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非肥胖型糖尿病(NOD)小鼠胰腺中的黏附分子与微血管变化。一氧化氮抑制剂(L-精氨酸甲酯)无法阻断黏附炎症诱导的激活。

Adhesion molecules and microvascular changes in the nonobese diabetic (NOD) mouse pancreas. An NO-inhibitor (L-NAME) is unable to block adhesion inflammation-induced activation.

作者信息

Papaccio G, Latronico M V, Pisanti F A, Federlin K, Linn T

机构信息

Institute of Anatomy, School of Medicine, Second University of Naples, Italy.

出版信息

Autoimmunity. 1998;27(2):65-77. doi: 10.3109/08916939809008037.

Abstract

The aim of the present study was to investigate the immunoreactivity of pancreatic microvasculature with emphasis on the adhesion molecule expression in NOD mice at a very early stage and after the start of infiltration, before the onset of the diabetic disease. Immunoreactivity for Ia-b, BM8 (mouse macrophages) and inter-cellular-adhesion-molecule-1 (ICAM-1) molecules in untreated control mice and in animals treated using an inhibitor of nitric oxide (NO) formation (L-arginine analogue), as well as islet culture, nitrite assay and ultrastructural studies were performed. Results showed that Ia-b and ICAM-1 immunoreactivities on endothelia are a very early phenomenon and that pancreatic blood vessels and, in particular, some peri-islet venules, as well as several venules of the exocrine parenchyma, undergo significant morphological changes. Several endothelial cells of both peri-islet and extra-islet compartments, often showed Ia-b and ICAM-1 immunoreactivities, demonstrating that these cells are important for the adhesion processes taking place during early autoimmune inflammation. Inhibition of NO formation does not significantly affect ICAM-1 and Ia-b immunoreactivity both in vivo and in vitro, BM8 immunoreactive cells were considerably less in number although these were detected either around islets or along pancreatic septa, but rarely within the epithelial layer.

摘要

本研究的目的是调查胰腺微血管的免疫反应性,重点是在糖尿病发病前的极早期和浸润开始后,非肥胖糖尿病(NOD)小鼠中黏附分子的表达情况。对未处理的对照小鼠和使用一氧化氮(NO)生成抑制剂(L-精氨酸类似物)处理的动物,以及胰岛培养、亚硝酸盐测定和超微结构研究进行了Ia-b、BM8(小鼠巨噬细胞)和细胞间黏附分子-1(ICAM-1)分子的免疫反应性检测。结果显示,内皮细胞上的Ia-b和ICAM-1免疫反应性是一种非常早期的现象,胰腺血管,特别是一些胰岛周围小静脉以及外分泌实质的一些小静脉会发生显著的形态变化。胰岛周围和胰岛外区域的几个内皮细胞经常显示出Ia-b和ICAM-1免疫反应性,表明这些细胞对早期自身免疫炎症期间发生的黏附过程很重要。抑制NO生成在体内和体外均未显著影响ICAM-1和Ia-b免疫反应性,BM8免疫反应性细胞数量明显较少,尽管在胰岛周围或胰腺间隔处可检测到这些细胞,但在上皮层内很少见。

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