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研究载体-自行车缀合物的穿透性和抗菌活性。

Investigating Penetration and Antimicrobial Activity of Vector-Bicycle Conjugates.

机构信息

Department of Biochemistry, University of Cambridge, Cambridge CB2 1QN, U.K.

BicycleTx Limited, Portway Building, Granta Park, Cambridge CB21 6GS, U.K.

出版信息

ACS Infect Dis. 2024 Jul 12;10(7):2381-2389. doi: 10.1021/acsinfecdis.3c00427. Epub 2024 Jun 12.

Abstract

Growing antibiotic resistance is rapidly threatening the efficacy of treatments for Gram-negative infections. Bicycle molecules, constrained bicyclic peptides from diverse libraries generated by bacteriophage display that bind with high affinity to a chosen target are a potential new class of antibiotics. The generally impermeable bacterial outer membrane currently limits the access of peptides to bacteria. The conjugation of membrane active peptides offers an avenue for outer membrane penetration. Here, we investigate which physicochemical properties of a specific membrane active peptide (MAP), derived from ixosin-B, could be tweaked to enhance the penetration of conjugates by generating multiple MAP-Bicycle conjugate variants. We demonstrate that charge and hydrophobicity are important factors, which enhance penetration and, therefore, antimicrobial potency. Interestingly, we show that induction of secondary structure, but not a change in amphipathicity, is vital for effective penetration of the Gram-negative outer membrane. These results offer insights into the ways vectors could be designed to deliver Bicycle molecules (and other cargos) through biological membranes.

摘要

抗生素耐药性的不断增长正在迅速威胁到针对革兰氏阴性感染的治疗效果。通过噬菌体展示生成的具有高亲和力结合特定靶标的约束双环肽( bicyclic peptides )是一类有潜力的新型抗生素。细菌外膜的普遍不可渗透性限制了肽类进入细菌的能力。膜活性肽的缀合为外膜穿透提供了一种途径。在这里,我们研究了从 ixosin-B 衍生的特定膜活性肽 (MAP) 的哪些物理化学性质可以通过生成多种 MAP-约束双环肽缀合物变体来调整,以增强缀合物的穿透能力。我们证明了电荷和疏水性是重要因素,它们可以增强穿透性,从而提高抗菌效力。有趣的是,我们表明,二级结构的诱导而不是两亲性的变化对于革兰氏阴性外膜的有效穿透至关重要。这些结果为设计载体以通过生物膜递送约束双环肽(和其他载体)的方法提供了深入了解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11e6/11249977/e1b1f18a1c4b/id3c00427_0001.jpg

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