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Cathelicidin Host Defence Peptide Augments Clearance of Pulmonary Pseudomonas aeruginosa Infection by Its Influence on Neutrophil Function In Vivo

机译:Cathelicidin宿主防御肽对肺中性粒细胞功能的影响增强了铜绿假单胞菌感染的清除率。

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摘要

Cathelicidins are multifunctional cationic host-defence peptides (CHDP; also known as antimicrobial peptides) and an important component of innate host defence against infection. In addition to microbicidal potential, these peptides have properties with the capacity to modulate inflammation and immunity. However, the extent to which such properties play a significant role during infection in vivo has remained unclear. A murine model of acute P. aeruginosa lung infection was utilised, demonstrating cathelicidin-mediated enhancement of bacterial clearance in vivo. The delivery of exogenous synthetic human cathelicidin LL-37 was found to enhance a protective pro-inflammatory response to infection, effectively promoting bacterial clearance from the lung in the absence of direct microbicidal activity, with an enhanced early neutrophil response that required both infection and peptide exposure and was independent of native cathelicidin production. Furthermore, although cathelicidin-deficient mice had an intact early cellular inflammatory response, later phase neutrophil response to infection was absent in these animals, with significantly impaired clearance of P. aeruginosa. These findings demonstrate the importance of the modulatory properties of cathelicidins in pulmonary infection in vivo and highlight a key role for cathelicidins in the induction of protective pulmonary neutrophil responses, specific to the infectious milieu. In additional to their physiological roles, CHDP have been proposed as future antimicrobial therapeutics. Elucidating and utilising the modulatory properties of cathelicidins has the potential to inform the development of synthetic peptide analogues and novel therapeutic approaches based on enhancing innate host defence against infection with or without direct microbicidal targeting of pathogens.
机译:鞘磷脂是多功能阳离子宿主防御肽(CHDP;也称为抗菌肽),是先天宿主防御感染的重要组成部分。除了潜在的杀菌作用外,这些肽还具有调节炎症和免疫能力的特性。但是,尚不清楚在体内感染期间这些特性起着重要作用的程度。利用急性铜绿假单胞菌肺部感染的小鼠模型,证明了cathelicidin介导的体内细菌清除的增强。已发现外源性合成人cathelicidin LL-37的递送增强了对感染的保护性促炎反应,在没有直接杀微生物活性的情况下有效地促进了从肺中的细菌清除,并增强了既需要感染又需要肽的早期中性粒细胞反应暴露,并独立于本地cathelicidin生产。此外,尽管缺乏cathelicidin的小鼠具有完整的早期细胞炎症反应,但在这些动物中却没有后期的中性粒细胞对感染的反应,这严重损害了铜绿假单胞菌的清除率。这些发现证明了cathelicidins的调节特性在体内肺部感染中的重要性,并突出了cathelicidins在诱导针对感染性环境的保护性肺中性粒细胞应答中的关键作用。除了其生理作用外,CHDP还被提议作为未来的抗菌治疗剂。阐明和利用Cathelicidins的调节特性,有可能为合成肽类似物的开发和基于增强先天宿主抵抗病原体直接或间接感染的防御能力的新型治疗方法提供信息。

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