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人T淋巴细胞转化生长因子β的产生及其在T细胞生长调节中的潜在作用。

Production of transforming growth factor beta by human T lymphocytes and its potential role in the regulation of T cell growth.

作者信息

Kehrl J H, Wakefield L M, Roberts A B, Jakowlew S, Alvarez-Mon M, Derynck R, Sporn M B, Fauci A S

出版信息

J Exp Med. 1986 May 1;163(5):1037-50. doi: 10.1084/jem.163.5.1037.

Abstract

This study examines the potential role of transforming growth factor beta (TGF-beta) in the regulation of human T lymphocyte proliferation, and proposes that TGF-beta is an important autoregulatory lymphokine that limits T lymphocyte clonal expansion, and that TGF-beta production by T lymphocytes is important in T cell interactions with other cell types. TGF-beta was shown to inhibit IL-2-dependent T cell proliferation. The addition of picograms amounts of TGF-beta to cultures of IL-2-stimulated human T lymphocytes suppressed DNA synthesis by 60-80%. A potential mechanism of this inhibition was found. TGF-beta inhibited IL-2-induced upregulation of the IL-2 and transferrin receptors. Specific high-affinity receptors for TGF-beta were found both on resting and activated T cells. Cellular activation was shown to result in a five- to sixfold increase in the number of TGF-beta receptors on a per cell basis, without a change in the affinity of the receptor. Finally, the observations that activated T cells produce TGF-beta mRNA and that TGF-beta biologic activity is present in supernatants conditioned by activated T cells is strong evidence that T cells themselves are a source of TGF-beta. Resting T cells were found to have low to undetectable levels of TGF-beta mRNA, while PHA activation resulted in a rapid increase in TGF-beta mRNA levels (within 2 h). Both T4 and T8 lymphocytes were found to make mRNA for TGF-beta upon activation. Using both a soft agar assay and a competitive binding assay, TGF-beta biologic activity was found in supernatants conditioned by T cells; T cell activation resulted in a 10-50-fold increase in TGF-beta production. Thus, TGF-beta may be an important antigen-nonspecific regulator of human T cell proliferation, and important in T cell interaction with other cell types whose cellular functions are modulated by TGF-beta.

摘要

本研究探讨了转化生长因子β(TGF-β)在调节人T淋巴细胞增殖中的潜在作用,并提出TGF-β是一种重要的自身调节性淋巴因子,可限制T淋巴细胞的克隆扩增,且T淋巴细胞产生TGF-β在T细胞与其他细胞类型的相互作用中具有重要意义。研究表明,TGF-β可抑制白细胞介素-2(IL-2)依赖的T细胞增殖。向经IL-2刺激的人T淋巴细胞培养物中添加皮克量的TGF-β可使DNA合成抑制60%-80%。发现了这种抑制作用的一种潜在机制。TGF-β抑制IL-2诱导的IL-2受体和转铁蛋白受体的上调。在静止和活化的T细胞上均发现了TGF-β的特异性高亲和力受体。细胞活化显示可使每个细胞上的TGF-β受体数量增加五至六倍,而受体亲和力不变。最后,活化的T细胞产生TGF-β mRNA以及活化的T细胞条件培养基中存在TGF-β生物活性这些观察结果有力地证明T细胞本身就是TGF-β的来源。发现静止的T细胞TGF-β mRNA水平低至无法检测,而经植物血凝素(PHA)活化后TGF-β mRNA水平迅速升高(2小时内)。发现T4和T8淋巴细胞活化后均产生TGF-β mRNA。使用软琼脂试验和竞争性结合试验,在T细胞条件培养基中发现了TGF-β生物活性;T细胞活化导致TGF-β产生增加10-50倍。因此,TGF-β可能是人类T细胞增殖的重要抗原非特异性调节因子,并且在T细胞与其他细胞类型的相互作用中具有重要意义,这些细胞类型的细胞功能受TGF-β调节。

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本文引用的文献

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