Genome-wide profiling of highly similar paralogous genes using HiFi sequencing

Author:

Chen XiaoORCID,Baker Daniel,Dolzhenko EgorORCID,Devaney Joseph M,Noya Jessica,Berlyoung April S,Brandon Rhonda,Hruska Kathleen S,Lochovsky Lucas,Kruszka Paul,Newman Scott,Farrow Emily,Thiffault Isabelle,Pastinen Tomi,Kasperaviciute Dalia,Gilissen ChristianORCID,Vissers LisenkaORCID,Hoischen AlexanderORCID,Berger Seth,Vilain Eric,Délot Emmanuèle, ,Eberle Michael AORCID

Abstract

AbstractVariant calling is hindered in segmental duplications by sequence homology. We developed Paraphase, a HiFi-based informatics method that resolves highly similar genes by phasing all haplotypes of a gene family. We applied Paraphase to 160 long (>10 kb) segmental duplication regions across the human genome with high (>99%) sequence similarity, encoding 316 genes. Analysis across five ancestral populations revealed highly variable copy numbers of these regions. We identified 23 families with exceptionally low within-family diversity, where extensive gene conversion and unequal-crossing over have resulted in highly similar gene copies. Furthermore, our analysis of 36 trios identified 7de novoSNVs and 4de novogene conversion events, 2 of which are non-allelic. Finally, we summarized extensive genetic diversity in 9 medically relevant genes previously considered challenging to genotype. Paraphase provides a framework for resolving gene paralogs, enabling accurate testing in medically relevant genes and population-wide studies of previously inaccessible genes.

Publisher

Cold Spring Harbor Laboratory

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