Skip to main content
Download PDF
- Main
Clinical Exome Sequencing for Genetic Identification of Rare Mendelian Disorders
- Lee, Hane;
- Deignan, Joshua L;
- Dorrani, Naghmeh;
- Strom, Samuel P;
- Kantarci, Sibel;
- Quintero-Rivera, Fabiola;
- Das, Kingshuk;
- Toy, Traci;
- Harry, Bret;
- Yourshaw, Michael;
- Fox, Michelle;
- Fogel, Brent L;
- Martinez-Agosto, Julian A;
- Wong, Derek A;
- Chang, Vivian Y;
- Shieh, Perry B;
- Palmer, Christina GS;
- Dipple, Katrina M;
- Grody, Wayne W;
- Vilain, Eric;
- Nelson, Stanley F
- et al.
Published Web Location
https://doi.org/10.1001/jama.2014.14604Abstract
Importance
Clinical exome sequencing (CES) is rapidly becoming a common molecular diagnostic test for individuals with rare genetic disorders.Objective
To report on initial clinical indications for CES referrals and molecular diagnostic rates for different indications and for different test types.Design, setting, and participants
Clinical exome sequencing was performed on 814 consecutive patients with undiagnosed, suspected genetic conditions at the University of California, Los Angeles, Clinical Genomics Center between January 2012 and August 2014. Clinical exome sequencing was conducted as trio-CES (both parents and their affected child sequenced simultaneously) to effectively detect de novo and compound heterozygous variants or as proband-CES (only the affected individual sequenced) when parental samples were not available.Main outcomes and measures
Clinical indications for CES requests, molecular diagnostic rates of CES overall and for phenotypic subgroups, and differences in molecular diagnostic rates between trio-CES and proband-CES.Results
Of the 814 cases, the overall molecular diagnosis rate was 26% (213 of 814; 95% CI, 23%-29%). The molecular diagnosis rate for trio-CES was 31% (127 of 410 cases; 95% CI, 27%-36%) and 22% (74 of 338 cases; 95% CI, 18%-27%) for proband-CES. In cases of developmental delay in children (<5 years, n = 138), the molecular diagnosis rate was 41% (45 of 109; 95% CI, 32%-51%) for trio-CES cases and 9% (2 of 23, 95% CI, 1%-28%) for proband-CES cases. The significantly higher diagnostic yield (P value = .002; odds ratio, 7.4 [95% CI, 1.6-33.1]) of trio-CES was due to the identification of de novo and compound heterozygous variants.Conclusions and relevance
In this sample of patients with undiagnosed, suspected genetic conditions, trio-CES was associated with higher molecular diagnostic yield than proband-CES or traditional molecular diagnostic methods. Additional studies designed to validate these findings and to explore the effect of this approach on clinical and economic outcomes are warranted.Many UC-authored scholarly publications are freely available on this site because of the UC's open access policies. Let us know how this access is important for you.
Main Content
For improved accessibility of PDF content, download the file to your device.
Enter the password to open this PDF file:
File name:
-
File size:
-
Title:
-
Author:
-
Subject:
-
Keywords:
-
Creation Date:
-
Modification Date:
-
Creator:
-
PDF Producer:
-
PDF Version:
-
Page Count:
-
Page Size:
-
Fast Web View:
-
Preparing document for printing…
0%