The limits of genome-wide methods for pharmacogenomic testing

Gamazon, Eric R.; Skol, Andrew D.; Perera, Minoli A.

doi:10.1097/fpc.0b013e328350ca5f

Cited by 34 publications

(28 citation statements)

References 39 publications

(43 reference statements)

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“…However, the use of GWAS in African–American individuals also has its limitations. A recent publication by our laboratory interrogated the coverage of approximately 250 pharmacogenes (i.e., genes important in pharmacogenomics) on several different high-throughput genotyping platforms [76]. We also investigated the coverage of these pharmacogenes in the HapMap Project, which is commonly used as the reference set for SNP imputation in GWAS, compared with the 1000 Genomes Project data, which were generated through deeper sequencing and provide greater SNP coverage.…”

Section: Future Directions In Pharmacogenetic Researchmentioning

confidence: 99%

The Future of Warfarin Pharmacogenetics in under-represented Minority Groups

Cavallari

Perera

2012

Future Cardiol.

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Genotype-based dosing recommendations are provided in the US FDA-approved warfarin labeling. However, data that informed these recommendations were from predominately Caucasian populations. Studies show that variants contributing to warfarin dose requirements in Caucasians provide similar contributions to dose requirements in US Hispanics, but significantly lesser contributions in African–Americans. Further data demonstrate that variants occurring commonly in individuals of African ancestry, but rarely in other racial groups, significantly influence dose requirements in African–Americans. These data suggest that it is important to consider variants specific for African–Americans when implementing genotype-guided warfarin dosing in this population.

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Section: Future Directions In Pharmacogenetic Researchmentioning

confidence: 99%

The Future of Warfarin Pharmacogenetics in under-represented Minority Groups

Cavallari

Perera

2012

Future Cardiol.

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“…27 Health professionals involved in the delivery of PGx testing may include the laboratorian, prescriber, pharmacist, and potentially a genetic counselor. With development of new and cheaper testing technologies, 29,30 it is possible that patients’ genetic predisposition for a panel of drugs will be ascertained through a single test and results consulted as new medications are prescribed.…”

Section: Pgx Testingmentioning

confidence: 99%

Challenges to Integrating Pharmacogenetic Testing into Medication Therapy Management

Haga

LaPointe²,

Moaddeb³

2015

JMCP

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Background Some have proposed the integration of pharmacogenetic (PGx) testing into medication therapy management (MTM) to enable further refinement of treatment(s) to reduce risk of adverse responses and improve efficacy. PGx testing involves the analysis of genetic variants associated with therapeutic or adverse response and may be useful in enhancing the ability to identify ineffective and/or harmful drugs or drug combinations. This “enhanced” MTM might also reduce patient concerns about side effects and increase confidence that the medication is effective, addressing two key factors that impact patient adherence - concern and necessity. However, the feasibility and effectiveness of the integration of PGx testing into MTM in clinical practice has not yet been determined. Objectives In this paper, we consider some of the challenges to the integration and delivery of PGx testing in MTM services. What is already known about this subject While the addition of pharmacogenetic testing has been suggested, little literature exists exploring the challenges or feasibility of doing so.

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“…Prior to the advances in high-throughput genome-wide technologies [16], pharmacogenetic studies focused primarily on candidate genes within a priori implicated pathways. In general, classic pharmacogenetic studies were restricted to pharmacologic traits in which a small number of variants (frequently, in a single candidate gene) had a large effect on drug response [17].…”

Section: The Central Premise Is Also the ‘Gap’ In Pharmacogenomic Stumentioning

confidence: 99%