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The Src family kinase Hck regulates mast cell activation by suppressing an inhibitory Src family kinase Lyn
Authors:Hong Hong  Kitaura Jiro  Xiao Wenbin  Horejsi Vaclav  Ra Chisei  Lowell Clifford A  Kawakami Yuko  Kawakami Toshiaki
Affiliation:Division of Cell Biology, La Jolla Institute for Allergy and Immunology, CA 92037, USA.
Abstract:IgE/antigen-dependent mast cell activation plays a central role in immediate hypersensitivity and other allergic reactions. The Src family tyrosine kinase (SFK) Lyn is activated by the cross-linking of high-affinity IgE receptors (Fc{epsilon}RI). Activated Lyn phosphorylates the Fc{epsilon}RI subunits, ß and {gamma}, leading to subsequent activation of various signaling pathways. Lyn also plays a negative regulatory function by activating negative regulatory molecules. Another SFK, Fyn, also contributes to mast cell degranulation by inducing Gab2-dependent microtubule formation. Here we show that a third SFK, Hck, plays a critical role in mast cell activation. Degranulation and cytokine production are reduced in Fc{epsilon}RI-stimulated hck–/– mast cells. The reduced degranulation can be accounted for by defects in Gab2 phosphorylation and microtubule formation. Importantly, Lyn activity is elevated in hck–/– cells, leading to increased phosphorylation of several negative regulators. However, positive regulatory events, such as activation of Syk, Btk, JNK, p38, Akt, and NF-{kappa}B, are substantially reduced in hck–/– mast cells. Analysis of lyn–/–hck–/–, lyn–/–Fc{epsilon}RIß–/–, and hck–/–Fc{epsilon}RIß–/– cells shows that Hck exerts these functions via both Lyn-dependent and Lyn-independent mechanisms. Thus, this study has revealed a hierarchical regulation among SFK members to fine-tune mast cell activation.
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