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抗真菌肽Cm-p5的衍生物在体外抑制生物膜的形成。

Derivates of the Antifungal Peptide Cm-p5 Inhibit Development of Biofilms In Vitro.

作者信息

Kubiczek Dennis, Raber Heinz, Gonzalez-García Melaine, Morales-Vicente Fidel, Staendker Ludger, Otero-Gonzalez Anselmo J, Rosenau Frank

机构信息

Institute of Pharmaceutical Biotechnology, Ulm University, 89081 Ulm, Germany.

Center for Protein Studies, Faculty of Biology, University of Havana, 25 Str. and I Str., La Habana 10400, Cuba.

出版信息

Antibiotics (Basel). 2020 Jun 27;9(7):363. doi: 10.3390/antibiotics9070363.

Abstract

Growth in biofilms as a fascinating and complex microbial lifestyle has become widely accepted as one of the key features of pathogenic microbes, to successfully express their full virulence potential and environmental persistence. This also increases the threat posed by , which has a high intrinsic ability to persist on abiotic surfaces including those of surgical instruments and medical tubing. In a previous study, cyclic and helical-stabilized analogues of the antifungal peptide Cm-p5 were designed and synthetized, and proved to have increased activities against and , but not against planktonic cells cultivated in suspension cultures. Here, we demonstrate, initially, that these derivatives, however, exhibited semi-inhibitory concentrations between 10-21 µg/mL toward biofilms. Maturated biofilms were also arrested between 71-97%. These novel biofilm inhibitors may open urgently needed new routes for the development of novel drugs and treatments for the next stage of fight against .

摘要

生物膜的生长作为一种迷人且复杂的微生物生存方式,已被广泛认为是致病微生物的关键特征之一,有助于它们充分发挥其全部毒力潜能并在环境中持久存在。这也增加了由[具体微生物名称未给出]所构成的威胁,该微生物具有很强的在非生物表面(包括手术器械和医用管道表面)持久存在的内在能力。在先前的一项研究中,设计并合成了抗真菌肽Cm-p5的环状和螺旋稳定类似物,事实证明这些类似物对[具体微生物名称未给出]和[具体微生物名称未给出]具有增强的活性,但对悬浮培养中生长的浮游[具体微生物名称未给出]细胞没有活性。在此,我们首先证明,这些衍生物对[具体微生物名称未给出]生物膜的半抑制浓度在10 - 21μg/mL之间。成熟生物膜的生长也被抑制了71 - 97%。这些新型生物膜抑制剂可能为开发对抗[具体微生物名称未给出]下一阶段所需的新型药物和治疗方法开辟迫切需要的新途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3456/7400495/d50085c9c1db/antibiotics-09-00363-g001.jpg

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