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开发全-D型奥米加南治疗耐莫匹罗星耐甲氧西林金黄色葡萄球菌皮肤感染的初步研究。

Preliminary investigations into developing all-D Omiganan for treating Mupirocin-resistant MRSA skin infections.

作者信息

Ng Siew Mei Samantha, Teo Shu Wei, Yong Yaqing Elena, Ng Fui Mee, Lau Qiu Ying, Jureen Roland, Hill Jeffrey, Chia C S Brian

机构信息

Experimental Therapeutics Centre, Agency for Science, Technology and Research (A*STAR), Singapore.

Department of Laboratory Medicine, National University Hospital, Singapore.

出版信息

Chem Biol Drug Des. 2017 Dec;90(6):1155-1160. doi: 10.1111/cbdd.13035. Epub 2017 Jul 11.

Abstract

Staphylococcus aureus is the primary pathogen responsible for the majority of human skin infections, and meticillin-resistant S. aureus (MRSA) currently presents a major clinical concern. The overuse of Mupirocin, the first-line topical antibacterial drug over 30 years, has led to the emergence of Mupirocin-resistant MRSA, creating a clinical concern. The antimicrobial peptide Omiganan was touted to be a promising antibacterial drug candidate due to its rapid membrane-disrupting bactericidal mode of action, entering clinical trials in 2005 as a topical gel to prevent catheter site infections. However, drug development ceased in 2009 due to a lack of efficacy. We postulate this to be due to proteolytic degradation caused by endogenous human skin proteases. Herein, we tested our hypothesis using Omiganan and its all-D enantiomer in a human skin protease stability assay, followed by anti-MRSA activity assay against of a panel of clinical MRSA isolates, a bactericidal/static determination and a time-kill assay to gauge all-D Omiganan's potential for further topical antibacterial drug development.

摘要

金黄色葡萄球菌是导致大多数人类皮肤感染的主要病原体,而耐甲氧西林金黄色葡萄球菌(MRSA)目前是一个主要的临床关注点。莫匹罗星作为一线外用抗菌药物已使用超过30年,其过度使用导致了耐莫匹罗星MRSA的出现,引发了临床关注。抗菌肽奥米加南因其快速破坏膜的杀菌作用方式而被吹捧为一种有前景的抗菌药物候选物,于2005年作为一种外用凝胶进入临床试验以预防导管部位感染。然而,由于缺乏疗效,药物研发于2009年停止。我们推测这是由于人体皮肤内源性蛋白酶引起的蛋白水解降解所致。在此,我们在人体皮肤蛋白酶稳定性试验中使用奥米加南及其全D对映体来检验我们的假设,随后针对一组临床MRSA分离株进行抗MRSA活性试验、杀菌/抑菌测定以及时间杀菌试验,以评估全D奥米加南用于进一步外用抗菌药物研发的潜力。

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