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In vitro and in vivo efficacy of Caenorhabditis elegans recombinant antimicrobial protein against Gram-negative bacteria

机译:在体外和体内肌肉杆菌的体内疗效重组抗菌蛋白免受革兰氏阴性细菌的体外抗微生物蛋白

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摘要

Antimicrobial peptides (AMPs) are short, positively charged host defense peptides, found in various life forms from microorganisms to humans. AMPs are gaining more attention as substitutes for antibiotics in order to combat the risk posed by multi-drug- resistant pathogens. The nematode Caenorhabditis elegans relies solely on its innate immune defense to cope with its challenging life-style. Bacterial infection in C. elegans leads to induction of antimicrobial proteins, defensins, nemapores, cecropins, and neuropeptide-like proteins, which act to limit bacterial proliferation. This study reports how the C. elegans recombinant antibacterial factor (ABF-1) rapidly inhibited bacterial growth (Salmonella Typhi, Klebsiella pneumonia, Shigella sonnei and Vibrio alginolyticus). The ABF-1 exposure on S. Typhi, showed differential regulation in cell-cycle, DNA repair mechanism, membrane stability, and stress related proteins. The exogenous supply of ABF-1 protein has extended C. elegans survival by reducing the bacterial colony forming units on the nematode intestine. Together, these findings indicate the valuable and potential therapeutic applications of ABF-1 protein as antimicrobial agents against intracellular pathogens.
机译:抗微生物肽(AMPS)是短,带正电荷的宿主防御肽,在各种生命中发现了来自微生物对人类的形式。安培在抗生素的替代品中获得更多关注,以便打击由多药物耐药病原体引起的风险。 Nematode CaenorhabditiseDellys仅依赖于其天生的免疫防御,以应对挑战性生活风格。 C.埃贝朗斯的细菌感染导致诱导抗菌蛋白质,防御素,Nemorcore,Cecropins和神经肽样蛋白,其采取限制细菌增殖。本研究报告了C. elegans重组抗菌因子(ABF-1)如何快速抑制细菌生长(沙门氏菌Typhi,Klebsiella Pneumonia,Shigella Sonnei和Vibrio Alginolyticus)。 ABF-1在S.Typhi上暴露,显示细胞周期,DNA修复机制,膜稳定性和应力相关蛋白的差异调节。通过在线虫肠道上减少细菌菌落形成单元,ABF-1蛋白的外源性供应延伸了C.杆状杆菌存活。这些发现在一起表明ABF-1蛋白作为针对细胞内病原体的抗微生物剂的有价值和潜在治疗应用。

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