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Immune response mechanisms against Pseudomonas aeruginosa associated with mucosal immunization with protein antigens in a rat model of acute lung infection

机译:急性肺部感染大鼠模型中铜绿假单胞菌与蛋白抗原黏膜免疫相关的免疫反应机制

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摘要

Pseudomonas aeruginosa is a major cause of nosocomal and community acquired chronic infections in subjects with compromised respiratory function. The microbe is environmentally ubiquitious and has a high level of innate antimicrobial resistance. This has led researchers to investigate vaccine and immunotherapeutic approaches to prevent and treat P. aeruginosa infections. Seven cytosolic non-integral proteins were studied as vaccine candidates in an acute lung infection model in the rat. Five of these (amidase, amidopeptidase, KatE, KatE and Pa13 a novel 13kDa protein) enhanced bacterial clearance from the lung compared to control animals following challenge and are worthy of further study. Immune mechanisms stimulated by these proteins in response to both immunization and infection varied. The most pronounced degree of bacterial clearance from the lung was associated with antigens, which demonstrated greater surface exposure and induced an increase in phagocyte recruitment, in particular, an increased proportion of polymorphonuclear leukocytes. Lymphocytic proliferation and specific antibody responses in the absence of enhanced clearance were less informative as immune correlates.
机译:铜绿假单胞菌是呼吸功能受损的患者发生医院和社区获得性慢性感染的主要原因。微生物在环境上无处不在,并且具有很高的先天抗药性。这导致研究人员研究了预防和治疗铜绿假单胞菌感染的疫苗和免疫疗法。在大鼠的急性肺部感染模型中,研究了七个胞质非整合蛋白作为候选疫苗。与攻击后的对照动物相比,其中的五种(酰胺酶,酰胺肽酶,KatE,KatE和Pa13是一种新型的13kDa蛋白)增强了从肺中清除细菌的能力,值得进一步研究。这些蛋白质对免疫和感染的反应所激发的免疫机制各不相同。细菌从肺部清除的最明显程度与抗原有关,抗原表现出更大的表面暴露并诱导吞噬细胞募集增加,特别是多形核白细胞比例增加。在缺乏增强清除率的情况下,淋巴细胞的增殖和特异性抗体反应由于免疫相关性而提供的信息较少。

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