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Cloning and characterization of human Lnk, an adaptor protein with pleckstrin homology and Src homology 2 domains that can inhibit T cell activation

被引:87
作者
Li, YJ
He, XQ
Schembri-King, J
Jakes, S
Hayashi, J
机构
[1] Univ Maryland, Sch Pharm, Baltimore, MD 21201 USA
[2] Boehringer Ingelheim, Ctr Res & Dev, Ridgefield, CT 06877 USA
来源
JOURNAL OF IMMUNOLOGY | 2000年 / 164卷 / 10期
关键词
D O I
10.4049/jimmunol.164.10.5199
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Lnk was originally cloned from a rat lymph node cDNA library and shown to participate in T cell signaling. Human Lnk (hLnk) was cloned by screening a Jurkat cell cDNA library. hLnk has a calculated molecular mass of 63 kDa, and its deduced amino acid sequence indicates the presence of an N-terminal proline-rich region, a pleckstrin homology domain, and a Src homology 2 domain. When expressed in COS cells, hLnk migrates with an apparent molecular mass of 75 kDa. Confocal fluorescence microscope analysis indicates that in COS cells transfected with an expression vector encoding a chimeric Lnk-green fluorescent protein, hLnk is found at the juxtanuclear compartment and also appears to be localized at the plasma membrane. Lnk is tyrosine-phosphorylated by p56(lck). Following phosphorylation, p56(lck) binds to tyrosine-phosphorylated hLnk through its Src homology 2 domain. In COS cells cotransfected with hLnk, p56(lck), and CD8-zeta. hLnk associated,vith tyrosine-phosphorylated TCR zeta-chain through its Src homology 2 domain. The overexpression of Lnk in Jurkat cells led to an inhibition of anti-CD3 mediated NF-AT-Luc activation. Our study reveals a potentially new mechanism of T cell-negative regulation.
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页码:5199 / 5206
页数:8
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