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人皮肤器官培养中毛细血管后微静脉内皮细胞上活化抗原的诱导。

Induction of an activation antigen on postcapillary venular endothelium in human skin organ culture.

作者信息

Messadi D V, Pober J S, Fiers W, Gimbrone M A, Murphy G F

出版信息

J Immunol. 1987 Sep 1;139(5):1557-62.

PMID:3497975
Abstract

We studied the effects of the immune mediators interleukin 1, interleukin 2, tumor necrosis factor, immune interferon, and lipopolysaccharide on the expression of the endothelial activation antigen recognized by the murine monoclonal antibody H4/18 in short term organ cultures of newborn foreskins. No endothelial staining was detectable before culture. Interleukin 1, tumor necrosis factor, and lipopolysaccharide each induced 2+ to 3+ H4/18 staining of microvascular endothelium at 6 hr. Combining mediators produced additive (3+ to 4+) effects, and reactivity was lost or markedly diminished by 24 hr. Incubation with culture medium alone resulted in 1+ to 2+ H4/18 staining at 6 hr, and medium conditioned by cultured foreskins, but not mock-conditioned medium, could induce H4/18 binding in cultured human umbilical vein endothelial cells. The spontaneous expression of microvascular staining in the foreskins was markedly inhibited by cyclosporin A, but not polymyxin B sulfate or dexamethasone; cyclosporin A did not inhibit induction of staining by exogenous mediators. Both light level and immunoultrastructural studies demonstrated H4/18 expression to be associated predominantly with postcapillary venular endothelial cells of the superficial vascular plexus. We conclude that microvascular endothelium of skin can undergo activation in response to exogenous and endogenous cytokines, with the greatest changes occurring in those portions of the vessels most involved in leukocyte and lymphocyte trafficking.

摘要

我们在新生儿包皮的短期器官培养中,研究了免疫介质白细胞介素1、白细胞介素2、肿瘤坏死因子、免疫干扰素和脂多糖对鼠单克隆抗体H4/18识别的内皮激活抗原表达的影响。培养前未检测到内皮染色。白细胞介素1、肿瘤坏死因子和脂多糖在6小时时均诱导微血管内皮出现2+至3+H4/18染色。联合使用介质产生累加(3+至4+)效应,且反应性在24小时时丧失或显著减弱。单独用培养基孵育在6小时时导致1+至2+H4/18染色,并且由培养的包皮条件化的培养基(而非模拟条件化的培养基)可诱导培养的人脐静脉内皮细胞中的H4/18结合。包皮中微血管染色的自发表达被环孢素A显著抑制,但未被硫酸多粘菌素B或地塞米松抑制;环孢素A不抑制外源性介质诱导的染色。光镜和免疫超微结构研究均表明H4/18表达主要与浅表血管丛的毛细血管后微静脉内皮细胞相关。我们得出结论,皮肤的微血管内皮可对外源性和内源性细胞因子作出反应而发生激活,在那些最参与白细胞和淋巴细胞运输的血管部分中发生的变化最大。

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