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Efficacy of a Proteus mirabilis outer membrane protein vaccine in preventing experimental Proteus pyelonephritis in a BALB/c mouse model.

机译:奇异变形杆菌外膜蛋白疫苗在BALB / c小鼠模型中预防实验性变形杆菌肾盂肾炎的功效。

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摘要

A BALB/c mouse model of nonobstructive, ascending Proteus mirabilis pyelonephritis was characterized bacteriologically, histologically, and serologically from 3 to 28 days. Intravesicular administration of 2 X 10(8) P. mirabilis K7 resulted in the septic death of 9 (16%) of 57 mice by day 15. Among the survivors, K7 colonized the kidneys in great numbers until day 21. Histological examination of the kidneys revealed acute inflammation which was characterized by neutrophil infiltration by day 3, renal necrosis by day 7, and fibroblastic infiltration by day 14 which persisted at least until day 28. The immunoglobulin G response to the outer membrane proteins (OMP) was assessed by enzyme-linked immunosorbent assay and Western blotting (immunoblotting). Anti-OMP immunoglobulin G antibodies were detected as early as day 7, and the reciprocals of their titers rose progressively up to day 28 (i.e., greater than or equal to 500). This model was also used to assess the efficacy of OMP and lipopolysaccharide (LPS) immunization in preventing renal infection. K7 OMP or LPS (100 micrograms) preparations were administered intramuscularly in Freund's complete adjuvant. After 2 weeks, mice were intravesicularly challenged with 2 X 10(8) bacteria of the homologous K7 strain or one of four heterologous strains. Compared with the saline-immunized control group and K7 LPS-immunized mice, K7 OMP recipients were protected from death when challenged by homologous or heterologous strains. In addition, K7 OMP recipients were protected (P less than 0.003) from subsequent renal infection when challenged by the K7 strain and had more rapid bacterial renal clearance when challenged by three of four heterologous strains. OMP recipients produced antibodies which bound major OMP moieties (viz., 36- to 39-kDa cell wall constituents) as assessed by Western blotting. These results support the concept that immunization with selected bacterial protein surface coat constituents can prevent uromucosal infection by interfering with colonization or renal injury.
机译:在3到28天的细菌学,组织学和血清学特征鉴定了非阻塞性升支奇异变形杆菌肾盂肾炎的BALB / c小鼠模型。到第15天,膀胱内施用2 X 10(8)奇异疟原虫K7导致57只小鼠中9例(16%)败血性死亡,在幸存者中,K7在第21天大量移居肾脏。肾脏显示急性炎症,其特征是第3天出现嗜中性白细胞浸润,第7天出现肾坏死,第14天出现纤维母细胞浸润,至少持续到第28天。通过酶评估免疫球蛋白G对外膜蛋白(OMP)的反应联免疫吸附测定和蛋白质印迹(免疫印迹)。最早在第7天就检测到了抗OMP免疫球蛋白G抗体,其效价的倒数一直上升到第28天(即大于或等于500)。该模型还用于评估OMP和脂多糖(LPS)免疫预防肾脏感染的功效。在弗氏完全佐剂中肌内注射K7 OMP或LPS(100微克)制剂。 2周后,用2 X 10(8)同源K7菌株或四种异源菌株之一对小鼠进行囊内攻击。与盐水免疫对照组和K7 LPS免疫小鼠相比,K7 OMP受体在受到同源或异源菌株攻击时可以保护免受死亡。此外,当受到K7菌株攻击时,K7 OMP受体受到保护(P小于0.003)免于随后的肾脏感染,而当受到四个异源菌株中的三个攻击时,其具有更快的细菌性肾脏清除率。通过Western印迹评估,OMP受体产生结合主要OMP部分(即36至39kDa细胞壁成分)的抗体。这些结果支持这样的概念,即用选定的细菌蛋白表面涂层成分进行免疫可以通过干扰定植或肾脏损伤来预防尿道粘膜感染。

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