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Shark IgW C region diversification through RNA processing and isotype switching
JournalArticle (Originalarbeit in einer wissenschaftlichen Zeitschrift)
 
ID 2309870
Author(s) Zhang, C; Du Pasquier, L; Hsu, E
Author(s) at UniBasel Du Pasquier, Louis
Year 2013
Title Shark IgW C region diversification through RNA processing and isotype switching
Journal Journal of immunology
Volume 191
Number 6
Pages / Article-Number 3410-3418
Abstract

Sharks and skates represent the earliest vertebrates with an adaptive immune system based on lymphocyte Ag receptors generated by V(D)J recombination. Shark B cells express two classical Igs, IgM and IgW, encoded by an early, alternative gene organization consisting of numerous autonomous miniloci, where the individual gene cluster carries a few rearranging gene segments and one C region, mu or omega. We have characterized eight distinct Ig miniloci encoding the nurse shark omega H chain. Each cluster consists of VH, D, and JH segments and six to eight C domain exons. Two interspersed secretory exons, in addition to the 3'-most C exon with tailpiece, provide the gene cluster with the ability to generate at least six secreted isoforms that differ as to polypeptide length and C domain combination. All clusters appear to be functional, as judged by the capability for rearrangement and absence of defects in the deduced amino acid sequence. We previously showed that IgW VDJ can perform isotype switching to mu C regions; in this study, we found that switching also occurs between v clusters. Thus, C region diversification for any IgW VDJ can take place at the DNA level by switching to other omega or mu C regions, as well as by RNA processing to generate different C isoforms. The wide array of pathogens recognized by Abs requires different disposal pathways, and our findings demonstrate complex and unique pathways for C effector function diversity that evolved independently in cartilaginous fishes.

Publisher American Assoc. of Immunologists
ISSN/ISBN 0022-1767
edoc-URL http://edoc.unibas.ch/dok/A6212080
Full Text on edoc No
Digital Object Identifier DOI 10.4049/jimmunol.1301257
PubMed ID http://www.ncbi.nlm.nih.gov/pubmed/23935192
ISI-Number WOS:000324206900059
Document type (ISI) Article
 
   

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29/04/2024