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Publication : Syk tyrosine kinase is critical for B cell antibody responses and memory B cell survival.

First Author  Ackermann JA Year  2015
Journal  J Immunol Volume  194
Issue  10 Pages  4650-6
PubMed ID  25862820 Mgi Jnum  J:324122
Mgi Id  MGI:6208359 Doi  10.4049/jimmunol.1500461
Citation  Ackermann JA, et al. (2015) Syk tyrosine kinase is critical for B cell antibody responses and memory B cell survival. J Immunol 194(10):4650-6
abstractText  Signals from the BCR are required for Ag-specific B cell recruitment into the immune response. Binding of Ag to the BCR induces phosphorylation of immune receptor tyrosine-based activation motifs in the cytoplasmic domains of the CD79a and CD79b signaling subunits, which subsequently bind and activate the Syk protein tyrosine kinase. Earlier work with the DT40 chicken B cell leukemia cell line showed that Syk was required to transduce BCR signals to proximal activation events, suggesting that Syk also plays an important role in the activation and differentiation of primary B cells during an immune response. In this study, we show that Syk-deficient primary mouse B cells have a severe defect in BCR-induced activation, proliferation, and survival. Furthermore, we demonstrate that Syk is required for both T-dependent and T-independent Ab responses, and that this requirement is B cell intrinsic. In the absence of Syk, Ag fails to induce differentiation of naive B cells into germinal center B cells and plasma cells. Finally, we show that the survival of existing memory B cells is dependent on Syk. These experiments demonstrate that Syk plays a critical role in multiple aspects of B cell Ab responses.
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