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CD8αα和CD8αβ在与MHC I类分子相互作用中作用的比较。

Comparison of the roles of CD8 alpha alpha and CD8 alpha beta in interaction with MHC class I.

作者信息

Sun J, Kavathas P B

机构信息

Department of Laboratory Medicine, Yale University School of Medicine, New Haven, CT 06520, USA.

出版信息

J Immunol. 1997 Dec 15;159(12):6077-82.

PMID:9550407
Abstract

The CD8 molecule is expressed either as an alpha/alpha homodimer or an alpha/beta heterodimer on thymocytes and cytotoxic T cells, and functions as a coreceptor in concert with TCR for binding the MHC class I/peptide complex. Although CD8alpha/beta heterodimers have been shown to be more effective coreceptors, the precise role of the beta-chain in TCR-mediated thymic maturation and T cell activation is not understood. To understand the role of CD8beta in mediating CD8/MHC class I interaction, we examined whether cell surface CD8alpha/beta heterodimer promotes better cell-cell adhesion with MHC class I than the CD8alpha/alpha homodimer. The abilities of different forms of CD8 to adhere to MHC class I were measured with a cell-cell binding assay. Using a wild-type CD8beta and -alpha, we found that CD8alphabeta heterodimers did not mediate greater cell-cell adhesion than CD8alphaalpha homodimers. Furthermore, we found that chimeric CD8beta-alpha homodimers afforded no detectable binding. These results do not support the idea that CD8alphabeta binding to MHC class I is greater than that of CD8alphaalpha. Rather, they point to an alternative explanation in which CD8beta may play an role in promoting CD8/TCR interaction and/or in signaling/regulatory pathways.

摘要

CD8分子在胸腺细胞和细胞毒性T细胞上以α/α同二聚体或α/β异二聚体的形式表达,并作为共受体与TCR协同作用,以结合MHC I类/肽复合物。尽管已证明CD8α/β异二聚体是更有效的共受体,但β链在TCR介导的胸腺成熟和T细胞活化中的精确作用尚不清楚。为了了解CD8β在介导CD8/MHC I类相互作用中的作用,我们研究了细胞表面的CD8α/β异二聚体是否比CD8α/α同二聚体更能促进与MHC I类的细胞间黏附。通过细胞间结合试验测量了不同形式的CD8与MHC I类黏附的能力。使用野生型CD8β和α,我们发现CD8αβ异二聚体并不比CD8αα同二聚体介导更强的细胞间黏附。此外,我们发现嵌合的CD8β-α同二聚体没有可检测到的结合。这些结果不支持CD8αβ与MHC I类的结合大于CD8αα的观点。相反,它们指向另一种解释,即CD8β可能在促进CD8/TCR相互作用和/或信号传导/调节途径中发挥作用。

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