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白细胞介素-2和T细胞受体抗体调节辐射白血病病毒转化的T细胞淋巴瘤的增殖。

Interleukin-2 and antibody to the T cell receptor regulate proliferation of a radiation leukemia virus-transformed T cell lymphoma.

作者信息

O'Neill H C

机构信息

Department of Experimental Pathology, John Curtin School of Medical Research, Canberra, Australia.

出版信息

Leukemia. 1988 Feb;2(2):108-14.

PMID:2830440
Abstract

In this report, a Radiation leukemia virus-transformed murine T cell lymphoma is described which is dependent on the interleukin-2 (IL-2) growth factor for proliferation under single cell conditions of growth. It was isolated from a C57BL mouse which had been primed with the Radiation leukemia virus-induced thymoma, C6VL/1, and has been shown to be phenotypically and karyotypically distinct from C6VL/1. IL-2 dependency has been stable over many in vitro passages, and this property also serves to distinguish this cell line from C6VL/1. 5C2 constitutively expresses a T cell receptor (TCR) and can respond by increased proliferation to external stimulation with anti-TCR antibody. This antibody acts to stimulate 5C2 growth in the absence of added IL-2. Maximum stimulation was achieved in the presence of a 50-ng/ml concentration of purified antibody. 5C2 has also been shown to produce detectable levels of IL-2 which can be increased by 8- to 16-fold after exposure of cells to anti-TCR antibody. The C6VL/1 T cell lymphoma has served as a control cell line in three experiments since it cannot be stimulated either to increased proliferation or to lymphokine release by this same antibody. However, a 10-ng/ml concentration of anti-TCR antibody was found to inhibit proliferation of both T cell lymphomas when they were cultured under optimal conditions, i.e., in the presence of an IL-2 source for 5C2. The proliferation of both T cell lymphomas appears to be regulated, although in different ways, by the binding of antibody in the vicinity of the TCR complex. While 5C2 is dependent on IL-2 production (and TCR triggering) to proliferate, C6VL/1 replicates independently of any growth factors. Signal transduction through the TCR/T3 complex, together with the subsequent production of growth factors, may be important for driving the proliferation of T cells such as 5C2 at an early stage in oncogenic progression following infection with an RNA tumor virus.

摘要

在本报告中,描述了一种辐射白血病病毒转化的小鼠T细胞淋巴瘤,在单细胞生长条件下,其增殖依赖于白细胞介素-2(IL-2)生长因子。它是从一只用辐射白血病病毒诱导的胸腺瘤C6VL/1进行预处理的C57BL小鼠中分离出来的,并且已显示在表型和核型上与C6VL/1不同。IL-2依赖性在许多体外传代中一直稳定,并且这种特性也用于将该细胞系与C6VL/1区分开来。5C2组成性表达T细胞受体(TCR),并且可以通过用抗TCR抗体进行外部刺激而以增加的增殖做出反应。该抗体在不添加IL-2的情况下刺激5C2生长。在存在50 ng/ml浓度的纯化抗体的情况下实现了最大刺激。5C2也已显示产生可检测水平的IL-2,在细胞暴露于抗TCR抗体后,其水平可增加8至16倍。C6VL/1 T细胞淋巴瘤在三个实验中用作对照细胞系,因为相同的抗体既不能刺激其增加增殖也不能刺激其释放淋巴因子。然而,当在最佳条件下培养时,即5C2存在IL-2来源时,发现10 ng/ml浓度的抗TCR抗体抑制两种T细胞淋巴瘤的增殖。两种T细胞淋巴瘤的增殖似乎都受到TCR复合物附近抗体结合的调节,尽管方式不同。虽然5C2依赖于IL-2产生(和TCR触发)来增殖,但C6VL/1独立于任何生长因子进行复制。通过TCR/T3复合物的信号转导以及随后生长因子的产生,可能对于在感染RNA肿瘤病毒后的致癌进展早期驱动诸如5C2的T细胞增殖很重要。

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