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两种肿瘤坏死因子(TNF)受体在调节TNF和淋巴毒素α效应中的不同作用。

Distinct roles of the two tumor necrosis factor (TNF) receptors in modulating TNF and lymphotoxin alpha effects.

作者信息

Medvedev A E, Espevik T, Ranges G, Sundan A

机构信息

Institute of Cancer Research and Molecular Biology, Trondheim, Norway.

出版信息

J Biol Chem. 1996 Apr 19;271(16):9778-84. doi: 10.1074/jbc.271.16.9778.

Abstract

The role for the two tumor necrosis factor (TNF) receptors in discriminating TNF and lymphotoxin alpha (LTalpha) effects has been studied. TNF and LTalpha were equally mitogenic in Fs4 fibroblasts, which express a high amount of the p55 compared to the p75 TNF receptors (TNFRs). In contrast, TNF was more potent than LTalpha in mediating gene regulation and cytotoxicity in SW480-betaGal cells and KYM-1 cells, which have a high p75/p55 TNFR ratio. Both TNF and LTalpha showed comparable affinities for the two TNFRs. However, in contrast to LTalpha, TNF dissociated rapidly from the p75 TNFR, whereas both cytokines dissociated slowly from the p55 TNFR. Soluble p55 TNFR was much more potent than soluble p75 TNFR in inhibiting TNF cytotoxicity, whereas both soluble receptors moderately decreased LTalpha-mediated cytotoxicity with comparable efficacy. Antagonistic monoclonal antibodies against either TNFR types markedly inhibited TNF effects. However, only the p55 TNFR antagonistic antibody significantly decreased LTalpha-mediated cytotoxicity and cytomegalovirus promoter activation, whereas blocking of the p75 TNFR enhanced the LTalpha effects. These data suggest that whereas the p75 TNFR can both directly propagate TNF signals and "pass" TNF to the p55 TNFR, it attenuates LTalpha and may serve as a decoy receptor for this cytokine.

摘要

对两种肿瘤坏死因子(TNF)受体在区分TNF和淋巴毒素α(LTα)作用方面的作用进行了研究。在Fs4成纤维细胞中,TNF和LTα具有同等的促有丝分裂作用,与p75 TNF受体(TNFRs)相比,该细胞表达大量的p55。相反,在具有高p75/p55 TNFR比率的SW480-βGal细胞和KYM-1细胞中,TNF在介导基因调控和细胞毒性方面比LTα更有效。TNF和LTα对两种TNFRs表现出相当的亲和力。然而,与LTα不同,TNF从p75 TNFR上迅速解离,而两种细胞因子从p55 TNFR上解离缓慢。可溶性p55 TNFR在抑制TNF细胞毒性方面比可溶性p75 TNFR有效得多,而两种可溶性受体以相当的效力适度降低LTα介导的细胞毒性。针对任何一种TNFR类型的拮抗单克隆抗体均显著抑制TNF的作用。然而,只有p55 TNFR拮抗抗体显著降低LTα介导的细胞毒性和巨细胞病毒启动子激活,而阻断p75 TNFR则增强LTα的作用。这些数据表明,虽然p75 TNFR既可以直接传递TNF信号,又可以将TNF“传递”给p55 TNFR,但它会减弱LTα的作用,并且可能作为这种细胞因子的诱饵受体。

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