Regional nonsense constraint offers clinical and biological insights into rare genetic disorders

Alexander Blakes
Nicola Whiffin
Colin Johnson
Jamie M Ellingford
Siddharth Banka

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Abstract

Understanding the molecular consequences of variants which introduce premature termination codons (PTCs) is essential to predicting their clinical impact. Although transcripts with PTCs are generally expected to undergo nonsense-mediated mRNA decay (NMD), up to 45% of all possible PTCs in the human genome are predicted to escape NMD. Existing studies of constraint against predicted loss-of-function variants at the transcript level do not account for regional differences in NMD efficiency. Here, we developed an NMD-informed constraint metric using sequencing data from 730,947 individuals and found 2,764 transcripts with regional nonsense constraint. In rare disease cohorts, de novo nonsense and frameshift variants in constrained regions are up to 9.4-fold enriched and associated with up to 6.4-fold higher odds of diagnosis than in unconstrained regions. We prioritise fourteen candidate disease genes in which constrained regions harbour clusters of nonsense and frameshift variants. These findings will enhance variant interpretation, deliver mechanistic insights, and empower the discovery of novel disease genes.

Version published to 10.1101/2024.10.10.24315185v1 on medRxiv
Oct 13, 2024

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Regional nonsense constraint offers clinical and biological insights into rare genetic disorders

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Abstract

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When Two plus Four Does Not Equal Six: Combining Computational and Functional Evidence Towards Classification of BRCA1 Key Domain Missense Substitutions.

Deleterious Variants Contribute Minimal Excess Risk in Large-Scale Testing

TP53 minigene analysis of 161 sequence changes provides evidence for role of spatial constraint and regulatory elements on variant-induced splicing impact

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Abstract

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