作者
Yongjian Wu, Monica JS Nadler, Laurie A Brennan, Gerald D Gish, John F Timms, Noemi Fusaki, Jenny Jongstra-Bilen, Nobuhiko Tada, Tony Pawson, Joan Wither, Benjamin G Neel, Nobumichi Hozumi
发表日期
1998/9/10
期刊
Current biology
卷号
8
期号
18
页码范围
1009-1017
出版商
Elsevier
简介
Background: Signals from the B-cell antigen receptor (BCR) help to determine B-cell fate, directing either proliferation, differentiation, or growth arrest/apoptosis. The protein tyrosine phosphatase SHP-1 is known to regulate the strength of BCR signaling. Although the B-cell co-receptor CD22 binds SHP-1, B cells in CD22-deficient mice are much less severely affected than those in SHP-1-deficient mice, suggesting that SHP-1 may also regulate B-cell signaling by affecting other signaling molecules. Moreover, direct substrates of SHP-1 have not been identified in any B-cell signaling pathway.
Results: We identified the B-cell transmembrane protein CD72 as a new SHP-1 binding protein and as an in vivo substrate of SHP-1 in B cells. We also defined the binding sites for SHP-1 and the adaptor protein Grb2 on CD72. Tyrosine phosphorylation of CD72 correlated strongly with BCR-induced growth arrest/apoptosis in B …
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