Automated typing of red blood cell and platelet antigens: a whole-genome sequencing study

William J Lane; Connie M Westhoff; Nicholas S Gleadall; Maria Aguad; Robin Smeland-Wagman; Sunitha Vege; Daimon P Simmons; Helen H Mah; Matthew S Lebo; Klaudia Walter; Nicole Soranzo; Emanuele Di Angelantonio; John Danesh; David J Roberts; Nick A Watkins; Willem H Ouwehand; Adam S Butterworth; Richard M Kaufman; Heidi L Rehm; Leslie E Silberstein; Robert C Green; MedSeq Project

doi:10.1016/S2352-3026(18)30053-X

Automated typing of red blood cell and platelet antigens: a whole-genome sequencing study

Lancet Haematol. 2018 Jun;5(6):e241-e251. doi: 10.1016/S2352-3026(18)30053-X. Epub 2018 May 17.

Authors

William J Lane¹, Connie M Westhoff², Nicholas S Gleadall³, Maria Aguad⁴, Robin Smeland-Wagman⁴, Sunitha Vege², Daimon P Simmons⁴, Helen H Mah⁴, Matthew S Lebo⁵, Klaudia Walter⁶, Nicole Soranzo⁷, Emanuele Di Angelantonio⁸, John Danesh⁹, David J Roberts¹⁰, Nick A Watkins¹¹, Willem H Ouwehand¹², Adam S Butterworth⁸, Richard M Kaufman⁴, Heidi L Rehm¹³, Leslie E Silberstein¹⁴, Robert C Green¹⁵; MedSeq Project

Collaborators

MedSeq Project:
David W Bates, Carrie Blout, Kurt D Christensen, Allison L Cirino, Carolyn Y Ho, Joel B Krier, Lisa S Lehmann, Calum A MacRae, Cynthia C Morton, Denise L Perry, Christine E Seidman, Shamil R Sunyaev, Jason L Vassy, Erica Schonman, Tiffany Nguyen, Eleanor Steffens, Wendi Nicole Betting, Samuel J Aronson, Ozge Ceyhan-Birsoy, Kalotina Machini, Heather M McLaughlin, Danielle R Azzariti, Ellen A Tsai, Jennifer Blumenthal-Barby, Lindsay Z Feuerman, Amy L McGuire, Kaitlyn Lee, Jill O Robinson, Melody J Slashinski, Pamela M Diamond, Kelly Davis, Peter A Ubel, Peter Kraft, J Scott Roberts, Judy E Garber, Tina Hambuch, Michael F Murray, Isaac Kohane, Sek Won Kong

Affiliations

¹ Department of Pathology, Brigham and Women's Hospital, Boston, MA, USA; Harvard Medical School, Boston, MA, USA. Electronic address: wlane@bwh.harvard.edu.
² New York Blood Center, New York, NY, USA.
³ Department of Haematology, University of Cambridge, Cambridge, UK; National Health Service (NHS) Blood and Transplant, Cambridge, UK.
⁴ Department of Pathology, Brigham and Women's Hospital, Boston, MA, USA.
⁵ Department of Pathology, Brigham and Women's Hospital, Boston, MA, USA; Harvard Medical School, Boston, MA, USA; Laboratory for Molecular Medicine, Boston, MA, USA; Partners Personalized Medicine, Boston, MA, USA.
⁶ Wellcome Trust Sanger Institute, Hinxton, UK.
⁷ Department of Haematology, University of Cambridge, Cambridge, UK; Wellcome Trust Sanger Institute, Hinxton, UK; Cambridge Substantive Site, Health Data Research UK, Wellcome Genome Campus, Hinxton, UK.
⁸ Medical Research Council and British Heart Foundation Cardiovascular Epidemiology Unit, University of Cambridge, Cambridge, UK; National Institute for Health Research Blood and Transplant Research Unit in Donor Health and Genomics, University of Cambridge, Cambridge, UK; Cambridge Substantive Site, Health Data Research UK, Wellcome Genome Campus, Hinxton, UK.
⁹ Medical Research Council and British Heart Foundation Cardiovascular Epidemiology Unit, University of Cambridge, Cambridge, UK; National Institute for Health Research Blood and Transplant Research Unit in Donor Health and Genomics, University of Cambridge, Cambridge, UK; Department of Public Health and Primary Care, and British Heart Foundation Cambridge Centre of Excellence, Department of Medicine, University of Cambridge, Cambridge, UK; Wellcome Trust Sanger Institute, Hinxton, UK; Cambridge Substantive Site, Health Data Research UK, Wellcome Genome Campus, Hinxton, UK.
¹⁰ National Institute for Health Research Blood and Transplant Research Unit in Donor Health and Genomics, University of Cambridge, Cambridge, UK; NHS Blood and Transplant-Oxford Centre, Oxford, UK; Biomedical Research Centre Haematology Theme and Radcliffe Department of Medicine, University of Oxford, Oxford, UK.
¹¹ National Health Service (NHS) Blood and Transplant, Cambridge, UK.
¹² Department of Haematology, University of Cambridge, Cambridge, UK; Department of Public Health and Primary Care, and British Heart Foundation Cambridge Centre of Excellence, Department of Medicine, University of Cambridge, Cambridge, UK; National Health Service (NHS) Blood and Transplant, Cambridge, UK; NHS Blood and Transplant-Oxford Centre, Oxford, UK.
¹³ Harvard Medical School, Boston, MA, USA; Laboratory for Molecular Medicine, Boston, MA, USA; Partners Personalized Medicine, Boston, MA, USA; Department of Medicine, Massachusetts General Hospital, Boston, MA, USA; Broad Institute of Massachusetts Institute of Technology and Harvard, Boston, MA, USA.
¹⁴ Division of Transfusion Medicine, Brigham and Women's Hospital, Boston, MA, USA; Harvard Medical School, Boston, MA, USA.
¹⁵ Division of Genetics, Department of Medicine, Brigham and Women's Hospital, Boston, MA, USA; Harvard Medical School, Boston, MA, USA; Partners Personalized Medicine, Boston, MA, USA; Broad Institute of Massachusetts Institute of Technology and Harvard, Boston, MA, USA.

Abstract

Background: There are more than 300 known red blood cell (RBC) antigens and 33 platelet antigens that differ between individuals. Sensitisation to antigens is a serious complication that can occur in prenatal medicine and after blood transfusion, particularly for patients who require multiple transfusions. Although pre-transfusion compatibility testing largely relies on serological methods, reagents are not available for many antigens. Methods based on single-nucleotide polymorphism (SNP) arrays have been used, but typing for ABO and Rh-the most important blood groups-cannot be done with SNP typing alone. We aimed to develop a novel method based on whole-genome sequencing to identify RBC and platelet antigens.

Methods: This whole-genome sequencing study is a subanalysis of data from patients in the whole-genome sequencing arm of the MedSeq Project randomised controlled trial (NCT01736566) with no measured patient outcomes. We created a database of molecular changes in RBC and platelet antigens and developed an automated antigen-typing algorithm based on whole-genome sequencing (bloodTyper). This algorithm was iteratively improved to address cis-trans haplotype ambiguities and homologous gene alignments. Whole-genome sequencing data from 110 MedSeq participants (30 × depth) were used to initially validate bloodTyper through comparison with conventional serology and SNP methods for typing of 38 RBC antigens in 12 blood-group systems and 22 human platelet antigens. bloodTyper was further validated with whole-genome sequencing data from 200 INTERVAL trial participants (15 × depth) with serological comparisons.

Findings: We iteratively improved bloodTyper by comparing its typing results with conventional serological and SNP typing in three rounds of testing. The initial whole-genome sequencing typing algorithm was 99·5% concordant across the first 20 MedSeq genomes. Addressing discordances led to development of an improved algorithm that was 99·8% concordant for the remaining 90 MedSeq genomes. Additional modifications led to the final algorithm, which was 99·2% concordant across 200 INTERVAL genomes (or 99·9% after adjustment for the lower depth of coverage).

Interpretation: By enabling more precise antigen-matching of patients with blood donors, antigen typing based on whole-genome sequencing provides a novel approach to improve transfusion outcomes with the potential to transform the practice of transfusion medicine.

Funding: National Human Genome Research Institute, Doris Duke Charitable Foundation, National Health Service Blood and Transplant, National Institute for Health Research, and Wellcome Trust.

MeSH terms

ABO Blood-Group System / classification
ABO Blood-Group System / genetics*
Adolescent
Adult
Aged
Aged, 80 and over
Algorithms
Antigens, Human Platelet / classification
Antigens, Human Platelet / genetics*
Blood Grouping and Crossmatching / methods*
Blood Platelets / immunology
Databases, Genetic
Erythrocytes / immunology
Genome, Human
Humans
Middle Aged
Randomized Controlled Trials as Topic
Rh-Hr Blood-Group System / classification
Rh-Hr Blood-Group System / genetics*
Whole Genome Sequencing*
Young Adult

Substances

ABO Blood-Group System
Antigens, Human Platelet
RHCE protein, human
Rh-Hr Blood-Group System

Abstract

MeSH terms

Substances

Grants and funding