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白细胞介素1的不同分子形式对内皮细胞功能的调节

Modulation of endothelial cell functions by different molecular species of interleukin 1.

作者信息

Dejana E, Breviario F, Erroi A, Bussolino F, Mussoni L, Gramse M, Pintucci G, Casali B, Dinarello C A, Van Damme J

出版信息

Blood. 1987 Feb;69(2):695-9.

PMID:3542082
Abstract

Different molecular species of interleukin 1 (IL 1) were examined for the spectrum of responses elicited in human endothelial cells (HEC), including synthesis of prostacyclin (PGI2), tissue-type procoagulant activity (PCA), platelet activating factor (PAF), and plasminogen activator inhibitor (PA-I). The IL 1 preparations utilized for the present study included a natural, partially purified IL 1, a preparation purified to homogeneity with extensive homology with the derived aminoacid IL 1 beta (pI7) sequence denominated "22K factor," murine recombinant IL 1 alpha, human recombinant IL 1 alpha (pI5) and beta (pI7). Natural, partially purified IL 1, a mixture of alpha and beta species, induced the entire spectrum of responses in HEC. Production of PA-I was elicited by all forms of IL 1 tested. PGI2 and PCA were elicited by "22K factor" and by human recombinant IL 1 beta and alpha but not by murine recombinant IL 1 alpha. PAF synthesis was stimulated by murine and human recombinant IL 1 alpha but not by human recombinant IL 1 beta and 22K factor. Thus the available different molecular forms of IL 1 elicit largely but not completely overlapping patterns of responses in HEC. The IL 1 pathway of regulation of HEC functions might provide a basis for novel strategies in therapeutically oriented research on vessel wall disorders.

摘要

检测了白细胞介素1(IL-1)的不同分子种类对人内皮细胞(HEC)引发的反应谱,包括前列环素(PGI2)的合成、组织型促凝血活性(PCA)、血小板活化因子(PAF)和纤溶酶原激活物抑制剂(PA-I)。本研究使用的IL-1制剂包括天然的、部分纯化的IL-1,一种纯化至同质且与推导的氨基酸IL-1β(pI7)序列具有广泛同源性的制剂,称为“22K因子”,小鼠重组IL-1α,人重组IL-1α(pI5)和β(pI7)。天然的、部分纯化的IL-1,α和β种类的混合物,在HEC中诱导了整个反应谱。所有测试形式的IL-1均能引发PA-I的产生。“22K因子”以及人重组IL-1β和α能引发PGI2和PCA,但小鼠重组IL-1α不能。小鼠和人重组IL-1α能刺激PAF的合成,但人重组IL-1β和22K因子不能。因此,现有的不同分子形式的IL-1在HEC中引发的反应模式在很大程度上但并非完全重叠。IL-1调节HEC功能的途径可能为血管壁疾病的治疗导向研究中的新策略提供基础。

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