| Literature DB >> 30503770 |
Rocky Cheung1, Kimberly D Insigne2, David Yao3, Christina P Burghard2, Jeffrey Wang1, Yun-Hua E Hsiao4, Eric M Jones1, Daniel B Goodman5, Xinshu Xiao6, Sriram Kosuri7.
Abstract
Mutations that lead to splicing defects can have severe consequences on gene function and cause disease. Here, we explore how human genetic variation affects exon recognition by developing a multiplexed functional assay of splicing using Sort-seq (MFASS). We assayed 27,733 variants in the Exome Aggregation Consortium (ExAC) within or adjacent to 2,198 human exons in the MFASS minigene reporter and found that 3.8% (1,050) of variants, most of which are extremely rare, led to large-effect splice-disrupting variants (SDVs). Importantly, we find that 83% of SDVs are located outside of canonical splice sites, are distributed evenly across distinct exonic and intronic regions, and are difficult to predict a priori. Our results indicate extant, rare genetic variants can have large functional effects on splicing at appreciable rates, even outside the context of disease, and MFASS enables their empirical assessment at scale.Entities:
Keywords: exon recognition; massively parallel reporter assay; population variation; rare variation; splicing; variant classification
Mesh:
Year: 2018 PMID: 30503770 PMCID: PMC6599603 DOI: 10.1016/j.molcel.2018.10.037
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970