Literature DB >> 20495067

Individual variation in the germline Ig gene repertoire inferred from variable region gene rearrangements.

Scott D Boyd1, Bruno A Gaëta, Katherine J Jackson, Andrew Z Fire, Eleanor L Marshall, Jason D Merker, Jay M Maniar, Lyndon N Zhang, Bita Sahaf, Carol D Jones, Birgitte B Simen, Bozena Hanczaruk, Khoa D Nguyen, Kari C Nadeau, Michael Egholm, David B Miklos, James L Zehnder, Andrew M Collins.   

Abstract

Individual variation in the Ig germline gene repertoire leads to individual differences in the combinatorial diversity of the Ab repertoire, but the study of such variation has been problematic. The application of high-throughput DNA sequencing to the study of rearranged Ig genes now makes this possible. The sequencing of thousands of VDJ rearrangements from an individual, either from genomic DNA or expressed mRNA, should allow their germline IGHV, IGHD, and IGHJ repertoires to be inferred. In addition, where previously mere glimpses of diversity could be gained from sequencing studies, new large data sets should allow the rearrangement frequency of different genes and alleles to be seen with clarity. We analyzed the DNA of 108,210 human IgH chain rearrangements from 12 individuals and determined their individual IGH genotypes. The number of reportedly functional IGHV genes and allelic variants ranged from 45 to 60, principally because of variable levels of gene heterozygosity, and included 14 previously unreported IGHV polymorphisms. New polymorphisms of the IGHD3-16 and IGHJ6 genes were also seen. At heterozygous loci, remarkably different rearrangement frequencies were seen for the various IGHV alleles, and these frequencies were consistent between individuals. The specific alleles that make up an individual's Ig genotype may therefore be critical in shaping the combinatorial repertoire. The extent of genotypic variation between individuals is highlighted by an individual with aplastic anemia who appears to lack six contiguous IGHD genes on both chromosomes. These deletions significantly alter the potential expressed IGH repertoire, and possibly immune function, in this individual.

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Year:  2010        PMID: 20495067      PMCID: PMC4281569          DOI: 10.4049/jimmunol.1000445

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  26 in total

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Review 4.  Structural variation in the human genome.

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Journal:  Science       Date:  2001-02-16       Impact factor: 47.728

9.  VBASE2, an integrative V gene database.

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10.  Accuracy and quality of massively parallel DNA pyrosequencing.

Authors:  Susan M Huse; Julie A Huber; Hilary G Morrison; Mitchell L Sogin; David Mark Welch
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  125 in total

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5.  Epitope-specific human influenza antibody repertoires diversify by B cell intraclonal sequence divergence and interclonal convergence.

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Journal:  J Immunol       Date:  2011-08-31       Impact factor: 5.422

6.  Automated analysis of high-throughput B-cell sequencing data reveals a high frequency of novel immunoglobulin V gene segment alleles.

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Review 7.  The evolution within us.

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8.  Characterization of human IgG repertoires in an acute HIV-1 infection.

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9.  Identification of human neutralizing antibodies against MERS-CoV and their role in virus adaptive evolution.

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10.  Clustering-based identification of clonally-related immunoglobulin gene sequence sets.

Authors:  Zhiliang Chen; Andrew M Collins; Yan Wang; Bruno A Gaëta
Journal:  Immunome Res       Date:  2010-09-27
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