Combining genetic constraint with predictions of alternative splicing to prioritize deleterious splicing in rare disease studies

Michael J Cormier; Brent S Pedersen; Pinar Bayrak-Toydemir; Aaron R Quinlan

doi:10.1186/s12859-022-05041-x

Combining genetic constraint with predictions of alternative splicing to prioritize deleterious splicing in rare disease studies

BMC Bioinformatics. 2022 Nov 14;23(1):482. doi: 10.1186/s12859-022-05041-x.

Authors

Michael J Cormier^{1

2}, Brent S Pedersen^{1

2}, Pinar Bayrak-Toydemir³, Aaron R Quinlan^{4

5

6}

Affiliations

¹ Department of Human Genetics, University of Utah, Salt Lake City, UT, USA.
² Utah Center for Genetic Discovery, University of Utah, Salt Lake City, UT, USA.
³ Department of Pathology, University of Utah, Salt Lake City, UT, USA.
⁴ Department of Human Genetics, University of Utah, Salt Lake City, UT, USA. aquinlan@genetics.utah.edu.
⁵ Utah Center for Genetic Discovery, University of Utah, Salt Lake City, UT, USA. aquinlan@genetics.utah.edu.
⁶ Department of Biomedical Informatics, University of Utah, Salt Lake City, UT, USA. aquinlan@genetics.utah.edu.

Abstract

Background: Despite numerous molecular and computational advances, roughly half of patients with a rare disease remain undiagnosed after exome or genome sequencing. A particularly challenging barrier to diagnosis is identifying variants that cause deleterious alternative splicing at intronic or exonic loci outside of canonical donor or acceptor splice sites.

Results: Several existing tools predict the likelihood that a genetic variant causes alternative splicing. We sought to extend such methods by developing a new metric that aids in discerning whether a genetic variant leads to deleterious alternative splicing. Our metric combines genetic variation in the Genome Aggregate Database with alternative splicing predictions from SpliceAI to compare observed and expected levels of splice-altering genetic variation. We infer genic regions with significantly less splice-altering variation than expected to be constrained. The resulting model of regional splicing constraint captures differential splicing constraint across gene and exon categories, and the most constrained genic regions are enriched for pathogenic splice-altering variants. Building from this model, we developed ConSpliceML. This ensemble machine learning approach combines regional splicing constraint with multiple per-nucleotide alternative splicing scores to guide the prediction of deleterious splicing variants in protein-coding genes. ConSpliceML more accurately distinguishes deleterious and benign splicing variants than state-of-the-art splicing prediction methods, especially in "cryptic" splicing regions beyond canonical donor or acceptor splice sites.

Conclusion: Integrating a model of genetic constraint with annotations from existing alternative splicing tools allows ConSpliceML to prioritize potentially deleterious splice-altering variants in studies of rare human diseases.

Keywords: Alternative splicing; Genetic constraint; Genomic medicine; Genomics; Machine learning; Noncanonical cryptic splicing; Pathogenic interpretation; Purifying selection; Rare disease; Splicing.

MeSH terms

Alternative Splicing*
Exons
Humans
Introns
Mutation
RNA Splice Sites
RNA Splicing
Rare Diseases* / genetics

Substances

RNA Splice Sites

Abstract

MeSH terms

Substances

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