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通过cDNA转染在小鼠T细胞中表达功能性人白细胞介素-2受体

Expression of functional human interleukin-2 receptor in mouse T cells by cDNA transfection.

作者信息

Kondo S, Shimizu A, Maeda M, Tagaya Y, Yodoi J, Honjo T

出版信息

Nature. 1986;320(6057):75-7. doi: 10.1038/320075a0.

Abstract

Interleukin-2 (IL-2) in combination with the IL-2 receptor has an essential role in antigen-stimulated proliferation of T lymphocytes. It has been proposed that the constitutive expression of the IL-2 receptor on adult T-cell leukaemia (ATL) cells may be associated with transformation of T cells. Although we and others have isolated complementary DNA clones encoding a protein that binds IL-2, formal proof that this protein is the IL-2 receptor requires demonstration of IL-2-dependent growth stimulation of cells expressing the protein. In addition, a functional assay system other than binding of IL-2 is required to investigate the molecular mechanism of signal transmission through the IL-2 receptor using artificially mutated cDNA. The IL-2 receptor expressed in non-lymphoid cells by cDNA transfection did not mediate a growth signal, implying that lymphoid cells expressing the functional receptor might have specific accessory molecule(s) for signal transmission by the receptor. Therefore, we established a line of IL-2-dependent mouse cells (CT/hR) expressing both murine (endogenous) and human IL-2 receptors. Here, by blocking the endogenous mouse IL-2 receptors with monoclonal antibodies, we show that the human IL-2 receptor of CT/hR cells is functionally active. Although CT/hR expressed the human IL-2 receptor constitutively, growth of these cells was strictly dependent on IL-2, indicating that uncontrolled over-expression of the IL-2 receptor was not by itself sufficient for T-cell transformation.

摘要

白细胞介素-2(IL-2)与IL-2受体结合在抗原刺激的T淋巴细胞增殖中起重要作用。有人提出,成人T细胞白血病(ATL)细胞上IL-2受体的组成性表达可能与T细胞转化有关。尽管我们和其他人已经分离出编码与IL-2结合的蛋白质的互补DNA克隆,但要正式证明该蛋白质是IL-2受体,需要证明表达该蛋白质的细胞有IL-2依赖性生长刺激。此外,除了IL-2结合外,还需要一个功能测定系统来研究使用人工突变cDNA通过IL-2受体进行信号转导的分子机制。通过cDNA转染在非淋巴细胞中表达的IL-2受体不介导生长信号,这意味着表达功能性受体的淋巴细胞可能具有用于受体信号转导的特定辅助分子。因此,我们建立了一系列表达小鼠(内源性)和人IL-2受体的IL-2依赖性小鼠细胞系(CT/hR)。在此,我们用单克隆抗体阻断内源性小鼠IL-2受体,结果表明CT/hR细胞的人IL-2受体具有功能活性。尽管CT/hR组成性表达人IL-2受体,但这些细胞的生长严格依赖于IL-2,这表明IL-2受体的不受控制的过度表达本身不足以导致T细胞转化。

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