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含甲酰甲硫氨酸肽释放组胺的机制。

Mechanism of histamine release by formyl methionine-containing peptides.

作者信息

Siraganian R P, Hook W A

出版信息

J Immunol. 1977 Dec;119(6):2078-83.

PMID:72118
Abstract

Small, acylated, methionine-containing peptides release histamine from human basophils. The characteristics of this reaction were compared to that of C5a- and IgE-induced release. fMet peptide-induced release requires Ca++ and is inhibited by EDTA in a manner similar to IgE- and C5a-mediated reactions. The fMet-Phe-Met-initiated reaction is complete within 2 min at temperatures of 25, 30, and 37 degrees C; but does not occur at 0 degrees C. There was a large variation in the capacity of leukocytes from different donors to release histamine with fMet peptides. However, there was no correlation in the capacity of leukocytes to release histamine with fMet-Phe-Met and their release with C5a or anti-IgE. The release by fMet-Phe-Met (but not by C5a or anti-IgE) was reversibly inhibited by a nonreleasing tripeptide. Leukocytes could be desensitized to the action of active fMet-peptide by preincubation with the peptide in the absence of cations. After washing, these cells released normally with C5a or anti-IgE. Conversely, cells desensitized to the action of C5a- or IgE-mediated reactions released normally with fMet peptides. There was cross-desensitization between different active peptides, and inactive peptides could not desensitize the leukocytes. Pharmacologic agents had similar effects on C5a and fMet peptide-induced release (e.g., lack of enhancement with deuterium oxide; enhancement with cytochalasin B; and inhibition with aminophylline and dibutyryl cyclic AMP). Therefore, histamine release with fMet peptides is initiated by their binding to and activation of a specific receptor on the basophil; the reaction beyond that point is similar to the C5a-mediated reaction.

摘要

含甲硫氨酸的小分子酰化肽可使人嗜碱性粒细胞释放组胺。将该反应的特性与C5a和IgE诱导的释放反应进行了比较。甲硫氨酰肽诱导的释放需要Ca++,并且以类似于IgE和C5a介导反应的方式被EDTA抑制。在25、30和37摄氏度下,fMet-Phe-Met引发的反应在2分钟内完成;但在0摄氏度时不发生。不同供体的白细胞用fMet肽释放组胺的能力存在很大差异。然而,白细胞用fMet-Phe-Met释放组胺的能力与其用C5a或抗IgE释放组胺的能力之间没有相关性。fMet-Phe-Met(而非C5a或抗IgE)引起的释放可被一种无释放活性的三肽可逆抑制。通过在无阳离子的情况下用该肽预孵育,白细胞可对活性fMet肽的作用产生脱敏。洗涤后,这些细胞用C5a或抗IgE正常释放组胺。相反,对C5a或IgE介导反应作用产生脱敏的细胞用fMet肽正常释放组胺。不同活性肽之间存在交叉脱敏,无活性肽不能使白细胞脱敏。药理剂对C5a和fMet肽诱导的释放有类似作用(例如,氧化氘无增强作用;细胞松弛素B有增强作用;氨茶碱和二丁酰环磷腺苷有抑制作用)。因此,fMet肽引起的组胺释放是由它们与嗜碱性粒细胞上特定受体的结合和激活引发的;该点之后的反应类似于C5a介导的反应。

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