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不同的抗原呈递细胞在诱导脱辅基细胞色素c特异性T细胞克隆产生淋巴因子及增殖的能力方面存在差异。

Different antigen-presenting cells differ in their capacity to induce lymphokine production and proliferation of an apo-cytochrome c-specific T cell clone.

作者信息

Baumhüter S, Bron C, Corradin G

出版信息

J Immunol. 1985 Aug;135(2):989-94.

PMID:2409165
Abstract

The activation of an apo-cytochrome c-specific T cell clone was found to differ, depending on the antigen-presenting cell population. Whereas total syngeneic spleen cells and bone marrow macrophages could be shown to trigger proliferation, IL 2, and MAF production by the T cell clone, a B cell lymphoma only induced MAF secretion. Further studies demonstrated that this effect was not due to a different antigen processing by the B lymphoma or to limiting amounts of Ia and antigen molecules on the B lymphoma cell surface. The dissociation of induction of MAF production from IL-2 production/proliferation found with the different antigen-presenting cells indicates strongly that molecules other than Ia and antigen may be required for the complete functional activation of antigen-specific T cell clones.

摘要

已发现脱辅基细胞色素c特异性T细胞克隆的激活因抗原呈递细胞群体的不同而有所差异。虽然同基因脾细胞和骨髓巨噬细胞可引发T细胞克隆的增殖、白细胞介素2(IL 2)和巨噬细胞活化因子(MAF)的产生,但B细胞淋巴瘤仅诱导MAF分泌。进一步研究表明,这种效应并非由于B淋巴瘤对抗原的不同处理方式,也不是由于B淋巴瘤细胞表面Ia和抗原分子数量有限。不同抗原呈递细胞导致MAF产生的诱导与IL-2产生/增殖的解离强烈表明,除Ia和抗原外,可能还需要其他分子才能使抗原特异性T细胞克隆完全功能性激活。

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