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TCR的CD3ε亚基包含内吞信号。

The CD3 epsilon subunit of the TCR contains endocytosis signals.

作者信息

Borroto A, Lama J, Niedergang F, Dautry-Varsat A, Alarcón B, Alcover A

机构信息

Centro de Biología Molecular Severo Ochoa, Consejo Superior de Investigaciones Cientificas-Universidad Autónoma, Madrid, Spain.

出版信息

J Immunol. 1999 Jul 1;163(1):25-31.

Abstract

Ligand binding to TCR induces its internalization and cell surface down-modulation. These phenomena contribute to the extinction of activation signals. Due to the multicomponent nature of the TCR-CD3 complex, its internalization may be mediated by one or several of its subunits. Although it has been reported that CD3 gamma and CD3 delta contain endocytosis motifs involved in the internalization of the TCR-CD3 complex, other subunits could also be involved in this process. For instance, CD3 epsilon and CD zeta display amino acid sequences reminiscent of internalization motifs. To investigate whether CD3 epsilon bears endocytosis signals, we have analyzed the internalization capacity of a panel of deletion and point mutants of CD3 epsilon that were expressed on the cell surface independently of other TCR-CD3 subunits. Here we report that CD3 epsilon displays endocytosis determinants. These data indicate that CD3 epsilon could contribute to the internalization and cell surface down-regulation of TCR-CD3 complexes. Moreover, the existence of endocytosis signals in this polypeptide could serve to retrieve unassembled CD3 epsilon subunits or partial CD3 complexes from the plasma membrane, thus restricting the expression on the cell surface to fully functional TCR-CD3 complexes.

摘要

配体与TCR结合会诱导其内化以及细胞表面下调。这些现象有助于激活信号的消退。由于TCR-CD3复合物的多组分性质,其内化可能由其一个或几个亚基介导。尽管已有报道称CD3γ和CD3δ含有参与TCR-CD3复合物内化的内吞基序,但其他亚基也可能参与这一过程。例如,CD3ε和CDζ显示出类似于内吞基序的氨基酸序列。为了研究CD3ε是否带有内吞信号,我们分析了一组CD3ε缺失和点突变体的内化能力,这些突变体在细胞表面独立于其他TCR-CD3亚基表达。在此我们报告CD3ε显示出内吞决定簇。这些数据表明CD3ε可能有助于TCR-CD3复合物的内化和细胞表面下调。此外,该多肽中内吞信号的存在可能有助于从质膜中回收未组装的CD3ε亚基或部分CD3复合物,从而将细胞表面的表达限制为完全功能性的TCR-CD3复合物。

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