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p56lck与CD4的结合对于CD4与TCR/CD3复合物之间的相互作用以及最佳抗原刺激是必需的。

p56lck association with CD4 is required for the interaction between CD4 and the TCR/CD3 complex and for optimal antigen stimulation.

作者信息

Collins T L, Uniyal S, Shin J, Strominger J L, Mittler R S, Burakoff S J

机构信息

Division of Pediatric Oncology, Dana Farber Cancer Institute, Boston, MA 02115.

出版信息

J Immunol. 1992 Apr 1;148(7):2159-62.

PMID:1532002
Abstract

By fluorescence resonance energy transfer, we have previously demonstrated that upon anti-CD3 mAb-mediated activation of a murine T cell hybridoma expressing human CD4, CD4 moves into close association with the TCR/CD3 complex. It was shown that this association between CD4 and the TCR/CD3 complex was dependent upon the presence of an intact CD4 cytoplasmic domain. We have now expressed, in a murine T cell hybridoma, mutated forms of CD4 containing cysteine to serine point mutations at positions 420, 422, or 430. The mutations at positions 420 and 422, but not 430, abolish association with p56lck. By using fluorescence resonance energy transfer, we demonstrate that mutations of CD4 which fail to interact with p56lck are unable to associate with the TCR/CD3 complex under conditions in which wild-type CD4 and the 430 mutant CD4 do associate with the TCR/CD3 complex. In addition, these mutants have a diminished response to CD4-dependent stimuli. We conclude that the association between CD4 and the TCR/CD3 complex during T cell activation plays an important role in CD4-dependent responsiveness and this association requires the interaction of CD4 with p56lck. These results also suggest that a substrate for p56lck may be expressed in the TCR/CD3 complex.

摘要

通过荧光共振能量转移,我们先前已经证明,在抗CD3单克隆抗体介导的表达人CD4的鼠T细胞杂交瘤激活后,CD4会与TCR/CD3复合物紧密结合。结果表明,CD4与TCR/CD3复合物之间的这种结合依赖于完整的CD4胞质结构域的存在。我们现在在鼠T细胞杂交瘤中表达了CD4的突变形式,这些突变形式在第420、422或430位含有半胱氨酸到丝氨酸的点突变。第420和422位的突变,但不是430位的突变,消除了与p56lck的结合。通过使用荧光共振能量转移,我们证明,在野生型CD4和430突变型CD4与TCR/CD3复合物结合的条件下,不能与p56lck相互作用的CD4突变体无法与TCR/CD3复合物结合。此外,这些突变体对CD4依赖性刺激的反应减弱。我们得出结论,T细胞激活过程中CD4与TCR/CD3复合物之间的结合在CD4依赖性反应中起重要作用,并且这种结合需要CD4与p56lck相互作用。这些结果还表明,p56lck的底物可能在TCR/CD3复合物中表达。

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