Literature DB >> 17641032

Ig heavy chain promotes mature B cell survival in the absence of light chain.

Pedro Geraldes1, Michelle Rebrovich, Kai Herrmann, Jamie Wong, Hans-Martin Jäck, Matthias Wabl, Marilia Cascalho.   

Abstract

Survival of mature B cells is thought to depend on the BCR signaling (BCR) because ablation of either H chain (HC) expression or BCR signaling causes B cells to rapidly disappear. Whether a complete BCR is required for survival of mature B cells is not known. To address this question, we generated a mouse in which we can repress the expression of a transgenic Ig L chain (IgL) by doxycycline (IgL-repressible mouse). Repression of IgL abrogated expression. Surprisingly, however, IgL-negative B cells survived longer than 14 wk, expressed signal-competent HC on the cell's surface, and active unfolded protein response factors. Like postgerminal center B cells, IgL-negative B cells were small lymphocytes, not dividing and expressed Bcl-6. Our results indicate that expression of unpaired HC, as it may occur as a consequence of Ag ligation, somatic hypermutation, or receptor editing, facilitates the survival of cells either by inducing receptor signaling or by inducing unfolded protein response and/or the expression of survival genes such as Bcl-6.

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Year:  2007        PMID: 17641032     DOI: 10.4049/jimmunol.179.3.1659

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


  6 in total

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5.  One-step generation of monoclonal B cell receptor mice capable of isotype switching and somatic hypermutation.

Authors:  Johanne T Jacobsen; Luka Mesin; Styliani Markoulaki; Ariën Schiepers; Cecília B Cavazzoni; Djenet Bousbaine; Rudolf Jaenisch; Gabriel D Victora
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6.  Durable targeting of B-lymphocytes in living mice.

Authors:  M Cascalho; D Huynh; A R Lefferts; L Stein; T Lanigan; J Decker; L D Shea; J L Platt
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  6 in total

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