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Pseudomonas aeruginosa-induced lung and pleural injury in sheep. Differential protective effect of circulating versus alveolar immunoglobulin G antibody.

机译:铜绿假单胞菌诱发绵羊肺和胸膜损伤。循环与肺泡免疫球蛋白G抗体的差异保护作用。

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摘要

The overall objective of these studies was to determine whether IgG antibody to Pseudomonas aeruginosa would modify the acute lung and pleural injury that developed over 24 h after the instillation of 10(10) live P. aeruginosa into the distal airspaces of one lung in unanesthetized sheep. Using a quantitative experimental model to measure protein permeability across the alveolar epithelial, lung endothelial, and pleural mesothelial barriers, the effect of IgG antibody to P. aeruginosa was examined under four different experimental conditions. First, the effect of IgG antibody to P. aeruginosa in the circulation was examined by instilling 10(10) live P. aeruginosa in 5% ovine albumin in sheep that had been vaccinated. Under these conditions, the presence of circulating IgG antibody to P. aeruginosa reduced lung endothelial injury but did not modify the lung epithelial or pleural injury caused by intraalveolar P. aeruginosa. Therefore, the second experimental protocol determined the effect of instilling immune serum from a sheep that had been vaccinated so that IgG antibody to P. aeruginosa was present in both the circulation and in the airspaces along with instillation of live bacteria. Under these conditions, injury to the lung endothelium, alveolar epithelium, and pleural space was completely prevented. Therefore, the third protocol examined the protective effect of instillation of IgG antibody to P. aeruginosa in the airspaces concurrent with the live bacteria. Interestingly, intraalveolar IgG antibody to P. aeruginosa prevented all evidence of lung epithelial and pleural injury, and this effect was associated with a marked decrease in the number of viable bacteria in the lung after 24 h. Therefore, the fourth protocol examined the prophylactic effect of instillation of the specific IgG antibody to P. aeruginosa 24 h before instillation of the bacteria. With this prophylactic regimen, epithelial, endothelial, and pleural injury were prevented, and there was a significant decrease in the number of bacteria recovered from the lung. Thus, delivery of IgG antibody to P. aeruginosa the distal airspaces of the lung alone may provide a novel therapeutic approach to preventing acute pulmonary infection caused by P. aeruginosa.
机译:这些研究的总体目标是确定针对铜绿假单胞菌的IgG抗体是否会改变在未经麻醉的绵羊中将10(10)铜绿假单胞菌滴入一只肺的远端空域后24小时内发生的急性肺和胸膜损伤。使用定量实验模型测量跨肺泡上皮,肺内皮和胸膜间皮屏障的蛋白渗透性,在四种不同的实验条件下检查了针对绿脓杆菌的IgG抗体的作用。首先,通过将10(10)活铜绿假单胞菌滴入已接种疫苗的绵羊的5%绵羊白蛋白中来检查IgG抗体对铜绿假单胞菌在循环中的作用。在这些条件下,针对铜绿假单胞菌的循环IgG抗体的存在减少了肺内皮损伤,但并未改变由肺泡内铜绿假单胞菌引起的肺上皮或胸膜损伤。因此,第二个实验方案确定了从接种过疫苗的绵羊中滴注免疫血清的效果,以至于铜绿假单胞菌的IgG抗体与活菌一起滴注在循环和空域中。在这种情况下,完全防止了肺内皮,肺泡上皮和胸膜腔的损伤。因此,第三方案检查了在与活细菌同时向空域中滴入铜绿假单胞菌IgG抗体的保护作用。有趣的是,针对铜绿假单胞菌的肺泡内IgG抗体阻止了肺上皮和胸膜损伤的所有证据,并且这种作用与24小时后肺中的活菌数量显着减少有关。因此,第四方案检查了在细菌滴注前24 h向铜绿假单胞菌滴注特异性IgG抗体的预防作用。通过这种预防方案,可以预防上皮,内皮和胸膜损伤,并且从肺中回收的细菌数量显着减少。因此,将IgG抗体单独递送至铜绿假单胞菌仅在肺的远端空域可提供预防由铜绿假单胞菌引起的急性肺部感染的新颖治疗方法。

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