B cell defects in SLP65/BLNK-deficient mice can be partially corrected by the 
absence of CD22, an inhibitory coreceptor for BCR signaling

Gerlach, Judith; Ghosh, Snigdha; Jumaa, Hassan; Reth, Michael; Wienands, Jürgen; Chan, Andrew C.; Nitschke, Lars

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B cell defects in SLP65/BLNK-deficient mice can be partially corrected by the absence of CD22, an inhibitory coreceptor for BCR signaling

Gerlach, J., Ghosh, S., Jumaa, H., Reth, M., Wienands, J., Chan, A. C., et al. (2003). B cell defects in SLP65/BLNK-deficient mice can be partially corrected by the absence of CD22, an inhibitory coreceptor for BCR signaling. European Journal of Immunology, 33(12), 3418-3426.

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Item Permalink: https://hdl.handle.net/11858/00-001M-0000-002B-94D5-3 Version Permalink: https://hdl.handle.net/11858/00-001M-0000-002B-94D6-1

Genre: Journal Article

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Creators:
Gerlach, Judith, Author
Ghosh, Snigdha, Author
Jumaa, Hassan¹, Author
Reth, Michael¹, Author
Wienands, Jürgen, Author
Chan, Andrew C., Author
Nitschke, Lars, Author

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1Research Group and Chair of Molecular Immunology of the University of Freiburg, Max Planck Institute of Immunobiology and Epigenetics, Max Planck Society, ou_2243645

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Abstract: CD22 is an inhibitory coreceptor for B cell receptor (BCR) signaling. The inhibition is most likely mediated by activation of SHP-1. We found that SLP65/BLNK reaches maximal tyrosine-phosphorylation at earlier time points in CD22^-/- than in wild type B cells upon BCR cross-linking, suggesting that SLP65/BLNK is a substrate of SHP-1. However, in contrast to the defective Ca²⁺ mobilization of SLP65/BLNK^-/- B cells, there was a clear Ca²⁺ response in SLP65/BLNKxCD22 double-deficient B cells. This implies that SLP65/BLNK is not the sole target of SHP-1 in the regulation of the Ca²⁺ signaling strength. While SLP65^-/- mice show several blocks of B cell differentiation, in SLP65/BLNKxCD22 double-deficient mice the maturation block of B cells in the spleen was partially rescued. However, the proliferative responses of B cells from both SLP65/BLNK^-/- and double-deficient mice were defective after IgM- or CD40-stimulation. These results show that SLP65/BLNK is not absolutely essential for Ca²⁺ induction in B cells, because the deficiency of this adapter can be by-passed by the additional deletion of an inhibitory receptor. Furthermore, these experiments suggest that B cell maturation in the spleen is directly dependent on the strength of BCR-derived Ca²⁺ signals.

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Language(s): eng - English

Dates: Date issued: 2003-12

Publication Status: Issued

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Identifiers: eDoc: 125183
ISI: 000187363100022

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Title: European Journal of Immunology

Alternative Title : Eur. J. Immunol.

Source Genre: Journal

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Pages: - Volume / Issue: 33 (12) Sequence Number: - Start / End Page: 3418 - 3426 Identifier: ISSN: 0014-2980