical utility in guiding treatment decisions. Various trial designs exist but due to the nature of PGx testing serving as a support tool, traditional placebo-controlled, double-blind RCT designs do not necessarily provide adequate evidence for PGx testing [47][48][49][50]. While RCTs are valuable for evaluating the clinical validity of a test (especially one with an algorithm), it does not necessarily reflect real-world usage [51].…”
Section: Provision Of Clinical Pgx Testingmentioning
confidence: 99%
“…There is also no clear and specific guidance on "how to evaluate a PGx test" for clinical utility in guiding treatment decisions. Various trial designs exist but due to the nature of PGx testing serving as a support tool, traditional placebo-controlled, double-blind RCT designs do not necessarily provide adequate evidence for PGx testing [47][48][49][50]. While RCTs are valuable for evaluating the clinical validity of a test (especially one with an algorithm), it does not necessarily reflect real-world usage [51].…”
Section: Provision Of Clinical Pgx Testingmentioning
confidence: 99%
“…Our view is that such evaluation is necessary if a test is to be adopted widely in a financially constrained healthcare system. This might mean that the evidence threshold for implementation of pharmacogenomic testing is significantly higher than for other tests that guide therapeutic decisions 28,29 . For example, dosage adjustment in impaired kidney function has often been based on theoretical pharmacokinetic calculations rather than outcome data.…”
Section: Resultsmentioning
confidence: 99%
“…This might mean that the evidence threshold for implementation of pharmacogenomic testing is significantly higher than for other tests that guide therapeutic decisions. 28,29 For example, dosage adjustment in impaired kidney function has often been based on theoretical pharmacokinetic calculations rather than outcome data. However, studies demonstrate significant unwarranted variation and excessive use of non-genetic testing, which may contribute to patient harm and escalating costs, so this approach should not be regarded as a standard of best practice.…”
Section: Does the Addition Of The Pharmacogenomic Test Improve Clinic...mentioning
confidence: 99%
“…1 Yet there are examples of clinical PM commonly used in practice for which such data are also lacking, such as contraindication of potential drug interactions to guide pharmacotherapy. 2 Are there different evidence thresholds for genomic versus clinical PM?…”
Section: Introductionmentioning
confidence: 99%