Improving genetic diagnosis in Mendelian disease with transcriptome sequencing
Broad Institute · Harvard University · +19 more institutions
Abstract
That results in a dominantly acting splice-gain event, disrupting the critical glycine repeat motif of the triple helical domain. We identify this pathogenic variant in a total of 27 genetically unsolved patients in an external collagen VI-like dystrophy cohort, thus explaining approximately 25% of patients clinically suggestive of having collagen VI dystrophy in whom prior genetic analysis is negative. Overall, this study represents a large systematic application of transcriptome sequencing to rare disease diagnosis and highlights its utility for the detection and interpretation of variants missed by current standard diagnostic approaches.
Citation impact
- FWCI
- 71.03
- Percentile
- 100%
- References
- 50
Authors
38- BBBeryl B. Cummings
Broad Institute, Harvard University, Massachusetts General Hospital, Massachusetts Institute of Technology
- JLJamie L. Marshall
Broad Institute, Massachusetts General Hospital, Massachusetts Institute of Technology
- TTTaru Tukiainen
Broad Institute, Massachusetts General Hospital, Massachusetts Institute of Technology
- MLMonkol Lek
Broad Institute, The University of Sydney, Children's Hospital at Westmead, UNSW Sydney, Massachusetts General Hospital, Massachusetts Institute of Technology
- SDSandra Donkervoort
National Institute of Neurological Disorders and Stroke
Topics & keywords
- Transcriptome
- Mendelian inheritance
- Disease
- Biology
- Genetics
- DNA sequencing
- Genetic diagnosis
- Computational biology