The pace of exome and genome
sequencing is accelerating, with the identification of many new disease-causing
mutations in research settings, and it is likely that whole exome or genome
sequencing could have a major impact in the clinical arena in the relatively
near future. However, the human genomics community is currently facing several
challenges, including phenotyping, sample collection, sequencing strategies,
bioinformatics analysis, biological validation of variant function, clinical
interpretation and validity of variant data, and delivery of genomic
information to various constituents. Here we review these challenges and
summarize the bottlenecks for the clinical application of exome and genome
sequencing, and we discuss ways for moving the field forward. In particular, we
urge the need for clinical-grade sample collection, high-quality sequencing
data acquisition, digitalized phenotyping, rigorous generation of variant
calls, and comprehensive functional annotation of variants. Additionally, we
suggest that a 'networking of science' model that encourages much more
collaboration and online sharing of medical history, genomic data and
biological knowledge, including among research participants and
consumers/patients, will help establish causation and penetrance for disease
causal variants and genes. As we enter this new era of genomic medicine, we
envision that consumer-driven and consumer-oriented efforts will take center
stage, thus allowing insights from the human genome project to translate
directly back into individualized medicine.
Source: Identifying disease mutations in genomic medicine settings: current
challenges and how to accelerate progress. Lyon GJ, Wang K (kaichop@gmail.com). Genome Med. 2012 Jul 26;4(7):58.
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