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肿瘤坏死因子-α和白细胞介素-1β在单核细胞趋化蛋白-1介导的大鼠肺肉芽肿形成中的调节作用

Regulatory roles of tumor necrosis factor-alpha and interleukin-1 beta in monocyte chemoattractant protein-1-mediated pulmonary granuloma formation in the rat.

作者信息

Flory C M, Jones M L, Miller B F, Warren J S

机构信息

Pharmaceutical Research Division, Warner Lambert-Parke Davis, Ann Arbor, Michigan.

出版信息

Am J Pathol. 1995 Feb;146(2):450-62.

Abstract

Intravenous infusion of particulate yeast cell wall glucan into rats results in the synchronous development of angiocentric pulmonary granulomas that are composed almost entirely of monocytes and macrophages. Previous studies indicate that locally produced monocyte chemoattractant protein-1 (MCP-1) is required for full granuloma development. Because tumor necrosis factor-alpha (TNF-alpha) and interleukin 1 (IL-1) can induce MCP-1 production in a variety of cell types, we sought to determine their potential regulatory roles in this model. A single infusion of anti-TNF-alpha antibody at the time of glucan infusion (time 0) markedly reduced MCP-1 mRNA levels at 1 and 6 hours but not at later time points; there was no effect on granuloma size or number measured at 48 hours. When multiple infusions of anti-TNF-alpha antibody were administered over a 23-hour period (0 to 23 hours), MCP-1 mRNA was reduced through 24 hours, there was a significant reduction in peak bronchoalveolar lavage fluid MCP-1 activity at 48 hours, and there were marked reductions in granuloma size and number at 48 hours. Similar results were observed in animals that received infusions of anti-IL-1 beta. Infusion of anti-IL-1 beta at time 0 resulted in moderate reductions in MCP-1 mRNA at 1 and 6 hours and had no effect on granuloma size or number measured at 48 hours. When multiple infusions of anti-IL-1 beta were administered over a 23-hour period (0 to 23 hours), MCP-1 mRNA was reduced through 24 hours, there was a moderate reduction in peak bronchoalveolar lavage fluid MCP-1 activity at 48 hours, and there were marked reductions in granuloma size and number at 48 hours. A single infusion of anti-TNF-alpha and anti-IL-1 beta together at time 0 resulted in marked reductions in whole lung MCP-1 and mRNA at 1 and 6 hours, but not at 24 hours. Multiple combined infusions of anti-TNF-alpha and anti-IL-1 beta over a 23-hour period resulted in additive reductions in MCP-1 mRNA through 24 hours, bronchoalveolar lavage fluid MCP-1 activity at 48 hours, and granuloma size and number at 48 hours. These data suggest that locally produced TNF-alpha and IL-1 beta play regulatory roles in glucan-induced pulmonary granulomatous vasculitis through the modulation of local MCP-1 production.

摘要

给大鼠静脉注射颗粒状酵母细胞壁葡聚糖会导致以血管为中心的肺肉芽肿同步形成,这些肉芽肿几乎完全由单核细胞和巨噬细胞组成。先前的研究表明,局部产生的单核细胞趋化蛋白-1(MCP-1)是肉芽肿完全形成所必需的。由于肿瘤坏死因子-α(TNF-α)和白细胞介素1(IL-1)可在多种细胞类型中诱导MCP-1的产生,我们试图确定它们在该模型中的潜在调节作用。在注入葡聚糖时(时间0)单次注射抗TNF-α抗体可使1小时和6小时时的MCP-1 mRNA水平显著降低,但在之后的时间点则无此作用;对48小时时测量的肉芽肿大小或数量没有影响。当在23小时内(0至23小时)多次注射抗TNF-α抗体时,MCP-1 mRNA在24小时内均降低,48小时时支气管肺泡灌洗液中MCP-1活性的峰值显著降低,48小时时肉芽肿的大小和数量也显著减少。在接受抗IL-1β注射的动物中观察到了类似的结果。在时间0时注射抗IL-1β可使1小时和6小时时的MCP-1 mRNA适度降低,对48小时时测量的肉芽肿大小或数量没有影响。当在23小时内(0至23小时)多次注射抗IL-1β时,MCP-1 mRNA在24小时内均降低,48小时时支气管肺泡灌洗液中MCP-1活性的峰值适度降低,48小时时肉芽肿的大小和数量也显著减少。在时间0时同时单次注射抗TNF-α和抗IL-1β可使1小时和6小时时全肺MCP-1和mRNA显著降低,但在24小时时则无此作用。在23小时内多次联合注射抗TNF-α和抗IL-1β可使24小时内MCP-1 mRNA、48小时时支气管肺泡灌洗液中MCP-1活性以及48小时时肉芽肿的大小和数量呈累加性降低。这些数据表明,局部产生的TNF-α和IL-1β通过调节局部MCP-1的产生,在葡聚糖诱导的肺肉芽肿性血管炎中发挥调节作用。

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