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肿瘤坏死因子受体免疫黏附素对肿瘤坏死因子的抑制作用。与抗肿瘤坏死因子单克隆抗体的比较。

Inhibition of TNF by a TNF receptor immunoadhesin. Comparison to an anti-TNF monoclonal antibody.

作者信息

Haak-Frendscho M, Marsters S A, Mordenti J, Brady S, Gillett N A, Chen S A, Ashkenazi A

机构信息

Department of Molecular Biology, Genentech, Inc., South San Francisco, CA 94080.

出版信息

J Immunol. 1994 Feb 1;152(3):1347-53.

PMID:8301136
Abstract

TNF is an important mediator of inflammation, which can have deleterious effects when produced inappropriately. We have described a recombinant inhibitor of TNF, termed TNFR-IgG, or TNFR immunoadhesin, composed of the extracellular portion of the type 1 (p55) TNF receptor (TNFR) linked to the hinge and Fc regions of IgG heavy chain. This bivalent, Ab-like molecule is a potent inhibitor of TNF, exhibiting significantly higher affinity for the cytokine than soluble TNFR. Here, we compare the TNF-neutralizing capacity of TNFR-IgG to that of an anti-TNF mAb. In vitro, TNFR-IgG was 10- to 50-fold more potent than anti-TNF mAb at blocking the cytotoxic effect of exogenous TNF on actinomycin D-treated murine L-M cells. In vivo, the plasma half-life of TNFR-IgG in mice was approximately 6 days, similar to that reported for the anti-TNF mAb. However, the immunoadhesin was approximately 10-fold more effective than the Ab at neutralizing the activity of endogenous TNF, as assessed in a model for murine listeriosis. These results demonstrate a markedly greater potency of the TNFR immunoadhesin compared with the anti-TNF mAb at inhibiting TNF activity in vitro and in vivo.

摘要

肿瘤坏死因子(TNF)是炎症的重要介质,若产生不当可产生有害作用。我们已描述了一种TNF重组抑制剂,称为TNFR-IgG或TNFR免疫粘附素,它由1型(p55)TNF受体(TNFR)的胞外部分与IgG重链的铰链区和Fc区相连组成。这种二价的、类似抗体的分子是一种有效的TNF抑制剂,对细胞因子的亲和力明显高于可溶性TNFR。在此,我们比较了TNFR-IgG与抗TNF单克隆抗体(mAb)的TNF中和能力。在体外,在阻断外源性TNF对放线菌素D处理的小鼠L-M细胞的细胞毒性作用方面,TNFR-IgG的效力比抗TNF mAb高10至50倍。在体内,TNFR-IgG在小鼠体内的血浆半衰期约为6天,与抗TNF mAb报道的半衰期相似。然而,在小鼠李斯特菌病模型中评估发现,该免疫粘附素在中和内源性TNF活性方面比抗体约有效10倍。这些结果表明,与抗TNF mAb相比,TNFR免疫粘附素在体外和体内抑制TNF活性方面具有明显更强的效力。

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