作者
Fan Xia, Matthew N Bainbridge, Tiong Yang Tan, Michael F Wangler, Angela E Scheuerle, Elaine H Zackai, Margaret H Harr, V Reid Sutton, Roopa L Nalam, Wenmiao Zhu, Margot Nash, Monique M Ryan, Joy Yaplito-Lee, Jill V Hunter, Matthew A Deardorff, Samantha J Penney, Arthur L Beaudet, Sharon E Plon, Eric A Boerwinkle, James R Lupski, Christine M Eng, Donna M Muzny, Yaping Yang, Richard A Gibbs
发表日期
2014/5/1
期刊
The American Journal of Human Genetics
卷号
94
期号
5
页码范围
784-789
出版商
Elsevier
简介
Clinical whole-exome sequencing (WES) for identification of mutations leading to Mendelian disease has been offered to the medical community since 2011. Clinically undiagnosed neurological disorders are the most frequent basis for test referral, and currently, approximately 25% of such cases are diagnosed at the molecular level. To date, there are approximately 4,000 "known" disease-associated loci, and many are associated with striking dysmorphic features, making genotype-phenotype correlations relatively straightforward. A significant fraction of cases, however, lack characteristic dysmorphism or clinical pathognomonic traits and are dependent upon molecular tests for definitive diagnoses. Further, many molecular diagnoses are guided by recent gene-disease association discoveries. Hence, there is a critical interplay between clinical testing and research leading to gene-disease association discovery …
学术搜索中的文章
F Xia, MN Bainbridge, TY Tan, MF Wangler… - The American Journal of Human Genetics, 2014
