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白细胞介素2诱导抗原反应性T细胞系分泌BCGF-I。

Interleukin 2 induces antigen-reactive T cell lines to secrete BCGF-I.

作者信息

Howard M, Matis L, Malek T R, Shevach E, Kell W, Cohen D, Nakanishi K, Paul W E

出版信息

J Exp Med. 1983 Dec 1;158(6):2024-39. doi: 10.1084/jem.158.6.2024.

Abstract

Antigen-activated T lymphocytes produce within 24 h of stimulation a factor that is indistinguishable biochemically and functionally from the B cell co-stimulating growth factor, BCGF-I, originally identified in induced EL4 supernatants: Supernatants from antigen-stimulated T cell lines are not directly mitogenic for resting B cells, but synergize in an H-2-unrestricted manner with anti-Ig activated B cells to produce polyclonal proliferation but not antibody-forming-cell development; biochemical studies reveal the B cell co-stimulating factor present in antigen-stimulated T cell line supernatants is identical by phenyl Sepharose chromatography and isoelectric focusing (IEF) to EL4 supernatant BCGF-I. We thus conclude that normal T cells produce BCGF-I in response to antigenic stimulation. Analysis of the mechanism of BCGF-I production by antigen-stimulated T cells showed that optimum amounts of BCGF-I were obtained as quickly as 24 h post-stimulation, and that the factor producing cells in the T cell line investigated bore the Lyt-1+2- phenotype. As few as 10(4) T cells produced sufficient BCGF-I to support the proliferation of 5 X 10(4) purified anti-Ig activated B cells. Finally, the activation of normal T cell lines to produce BCGF-I required either antigen presented in the context of syngeneic antigen-presenting cells (APC) or interleukin 2 (IL-2).

摘要

抗原激活的T淋巴细胞在刺激后24小时内产生一种因子,该因子在生化和功能上与最初在诱导的EL4上清液中鉴定的B细胞共刺激生长因子BCGF-I无法区分:来自抗原刺激的T细胞系的上清液对静止B细胞没有直接的促有丝分裂作用,但能以H-2非限制性方式与抗Ig激活的B细胞协同作用,产生多克隆增殖,但不产生抗体形成细胞的发育;生化研究表明,抗原刺激的T细胞系上清液中存在的B细胞共刺激因子通过苯基琼脂糖层析和等电聚焦(IEF)与EL4上清液BCGF-I相同。因此,我们得出结论,正常T细胞在抗原刺激下产生BCGF-I。对抗原刺激的T细胞产生BCGF-I的机制分析表明,在刺激后24小时内就能迅速获得最佳量的BCGF-I,并且所研究的T细胞系中产生该因子的细胞具有Lyt-1+2-表型。低至10⁴个T细胞产生的BCGF-I足以支持5×10⁴个纯化的抗Ig激活的B细胞的增殖。最后,正常T细胞系激活产生BCGF-I需要同基因抗原呈递细胞(APC)呈递的抗原或白细胞介素2(IL-2)。

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