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Molecular cloning and expression of T11 cDNAs reveal a receptor-like structure on human T lymphocytes.

机译:T11 cDNA的分子克隆和表达揭示了人类T淋巴细胞上的受体样结构。

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摘要

The T11 (CD2) sheep-erythrocyte-binding protein is a T-cell surface molecule involved in activation of T lymphocytes and thymocytes, including those lacking the T3-Ti antigen-receptor complex. The primary structure of T11 was deduced from protein microsequencing and cDNA cloning. The mature human protein appears to be divided into three domains: a hydrophilic 185 amino acid external domain bearing only limited homology to the T-cell surface protein T4 and the immunoglobulin kappa light chain variable region, a 25 amino acid hydrophobic transmembrane segment, and a 126 amino acid cytoplasmic domain rich in prolines and basic residues. Transfection of cDNAs encoding either the 1.7- or the 1.3-kilobase T11 mRNA into COS-1 cells resulted in expression of surface T11 epitopes as well as sheep-erythrocyte-binding capacity. The predicted structure is consistent with the possibility that T11 functions in signal transduction.
机译:T11(CD2)绵羊红细胞结合蛋白是一种T细胞表面分子,参与激活T淋巴细胞和胸腺细胞,包括那些缺乏T3-Ti抗原受体复合物的细胞。 T11的一级结构是从蛋白质微测序和cDNA克隆推导出来的。成熟的人蛋白质似乎分为三个结构域:一个亲水性185个氨基酸的外部结构域,仅与T细胞表面蛋白T4和免疫球蛋白κ轻链可变区具有有限的同源性,一个25个氨基酸的疏水性跨膜片段,以及一个富含脯氨酸和碱性残基的126个氨基酸的细胞质结构域。将编码1.7或1.3碱基碱基的T11 mRNA的cDNA转染到COS-1细胞中会导致表面T11表位的表达以及绵羊与红细胞的结合能力。预测的结构与T11在信号转导中发挥作用的可能性一致。

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