GRAMM: A new method for analysis of HLA in families

Author:

Ansbacher‐Feldman Zuriya1ORCID,Israeli Sapir1ORCID,Maiers Martin23ORCID,Gragert Loren234ORCID,De Santis Dianne5ORCID,Israeli Moshe67ORCID,Louzoun Yoram1ORCID

Affiliation:

1. Department of Mathematics Bar‐Ilan University Ramat Gan Israel

2. Center for Blood and Marrow Transplant Research Minneapolis Minnesota USA

3. National Marrow Donor Program/Be The Match Minneapolis Minnesota USA

4. Department of Pathology and Laboratory Medicine, Tulane Cancer Center Tulane University School of Medicine New Orleans Louisiana USA

5. Department of Clinical Immunology, PathWest Fiona Stanley Hospital Perth Australia

6. Tissue Typing Laboratory Beilinson Hospital, Rabin Medical Center Petach‐Tikva Israel

7. Department of Digital Medical Technologies Holon Institute of Technology Holon Israel

Abstract

Recently, haplo‐identical transplantation with multiple HLA mismatches has become a viable option for stem cell transplants. Haplotype sharing detection requires the imputation of donor and recipient. We show that even in high‐resolution typing when all alleles are known, there is a 15% error rate in haplotype phasing, and even more in low‐resolution typings. Similarly, in related donors, the parents' haplotypes should be imputed to determine what haplotype each child inherited. We propose graph‐based family imputation (GRAMM) to phase alleles in family pedigree HLA typing data, and in mother‐cord blood unit pairs. We show that GRAMM has practically no phasing errors when pedigree data are available. We apply GRAMM to simulations with different typing resolutions as well as paired cord‐mother typings, and show very high phasing accuracy, and improved allele imputation accuracy. We use GRAMM to detect recombination events and show that the rate of falsely detected recombination events (false‐positive rate) in simulations is very low. We then apply recombination detection to typed families to estimate the recombination rate in Israeli and Australian population datasets. The estimated recombination rate has an upper bound of 10%–20% per family (1%–4% per individual).

Publisher

Wiley

Subject

Genetics,Immunology,Immunology and Allergy

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