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Identification of an anti-idiotypic antibody that defines a B-cell subset(s) producing xenoantibodies in primates.

Authors :
Fischer-Lougheed, Jacqueline
Gregory, Clare
White, Zena
Shulkin, Irina
Gunthart, Mirja
Kearns-Jonker, Mary
Source :
Immunology; Mar2008, Vol. 123 Issue 3, p390-397, 8p, 5 Diagrams, 3 Graphs
Publication Year :
2008

Abstract

Synthetic anti-idiotypic antibodies represent a potentially valuable tool for the isolation and characterization of B cells that produce xenoantibodies. An anti-idiotypic antibody that binds to a subset of B cells producing antibodies encoded by the variable-region heavy chain 3 (V<subscript>H</subscript>3) germline genes DP35 [immunoglobulin variable-region heavy chain 3-11 (IGHV3-11)], DP-53 and DP-54 plus a small number of V<subscript>H</subscript>4 gene-encoded antibodies in humans has recently been identified. These germline progenitors also encode xenoantibodies in humans. We tested whether the small, clearly defined group of B cells identified with this anti-idiotypic antibody produce xenoantibodies in non-human primates mounting active immune responses to porcine xenografts. Peripheral blood B cells were sorted by flow cytometry on the basis of phenotype, and cDNA libraries were prepared from each of these sorted groups of cells. Immunoglobulin V<subscript>H</subscript> gene libraries were prepared from the sorted cells, and the V<subscript>H</subscript> genes expressed in each of the sorted groups were identified by nucleic acid sequencing. Our results indicate that xenoantibody-producing peripheral blood B cells, defined on the basis of binding to fluorescein isothiocyanate (FITC)-conjugated galactose α(1,3) galactose–bovine serum albumin (Gal-BSA) and the anti-idiotypic antibody 2G10, used the IGHV3-11 germline gene to encode xenoantibodies and were phenotypically CD11b<superscript>+</superscript> (Mac-1<superscript>+</superscript>) and CD5<superscript>–</superscript>. This novel reagent may be used in numerous applications including definition of xenoantibody-producing B-cell subsets in humans and non-human primates and immunosuppression by depletion of B cells producing anti-Gal xenoantibodies. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
00192805
Volume :
123
Issue :
3
Database :
Complementary Index
Journal :
Immunology
Publication Type :
Academic Journal
Accession number :
28651775
Full Text :
https://doi.org/10.1111/j.1365-2567.2007.02704.x