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鉴定和表征人C5a中负责刺激IL-6合成的效应区域。

Identification and characterization of the effector region within human C5a responsible for stimulation of IL-6 synthesis.

作者信息

Morgan E L, Sanderson S, Scholz W, Noonan D J, Weigle W O, Hugli T E

机构信息

Department of Immunology, Scripps Research Institute, La Jolla, CA 92037.

出版信息

J Immunol. 1992 Jun 15;148(12):3937-42.

PMID:1602137
Abstract

Human C fragment C5a is known to be a proinflammatory mediator and more recently shown to be a potent modulator of both humoral and cell-mediated immunity. We recently reported that natural and recombinant C5a induces the synthesis of IL-6-specific mRNA and secreted protein from human monocytes. Our studies using analogue peptides that are homologous to the carboxyl-terminal sequence of human C5a, indicate that the "effector" site for inducing IL-6 synthesis resides within the C-terminal region (C5a (70-74)) of the C5a molecule. C5a peptides containing the exact sequence of the natural factor were found to retain full agonist activity but exhibited low potency (0.01-0.1% of intact C5a). It was also shown that amino acid substitutions in the C5a peptides by aromatic/hydrophobic residues, outside the immediate effector site, resulted in analogue peptides with a substantial increase in potency relative to the most active natural peptide (C5a (56-74)). Moreover, these peptides approach the potency of natural C5a for induction of IL-6. Taken together, these results suggest that the inflammatory and immunoregulatory activities associated with C5a may, in part, be due to the synthesis of IL-6.

摘要

人C片段C5a是一种促炎介质,最近还被证明是体液免疫和细胞介导免疫的有效调节剂。我们最近报道,天然和重组C5a可诱导人单核细胞合成IL-6特异性mRNA和分泌蛋白。我们使用与人C5a羧基末端序列同源的类似肽进行的研究表明,诱导IL-6合成的“效应”位点位于C5a分子的C末端区域(C5a(70 - 74))。发现含有天然因子确切序列的C5a肽保留了完全的激动剂活性,但效力较低(完整C5a的0.01 - 0.1%)。还表明,在紧邻效应位点之外的位置,用芳香族/疏水性残基替换C5a肽中的氨基酸,会产生效力相对于最具活性的天然肽(C5a(56 - 74))大幅增加的类似肽。此外,这些肽接近天然C5a诱导IL-6的效力。综上所述,这些结果表明,与C5a相关的炎症和免疫调节活性可能部分归因于IL-6的合成。

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