A deep learning method for HLA imputation and trans-ethnic MHC fine-mapping of type 1 diabetes

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作者
Tatsuhiko Naito
Ken Suzuki
Jun Hirata
Yoichiro Kamatani
Koichi Matsuda
Tatsushi Toda
Yukinori Okada
机构
[1] Osaka University Graduate School of Medicine,Department of Statistical Genetics
[2] The University of Tokyo,Department of Neurology, Graduate School of Medicine
[3] Pharmaceutical Discovery Research Laboratories,Laboratory of Complex Trait Genomics, Department of Computational Biology and Medical Sciences, Graduate School of Frontier Sciences
[4] Teijin Pharma Limited,Laboratory of Clinical Genome Sequencing, Department of Computational Biology and Medical Sciences, Graduate School of Frontier Sciences
[5] The University of Tokyo,Laboratory of Statistical Immunology, Immunology Frontier Research Center (WPI
[6] The University of Tokyo,IFReC)
[7] Osaka University,Integrated Frontier Research for Medical Science Division, Institute for Open and Transdisciplinary Research Initiatives
[8] Osaka University,undefined
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摘要
Conventional human leukocyte antigen (HLA) imputation methods drop their performance for infrequent alleles, which is one of the factors that reduce the reliability of trans-ethnic major histocompatibility complex (MHC) fine-mapping due to inter-ethnic heterogeneity in allele frequency spectra. We develop DEEP*HLA, a deep learning method for imputing HLA genotypes. Through validation using the Japanese and European HLA reference panels (n = 1,118 and 5,122), DEEP*HLA achieves the highest accuracies with significant superiority for low-frequency and rare alleles. DEEP*HLA is less dependent on distance-dependent linkage disequilibrium decay of the target alleles and might capture the complicated region-wide information. We apply DEEP*HLA to type 1 diabetes GWAS data from BioBank Japan (n = 62,387) and UK Biobank (n = 354,459), and successfully disentangle independently associated class I and II HLA variants with shared risk among diverse populations (the top signal at amino acid position 71 of HLA-DRβ1; P = 7.5 × 10−120). Our study illustrates the value of deep learning in genotype imputation and trans-ethnic MHC fine-mapping.
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