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分枝杆菌溃疡分枝杆菌毒素 mycolactone 的膜扰动特性。

Membrane perturbing properties of toxin mycolactone from Mycobacterium ulcerans.

机构信息

Theoretical Biology and Biophysics Group, Los Alamos National Laboratory, New Mexico, United States of America.

Center for Nonlinear Studies, Los Alamos National Laboratory, New Mexico, United States of America.

出版信息

PLoS Comput Biol. 2018 Feb 5;14(2):e1005972. doi: 10.1371/journal.pcbi.1005972. eCollection 2018 Feb.

Abstract

Mycolactone is the exotoxin produced by Mycobacterium ulcerans and is the virulence factor behind the neglected tropical disease Buruli ulcer. The toxin has a broad spectrum of biological effects within the host organism, stemming from its interaction with at least two molecular targets and the inhibition of protein uptake into the endoplasmic reticulum. Although it has been shown that the toxin can passively permeate into host cells, it is clearly lipophilic. Association with lipid carriers would have substantial implications for the toxin's distribution within a host organism, delivery to cellular targets, diagnostic susceptibility, and mechanisms of pathogenicity. Yet the toxin's interactions with, and distribution in, lipids are unknown. Herein we have used coarse-grained molecular dynamics simulations, guided by all-atom simulations, to study the interaction of mycolactone with pure and mixed lipid membranes. Using established techniques, we calculated the toxin's preferential localization, membrane translocation, and impact on membrane physical and dynamical properties. The computed water-octanol partition coefficient indicates that mycolactone prefers to be in an organic phase rather than in an aqueous environment. Our results show that in a solvated membrane environment the exotoxin mainly localizes in the water-membrane interface, with a preference for the glycerol moiety of lipids, consistent with the reported studies that found it in lipid extracts of the cell. The calculated association constant to the model membrane is similar to the reported association constant for Wiskott-Aldrich syndrome protein. Mycolactone is shown to modify the physical properties of membranes, lowering the transition temperature, compressibility modulus, and critical line tension at which pores can be stabilized. It also shows a tendency to behave as a linactant, a molecule that localizes at the boundary between different fluid lipid domains in membranes and promotes inter-mixing of domains. This property has implications for the toxin's cellular access, T-cell immunosuppression, and therapeutic potential.

摘要

Mycolactone 是分枝杆菌溃疡亚种产生的外毒素,也是被忽视的热带病——布鲁里溃疡的致病因子。该毒素在宿主生物体中有广泛的生物学效应,源于其与至少两个分子靶标相互作用,并抑制内质网中蛋白质的摄取。尽管已经表明该毒素可以被动地渗透进入宿主细胞,但它显然是亲脂性的。与脂质载体的结合将对毒素在宿主生物体中的分布、向细胞靶标的输送、诊断敏感性以及致病机制产生重大影响。然而,毒素与脂质的相互作用及其在脂质中的分布情况尚不清楚。在此,我们使用粗粒分子动力学模拟,在全原子模拟的指导下,研究了分枝杆菌溃疡素与纯质和混合脂质膜的相互作用。使用已建立的技术,我们计算了毒素的优先定位、膜转位以及对膜物理和动力学性质的影响。计算得到的水-辛醇分配系数表明,分枝杆菌溃疡素更倾向于存在于有机相中,而不是在水相环境中。我们的结果表明,在溶剂化的膜环境中,外毒素主要定位于水-膜界面,优先与脂质的甘油部分结合,这与报道的研究结果一致,该研究在细胞的脂质提取物中发现了分枝杆菌溃疡素。计算得到的与模型膜的结合常数与报道的威特综合征蛋白的结合常数相似。分枝杆菌溃疡素被证明会改变膜的物理性质,降低相变温度、压缩模量和临界线张力,从而稳定孔的形成。它还表现出作为一种 linactant 的倾向,linactant 是一种在膜中不同流体脂质区域的边界处定位并促进区域混合的分子。这种性质对毒素的细胞进入、T 细胞免疫抑制和治疗潜力都有影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3e01/5814095/6b912f2701ea/pcbi.1005972.g001.jpg

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