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      Expressed antibody repertoires in human cord blood cells: 454 sequencing and IMGT/HighV-QUEST analysis of germline gene usage, junctional diversity, and somatic mutations

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          Abstract

          Human cord blood cell-derived IgM antibodies are important for the neonate immune responses and construction of germline-based immunoglobulin libraries. Several previous studies of a relatively small number of sequences found that they exhibit restrictions in the usage of germline genes and in the diversity of the variable heavy chain complementarity determining region 3 compared to adults. To further characterize such restrictions on a larger scale and to compare the early B-cell diversity to adult IgM repertoires, we performed 454 sequencing and IMGT/HighV-QUEST analysis of cord blood IG libraries from two babies and determined germline gene usage, V-D-J rearrangement, VHCDR3 diversity, and somatic mutations to characterize human neonate repertoire. Most of the germline subgroups were identified with frequencies comparable to those present in the adult IgM repertoire except for the IGHV1–2 gene that was preferentially expressed in the cord blood cells. The gene usage diversity contributed to 1,430 unique IGH V-D-J rearrangement patterns while the exonuclease trimming and N region addition at the V-D-J junctions along with gene diversity created a wide range of VHCDR3 with different lengths and sequence variability. We observed a lower degree of somatic mutations in the CDR and framework regions of antibodies from cord blood cells compared to adults. These results provide insights into the characteristics of human cord blood antibody repertoires, which have gene usage diversity and VHCDR3 lengths similar to that of the adult IgM repertoire but differ significantly in some of the gene usages, V-D-J rearrangements, junctional diversity, and somatic mutations.

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          Author and article information

          Contributors
          Journal
          0420404
          4198
          Immunogenetics
          Immunogenetics
          Immunogenetics
          0093-7711
          1432-1211
          4 January 2020
          27 December 2011
          May 2012
          10 January 2020
          : 64
          : 5
          : 337-350
          Affiliations
          Protein Interactions Group, Center for Cancer Research, Nanobiology Program, National Cancer Institute (NCI)-Frederick, National Institutes of Health (NIH), Bldg 469, Rm 150B, Frederick, MD 21702, USA
          Basic Research Program, Science Applications International, Corporation-Frederick, Inc., NCI-Frederick, Frederick, MD 21702, USA
          Protein Interactions Group, Center for Cancer Research, Nanobiology Program, National Cancer Institute (NCI)-Frederick, National Institutes of Health (NIH), Bldg 469, Rm 150B, Frederick, MD 21702, USA
          1901 Harpers Court, Frederick, MD 21702, USA
          The Laboratory of Molecular Technology, Science Applications, International Corporation-Frederick, Inc., NCI-Frederick, Frederick, MD 21702, USA
          Protein Interactions Group, Center for Cancer Research, Nanobiology Program, National Cancer Institute (NCI)-Frederick, National Institutes of Health (NIH), Bldg 469, Rm 150B, Frederick, MD 21702, USA
          Basic Research Program, Science Applications International, Corporation-Frederick, Inc., NCI-Frederick, Frederick, MD 21702, USA
          Protein Interactions Group, Center for Cancer Research, Nanobiology Program, National Cancer Institute (NCI)-Frederick, National Institutes of Health (NIH), Bldg 469, Rm 150B, Frederick, MD 21702, USA
          Author notes
          Article
          PMC6953429 PMC6953429 6953429 nihpa1065963
          10.1007/s00251-011-0595-8
          6953429
          22200891
          5bee4cad-5915-431b-b863-aadcf35b51f2
          History
          Categories
          Article

          Immunoglobulin,454 Sequencing,IMGT/HighV-QUEST,Human cord blood,Antibodyome,Antibody library,Antibody repertoire,IgM

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