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research article

The Characteristics of Heterozygous Protein Truncating Variants in the Human Genome

Bartha, Istvan  
•
Rausell, Antonio
•
Mclaren, Paul J.  
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2015
Plos Computational Biology

Sequencing projects have identified large numbers of rare stop-gain and frameshift variants in the human genome. As most of these are observed in the heterozygous state, they test a gene's tolerance to haploinsufficiency and dominant loss of function. We analyzed the distribution of truncating variants across 16,260 autosomal protein coding genes in 11,546 individuals. We observed 39,893 truncating variants affecting 12,062 genes, which significantly differed from an expectation of 12,916 genes under a model of neutral de novo mutation (p<10(-4)). Extrapolating this to increasing numbers of sequenced individuals, we estimate that 10.8% of human genes do not tolerate heterozygous truncating variants. An additional 10 to 15% of truncated genes may be rescued by incomplete penetrance or compensatory mutations, or because the truncating variants are of limited functional impact. The study of protein truncating variants delineates the essential genome and, more generally, identifies rare heterozygous variants as an unexplored source of diversity of phenotypic traits and diseases.

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Type
research article
DOI
10.1371/journal.pcbi.1004647
Web of Science ID

WOS:000368521900042

Author(s)
Bartha, Istvan  
Rausell, Antonio
Mclaren, Paul J.  
Mohammadi, Pejman
Tardaguila, Manuel
Chaturvedi, Nimisha  
Fellay, Jacques  
Telenti, Amalio
Date Issued

2015

Publisher

Public Library Science

Published in
Plos Computational Biology
Volume

11

Issue

12

Article Number

e1004647

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
UPFELLAY  
Available on Infoscience
February 16, 2016
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/123932
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