Towards a Comprehensive Variation Benchmark for Challenging Medically-Relevant Autosomal Genes

Author:

Wagner Justin,Olson Nathan D,Harris Lindsay,McDaniel Jennifer,Cheng Haoyu,Fungtammasan Arkarachai,Hwang Yih-Chii,Gupta Richa,Wenger Aaron M,Rowell William J,Khan Ziad M,Farek Jesse,Zhu Yiming,Pisupati Aishwarya,Mahmoud Medhat,Xiao Chunlin,Yoo Byunggil,Sahraeian Sayed Mohammad Ebrahim,Miller Danny E.ORCID,Jáspez David,Lorenzo-Salazar José M.,Muñoz-Barrera Adrián,Rubio-Rodríguez Luis A.,Flores CarlosORCID,Narzisi GiuseppeORCID,Evani Uday Shanker,Clarke Wayne E.,Lee Joyce,Mason Christopher E.ORCID,Lincoln Stephen E.,Miga Karen H.,Ebbert Mark T. W.,Shumate Alaina,Li Heng,Chin Chen-Shan,Zook Justin MORCID,Sedlazeck Fritz J

Abstract

AbstractThe repetitive nature and complexity of multiple medically important genes make them intractable to accurate analysis, despite the maturity of short-read sequencing, resulting in a gap in clinical applications of genome sequencing. The Genome in a Bottle Consortium has provided benchmark variant sets, but these excluded some medically relevant genes due to their repetitiveness or polymorphic complexity. In this study, we characterize 273 of these 395 challenging autosomal genes that have multiple implications for medical sequencing. This extended, curated benchmark reports over 17,000 SNVs, 3,600 INDELs, and 200 SVs each for GRCh37 and GRCh38 across HG002. We show that false duplications in either GRCh37 or GRCh38 result in reference-specific, missed variants for short- and long-read technologies in medically important genes including CBS, CRYAA, and KCNE1. Our proposed solution improves variant recall in these genes from 8% to 100%. This benchmark will significantly improve the comprehensive characterization of these medically relevant genes and guide new method development.

Publisher

Cold Spring Harbor Laboratory

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