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Komodo 巨蜥防御素启发的肽对碳青霉烯类耐药的具有抗菌作用。

Komodo-dragon cathelicidin-inspired peptides are antibacterial against carbapenem-resistant .

机构信息

George Mason University, Manassas, VA, USA.

出版信息

J Med Microbiol. 2020 Nov;69(11):1262-1272. doi: 10.1099/jmm.0.001260. Epub 2020 Oct 21.

DOI:10.1099/jmm.0.001260
PMID:33084564
Abstract

The rise of carbapenem-resistant enterobacteriaceae (CRE) is a growing crisis that requires development of novel therapeutics. To this end, cationic antimicrobial peptides (CAMPs) represent a possible source of new potential therapeutics to treat difficult pathogens such as carbapenem-resistant (CRKP), which has gained resistance to many if not all currently approved antibiotics, making treatment difficult. To examine the anti-CRKP antimicrobial activity of the predicted cathelicidins derived from (Komodo dragon) as well as synthetic antimicrobial peptides that we created. We determined the minimum inhibitory concentrations of the peptides against CRKP. We also characterized the abilities of these peptides to disrupt the hyperpolarization of the bacterial membrane as well as their ability to form pores in the membrane. We did not observe significant anti-CRKP activity for the predicted native Komodo cathelicidin peptides. We found that the novel peptides DRGN-6,-7 and -8 displayed significant antimicrobial activity against CRKP with MICs of 4-8 µg ml. DRGN-6 peptide was the most effective peptide against CRKP. Unfortunately, these peptides showed higher than desired levels of hemolysis, although testing in the waxworm showed no mortality associated with treatment by the peptide; however, CRKP-infected waxworms treated with peptide did not show an improvement in survival. Given the challenges of treating CRKP, identification of peptides with activity against it represents a promising avenue for further research. Given DRGN-6's similar level of activity to colistin, DRGN-6 is a promising template for the development of novel antimicrobial peptide-based therapeutics.

摘要

耐碳青霉烯肠杆菌科 (CRE) 的出现是一个日益严重的危机,需要开发新的治疗方法。为此,阳离子抗菌肽 (CAMP) 代表了一种新的潜在治疗方法的可能来源,可以治疗一些具有挑战性的病原体,如耐碳青霉烯的 (CRKP),它对许多甚至所有目前批准的抗生素都产生了耐药性,使得治疗变得困难。为了研究源自 (科莫多巨蜥)的预测的抗菌肽和我们合成的抗菌肽对耐碳青霉烯肠杆菌的抗微生物活性。我们测定了这些肽对 CRKP 的最小抑菌浓度。我们还描述了这些肽破坏细菌膜超极化的能力以及它们在膜中形成孔的能力。我们没有观察到预测的天然科莫多巨蜥抗菌肽对 CRKP 有显著的抗活性。我们发现,新型肽 DRGN-6、-7 和 -8 对 CRKP 具有显著的抗菌活性,MIC 为 4-8μg/ml。DRGN-6 肽对 CRKP 最有效。不幸的是,这些肽的溶血水平高于预期,尽管在蜡虫中进行的测试表明,肽治疗没有导致死亡;然而,用肽治疗的感染 CRKP 的蜡虫在存活率上没有改善。鉴于治疗 CRKP 的挑战,鉴定对其具有活性的肽代表了进一步研究的有前途的途径。鉴于 DRGN-6 对粘菌素的活性相似,DRGN-6 是开发新型抗菌肽基于治疗的有前途的模板。

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