Literature DB >> 1376351

Development and function of the early B cell repertoire.

J F Kearney1, J Bartels, A M Hamilton, A Lehuen, N Solvason, M Vakil.   

Abstract

The early B cell repertoire is characterized by extensive interconnectivity, autoreactivity and multispecificity. Our preliminary sequence analysis of some of the idiotype specific antibodies is beginning to provide molecular clues to explain the observed multireactivity and the expression of shared idiotypic determinants on immunoglobulins of early B cells. The VH gene rearrangements analyzed are typical of the early pre-B cell and CD5 B cell repertoire. Some of these include shared or identical CDR3 regions resulting from the use of germline VH, D and JH gene segments in the absence of N region addition. As previously described, the most D proximal VH genes are also used most frequently. Collectively these genetic restrictions, together with the lack of somatic mutation, suggest that the characteristic self reactivity of the early B cell repertoire is related to the expression of germline gene segments and limited use of diversification mechanisms. It has also been possible for the first time to isolate hybridomas secreting functional IgM molecules which use the most D proximal VH gene, VH81X. These antibodies and another example from the VH7183 family have a broad multireactivity pattern possibly because of the presence of an unusually high number of charged amino acid groups present in the VH region. These findings are preliminary and more extensive studies are needed to establish if these groups are responsible for the highly cross-reactive nature of these antibodies. Nevertheless, these unusual characteristics signify a unique role for antibodies expressing this VH gene during B cell development. It is also clear that the observed anti-lymphocyte reactivity, another feature of the newborn repertoire, is the result of the prevalence of B cells using similar if not identical VHDJH genes and DJH joins. The development of these B cells appears to occur consistently in early ontogeny and, again, are not found in conventional splenic B cells obtained from the normal adult. Understanding the functional significance of the early appearance of these antibodies may help to clarify and understand their role during development as well as in autoimmunity. We propose that the unique self reactive nature of the early repertoire provides a pattern within which self-assertiveness develops and results in the establishment of the adult repertoire. In doing so, dominant clones are established which may or may not be within, but whose selection and differentiation is directed by the CD5 B cell subset.(ABSTRACT TRUNCATED AT 400 WORDS)

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Year:  1992        PMID: 1376351     DOI: 10.3109/08830189209055577

Source DB:  PubMed          Journal:  Int Rev Immunol        ISSN: 0883-0185            Impact factor:   5.311


  10 in total

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2.  Isolation of germinal centerlike events from human spleen RNA. Somatic hypermutation of a clonally related VH6DJH rearrangement expressed with IgM, IgG, and IgA.

Authors:  W S Varade; R A Insel
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Review 3.  Balancing immunity and tolerance: deleting and tuning lymphocyte repertoires.

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Journal:  Am J Pathol       Date:  1995-07       Impact factor: 4.307

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7.  Omental immune aggregates and tumor metastasis within the peritoneal cavity.

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8.  Characterization of omental immune aggregates during establishment of a latent gammaherpesvirus infection.

Authors:  Kathleen S Gray; Christopher M Collins; Samuel H Speck
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9.  Repertoire-based selection into the marginal zone compartment during B cell development.

Authors:  John B Carey; Chantelle S Moffatt-Blue; Lisa C Watson; Amanda L Gavin; Ann J Feeney
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10.  Mapping an epitope in EBNA-1 that is recognized by monoclonal antibodies to EBNA-1 that cross-react with dsDNA.

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  10 in total

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