Molecular genetic testing and the future of clinical genomics

被引:0
|
作者
Sara Huston Katsanis
Nicholas Katsanis
机构
[1] Duke Institute for Genome Sciences and Policy,
[2] Duke University Medical Center,undefined
[3] Center for Human Disease Modeling,undefined
[4] Duke University Medical Center,undefined
来源
Nature Reviews Genetics | 2013年 / 14卷
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摘要
Clinical molecular genetic testing is transforming personalized medicine and is appropriate for a range of applications, such as rare disease diagnostics and predictive testing for common disorders.Whole-exome and whole-genome sequencing may become a first-line clinical test for some naive diagnostic cases, but classic genetic tests will continue to be used for the high analytical sensitivity of specific defects and for the confirmation of genome findings.There remains no single test to detect the wide array of genetic defects that may be inherited or arise de novo; clinical diagnostics requires multiple approaches to determine a causal genetic defect.Although genome sequencing may transform diagnostic approaches in large academic medical centres, access to expensive and sophisticated tests are not universal. Genetic testing must be available globally through validated simple technologies for molecular diagnostics (such as direct PCR, linkage analysis or multiplex ligation-dependent probe amplification).The greatest challenge to clinical genomics is the reliable interpretation of the multiple and novel variants found through genome sequencing. Pathogenicity of genetic variants can be examined with bioinformatics prediction approaches, protein stability studies, transcriptional activity studies and allele- and/or gene-specific animal models.As broader genomic information becomes available to providers and patients, partnerships will develop to convey patient-centred data, including incidental findings. The regulatory environment must adapt to the coming volume of genomic information to maximize benefit to patients and health-care systems and to match the expectations of the patient population with regard to these technologies.
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页码:415 / 426
页数:11
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