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提高桃金娘烯醇对混合感染的治疗效果

Increasing the Efficacy of Treatment of - Mixed Infections with Myrtenol.

作者信息

Mahmoud Ruba Y, Trizna Elena Y, Sulaiman Rand K, Pavelyev Roman S, Gilfanov Ilmir R, Lisovskaya Svetlana A, Ostolopovskaya Olga V, Frolova Larisa L, Kutchin Alexander V, Guseva Galina B, Antina Elena V, Berezin Mikhail B, Nikitina Liliya E, Kayumov Airat R

机构信息

Institute of Fundamental Medicine and Biology, Kazan Federal University, 420008 Kazan, Russia.

Varnishes and Paints Department, Kazan National Research Technological University, 420015 Kazan, Russia.

出版信息

Antibiotics (Basel). 2022 Dec 2;11(12):1743. doi: 10.3390/antibiotics11121743.

Abstract

Infectious diseases caused by various nosocomial microorganisms affect worldwide both immunocompromised and relatively healthy persons. Bacteria and fungi have different tools to evade antimicrobials, such as hydrolysis damaging the drug, efflux systems, and the formation of biofilm that significantly complicates the treatment of the infection. Here, we show that myrtenol potentiates the antimicrobial and biofilm-preventing activity of conventional drugs against and mono- and dual-species cultures. In our study, the two optical isomers, (-)-myrtenol and (+)-myrtenol, have been tested as either antibacterials, antifungals, or enhancers of conventional drugs. (+)-Myrtenol demonstrated a synergistic effect with amikacin, fluconazole, and benzalkonium chloride on 64-81% of the clinical isolates of and , including MRSA and fluconazole-resistant fungi, while (-)-myrtenol increased the properties of amikacin and fluconazole to repress biofilm formation in half of the and isolates. Furthermore, myrtenol was able to potentiate benzalkonium chloride up to sixteen-fold against planktonic cells in an - mixed culture and repressed the adhesion of . The mechanism of both (-)-myrtenol and (+)-myrtenol synergy with conventional drugs was apparently driven by membrane damage since the treatment with both terpenes led to a significant drop in membrane potential similar to the action of benzalkonium chloride. Thus, due to the low toxicity of myrtenol, it seems to be a promising agent to increase the efficiency of the treatment of infections caused by bacteria and be fungi of the genus Candida as well as mixed fungal-bacterial infections, including resistant strains.

摘要

由各种医院微生物引起的传染病在全球范围内影响免疫功能低下者和相对健康的人。细菌和真菌有不同的逃避抗菌药物的手段,如水解破坏药物、外排系统以及形成生物膜,这显著使感染的治疗复杂化。在此,我们表明桃金娘烯醇可增强传统药物对 以及单菌种和双菌种培养物的抗菌和预防生物膜形成的活性。在我们的研究中,两种旋光异构体,(-)-桃金娘烯醇和(+)-桃金娘烯醇,已被作为抗菌剂、抗真菌剂或传统药物的增强剂进行测试。(+)-桃金娘烯醇与阿米卡星、氟康唑和苯扎氯铵对64 - 81%的 和 的临床分离株(包括耐甲氧西林金黄色葡萄球菌和耐氟康唑真菌)表现出协同作用,而(-)-桃金娘烯醇在一半的 和 分离株中增强了阿米卡星和氟康唑抑制生物膜形成的特性。此外,在 混合培养中,桃金娘烯醇能够使苯扎氯铵对浮游细胞的活性增强至16倍,并抑制 的黏附。(-)-桃金娘烯醇和(+)-桃金娘烯醇与传统药物协同作用的机制显然是由膜损伤驱动的,因为用这两种萜类化合物处理都会导致膜电位显著下降,类似于苯扎氯铵的作用。因此,由于桃金娘烯醇的低毒性,它似乎是一种有前途的药物,可提高由细菌和念珠菌属真菌引起的感染以及包括耐药菌株在内的真菌 - 细菌混合感染的治疗效率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f071/9774912/4af09908a9bb/antibiotics-11-01743-g001.jpg

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