Genetic variation in the immunoglobulin heavy chain locus shapes the human antibody repertoire

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作者
Oscar L. Rodriguez
Yana Safonova
Catherine A. Silver
Kaitlyn Shields
William S. Gibson
Justin T. Kos
David Tieri
Hanzhong Ke
Katherine J. L. Jackson
Scott D. Boyd
Melissa L. Smith
Wayne A. Marasco
Corey T. Watson
机构
[1] University of Louisville School of Medicine,Department of Biochemistry and Molecular Genetics
[2] Johns Hopkins University,Department of Computer Science
[3] Harvard Medical School,Department of Cancer Immunology and Virology, Dana
[4] Department of Medicine,Farber Cancer Institute
[5] Harvard Medical School,Department of Pathology
[6] The Garvan Institute of Medical Research,undefined
[7] Stanford University School of Medicine,undefined
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Variation in the antibody response has been linked to differential outcomes in disease, and suboptimal vaccine and therapeutic responsiveness, the determinants of which have not been fully elucidated. Countering models that presume antibodies are generated largely by stochastic processes, we demonstrate that polymorphisms within the immunoglobulin heavy chain locus (IGH) impact the naive and antigen-experienced antibody repertoire, indicating that genetics predisposes individuals to mount qualitatively and quantitatively different antibody responses. We pair recently developed long-read genomic sequencing methods with antibody repertoire profiling to comprehensively resolve IGH genetic variation, including novel structural variants, single nucleotide variants, and genes and alleles. We show that IGH germline variants determine the presence and frequency of antibody genes in the expressed repertoire, including those enriched in functional elements linked to V(D)J recombination, and overlapping disease-associated variants. These results illuminate the power of leveraging IGH genetics to better understand the regulation, function, and dynamics of the antibody response in disease.
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