Title of article
Structural requirements of Syk kinase for Fcγ receptor– phagocytosis
Author/Authors
Sharon Hunter، نويسنده , , Norihito Sato، نويسنده , , Moo-Kyung Kim، نويسنده , , Zhenyu Huang، نويسنده , , David H. Chu، نويسنده , , Jong-Gu Park، نويسنده , , Alan D. Schreiber، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 1999
Pages
10
From page
875
To page
884
Abstract
The tyrosine kinase Syk plays a critical role in the phagocytic pathway mediated by Fcγ receptors (FcγR). In transfected COS1 cells co-expression of Syk enhances FcγR mediated phagocytosis. The other member of the Syk kinase family, the highly homologous tyrosine kinase Zap70, also plays a role in signaling by immunoglobulin gene family receptors, but does not increase the phagocytic efficiency of FcγRs. The homologous tandem SH2 and kinase domains of Syk and Zap70 are separated by a nonhomologous region referred to as the unique domain. Zap70’s inability to enhance phagocytosis was not due to unique domain tyrosine 292, previously implicated in negative regulation of Zap70 function. We determined the regions of Syk important for its interaction with the phagocytic pathway. An intact kinase domain was required for Syk’s effect on phagocytosis. Furthermore, the Syk variant SykB, lacking 23 amino acids in the unique region, signaled for phagocytosis as efficiently as did Syk. We then constructed exchange chimeras between Syk and Zap70 and determined the contributions of the SH2, unique and kinase domains to phagocytic signaling. Our data suggest that the Syk kinase domain, which has high intrinsic kinase activity, is important for facilitating phagocytic signaling by FcγRI and FcγRIIIA.
Keywords
Receptors—Signaling—Tyrosine kinases—Phagocytosis
Journal title
Experimental Hematology
Serial Year
1999
Journal title
Experimental Hematology
Record number
513044
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