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Molecular cloning and chromosomal localization of the human T-cell receptor zeta chain: distinction from the molecular CD3 complex.人类T细胞受体ζ链的分子克隆与染色体定位:与分子CD3复合体的区别
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Interdependence of CD3-Ti and CD2 activation pathways in human T lymphocytes.人T淋巴细胞中CD3-Ti和CD2激活途径的相互依赖性。
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Activation of cytolytic T lymphocyte and natural killer cell function through the T11 sheep erythrocyte binding protein.通过T11绵羊红细胞结合蛋白激活细胞毒性T淋巴细胞和自然杀伤细胞功能。
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Triggering of T-lymphocytes via either T3-Ti or T11 surface structures opens a voltage-insensitive plasma membrane calcium-permeable channel: requirement for interleukin-2 gene function.通过T3-Ti或T11表面结构触发T淋巴细胞会打开一个电压不敏感的质膜钙通透通道:白细胞介素-2基因功能的必要条件。
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CD3 ζ 细胞质结构域介导 CD2 诱导的 T 细胞活化。

The CD3 zeta cytoplasmic domain mediates CD2-induced T cell activation.

作者信息

Howard F D, Moingeon P, Moebius U, McConkey D J, Yandava B, Gennert T E, Reinherz E L

机构信息

Laboratory of Immunobiology, Dana-Farber Cancer Institute, Boston, Massachusetts.

出版信息

J Exp Med. 1992 Jul 1;176(1):139-45. doi: 10.1084/jem.176.1.139.

DOI:10.1084/jem.176.1.139
PMID:1351920
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2119282/
Abstract

CD2-mediated T lymphocyte activation requires surface expression of CD3-Ti, the T cell receptor (TCR) for antigen major histocompatibility complex protein. Given the importance of CD3 zeta in TCR signaling, we have directly examined the ability of the CD3 zeta cytoplasmic domain to couple CD2 to intracellular signal transduction pathways. A cDNA encoding a chimeric protein consisting of the human CD3 zeta cytoplasmic domain (amino acid residues 31-142) fused to the CD8 alpha extracellular and transmembrane domains (amino acid residues 1-187) was transfected into a CD2+CD3-CD8- variant of the human T cell line Jurkat. The resulting transfectants expressed the CD8 alpha/CD3 zeta chimeric receptor at the cell surface in the absence of other TCR subunits. Stimulation of these transfectants with anti-T11(2) + anti-T11(3) monoclonal antibodies (mAbs) initiated both a prompt cytosolic free calcium ([Ca2+]i) rise and protein tyrosine kinase activation. Stimulation with either intact anti-T11(2) + anti-T11(3) mAbs or purified F(ab')2 fragments resulted in interleukin 2 (IL-2) secretion. In contrast, control cell lines transfected with a cDNA encoding wild-type CD8 alpha, and thus lacking surface expression of the CD3 zeta cytoplasmic domain, failed to show any [Ca2+]i rise, protein tyrosine kinase activation, or IL-2 secretion after identical stimulation. These data directly establish the CD3 zeta cytoplasmic domain as a necessary and sufficient component of the CD3-Ti complex involved in T lymphocyte activation through CD2. Moreover, they show that CD2 signaling can function in the absence of Fc receptors.

摘要

CD2介导的T淋巴细胞激活需要CD3-Ti的表面表达,CD3-Ti是抗原主要组织相容性复合体蛋白的T细胞受体(TCR)。鉴于CD3ζ在TCR信号传导中的重要性,我们直接研究了CD3ζ胞质结构域将CD2与细胞内信号转导途径偶联的能力。将编码由人CD3ζ胞质结构域(氨基酸残基31-142)与CD8α细胞外和跨膜结构域(氨基酸残基1-187)融合而成的嵌合蛋白的cDNA转染到人T细胞系Jurkat的CD2 + CD3 - CD8 - 变体中。所得转染子在没有其他TCR亚基的情况下在细胞表面表达CD8α/CD3ζ嵌合受体。用抗T11(2)+抗T11(3)单克隆抗体(mAb)刺激这些转染子会引发胞质游离钙([Ca2+]i)迅速升高和蛋白酪氨酸激酶激活。用完整的抗T11(2)+抗T11(3) mAb或纯化的F(ab')2片段刺激会导致白细胞介素2(IL-2)分泌。相比之下,用编码野生型CD8α的cDNA转染的对照细胞系,因此缺乏CD3ζ胞质结构域的表面表达,在相同刺激后未显示任何[Ca2+]i升高、蛋白酪氨酸激酶激活或IL-2分泌。这些数据直接确立了CD3ζ胞质结构域是通过CD2参与T淋巴细胞激活的CD3-Ti复合物的必要和充分组成部分。此外,它们表明CD2信号传导可以在没有Fc受体的情况下发挥作用。