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革兰氏阴性杆菌对宿主抗菌蛋白的敏感性。

Sensitization of Gram-Negative Bacilli to Host Antibacterial Proteins.

机构信息

Department of Biotechnology and Food Engineering, Technion-Israel Institute of Technology, Haifa, Israel.

出版信息

J Infect Dis. 2017 May 15;215(10):1599-1607. doi: 10.1093/infdis/jix119.

Abstract

To address the need for novel alternatives to antibiotics, we attempted to sensitize gram-negative bacilli to innate antibacterial protagonists. We report a lipopeptide-like sequence (C10OOc12O) that inflicted outer membrane damage at a low micromolar range, whereas measurable bacterial growth inhibition in broth medium required >10-fold higher concentrations. In serum, however, C10OOc12O induced antibacterial activity in a manner suppressible by anticomplement antibodies or heat treatment and acted synergistically with exogenous lysozyme in broth and serum media. Upon subcutaneous administration, C10OOc12O exhibited high circulating levels that correlated with significant therapeutic efficacies, using either the mouse peritonitis-sepsis model or the thigh infection model. These findings are consistent with the view that, by damaging the outer membrane, C10OOc12O was able to enhance gram-negative bacilli susceptibility to antibacterial components of the immune humoral arm. Such lipopeptides may therefore be useful in fighting gram-negative bacilli threats through sensitization to endogenous and/or exogenous antibacterial proteins such as lysozyme and complements.

摘要

为了解决对抗生素的新需求,我们试图使革兰氏阴性菌对先天的抗菌主角敏感。我们报告了一个类似脂肽的序列(C10OOc12O),它在低微摩尔范围内造成外膜损伤,而在肉汤培养基中可测量的细菌生长抑制需要高出 10 倍的浓度。然而,在血清中,C10OOc12O 以可被抗补体抗体或热处理抑制的方式诱导抗菌活性,并在肉汤和血清培养基中与外源性溶菌酶协同作用。皮下给药后,C10OOc12O 表现出与显著治疗功效相关的高循环水平,无论是在小鼠腹膜炎-败血症模型还是大腿感染模型中。这些发现与以下观点一致,即通过破坏外膜,C10OOc12O 能够增强革兰氏阴性菌对免疫体液臂中抗菌成分的敏感性。因此,此类脂肽可通过对溶菌酶和补体等内源性和/或外源性抗菌蛋白的敏感化来用于对抗革兰氏阴性菌的威胁。

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