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Resistance to Antimicrobial Peptides in Vibrios

机译:对弧菌中抗菌肽的耐药性

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Vibrios are associated with a broad diversity of hosts that produce antimicrobial peptides (AMPs) as part of their defense against microbial infections. In particular, vibrios colonize epithelia, which function as protective barriers and express AMPs as a first line of chemical defense against pathogens. Recent studies have shown they can also colonize phagocytes, key components of the animal immune system. Phagocytes infiltrate infected tissues and use AMPs to kill the phagocytosed microorganisms intracellularly, or deliver their antimicrobial content extracellularly to circumvent tissue infection. We review here the mechanisms by which vibrios have evolved the capacity to evade or resist the potent antimicrobial defenses of the immune cells or tissues they colonize. Among their strategies to resist killing by AMPs, primarily vibrios use membrane remodeling mechanisms. In particular, some highly resistant strains substitute hexaacylated Lipid A with a diglycine residue to reduce their negative surface charge, thereby lowering their electrostatic interactions with cationic AMPs. As a response to envelope stress, which can be induced by membrane-active agents including AMPs, vibrios also release outer membrane vesicles to create a protective membranous shield that traps extracellular AMPs and prevents interaction of the peptides with their own membranes. Finally, once AMPs have breached the bacterial membrane barriers, vibrios use RND efflux pumps, similar to those of other species, to transport AMPs out of their cytoplasmic space.
机译:弧菌与产生抗微生物肽(AMP)的宿主的多样性有关,这是它们抵抗微生物感染的一部分。特别地,弧菌定植在上皮细胞上,其起到保护屏障的作用,并表达AMPs作为抵抗病原体的第一道化学防线。最近的研究表明,它们还可以在吞噬细胞(动物免疫系统的关键组成部分)中定殖。吞噬细胞会渗透到感染的组织中,并使用AMP在细胞内杀死被吞噬的微生物,或者将其抗菌成分释放到细胞外以规避组织感染。我们在这里回顾了弧菌进化出逃避或抵抗其定殖的免疫细胞或组织的有效抗微生物防御能力的机制。在抵抗AMP杀死的策略中,弧菌主要利用膜重塑机制。特别地,一些高抗性菌株用二甘氨酸残基代替六酰化脂质A,以减少其负表面电荷,从而降低其与阳离子AMP的静电相互作用。作为对包膜应力的响应(可能由包括AMP的膜活性剂诱导),弧菌还会释放外膜囊泡,从而形成保护性膜屏障,从而捕获细胞外AMP并阻止肽与自身膜的相互作用。最后,一旦AMP突破了细菌膜屏障,弧菌就使用RND外排泵(与其他物种类似)将AMP运出其细胞质空间。

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