Toxic Effects of Butanol in the Plane of the Cell Membrane

IF 3.9 2区 化学 Q2 CHEMISTRY, MULTIDISCIPLINARY Langmuir Pub Date : 2025-01-08 DOI:10.1021/acs.langmuir.4c03677
Luoxi Tan, Haden L. Scott, Micholas Dean Smith, Sai Venkatesh Pingali, Xiaolin Cheng, Hugh M. O’Neill, John Katsaras, Jeremy C. Smith, James G. Elkins, Brian H. Davison, Jonathan D. Nickels
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Abstract

Solvent toxicity limits n-butanol fermentation titer, increasing the cost and energy consumption for subsequent separation processes and making biobased production more expensive and energy-intensive than petrochemical approaches. Amphiphilic solvents such as n-butanol partition into the cell membrane of fermenting microorganisms, thinning the transverse structure, and eventually causing a loss of membrane potential and cell death. In this work, we demonstrate the deleterious effects of n-butanol partitioning upon the lateral dimension of the membrane structure, called membrane domains or lipid rafts. Lipid rafts are regions of the cell membrane enriched with certain lipids, providing a reservoir of high melting temperature lipids and a platform for membrane protein partitioning and oligomerization. Neutron scattering experiments and molecular dynamics simulations revealed that n-butanol increased the size of the lipid domains in a model membrane system. The data showed that n-butanol partitions more into the disordered lipid regions than into the raft-like phase, leading to a differential thinning of these coexisting phases in the plane of the membrane and increasing the hydrophobic mismatch. The resulting increase in line tension at the interface favors domain coalescence to minimize the ratio of the interfacial length to domain area. A detailed computational investigation of the lipid domain interface identifies the boundary as a site of membrane disorder and thinning due to an accumulation of n-butanol. Solvent-induced changes to domain morphology and membrane instability at the domain interface are unrecognized modes of solvent-induced stress to fermenting microbes, representing targets for new solvent tolerance strategies to increase the n-butanol titer.

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丁醇在细胞膜平面的毒性作用
溶剂毒性限制了正丁醇发酵滴度,增加了后续分离过程的成本和能源消耗,使生物基生产比石化方法更昂贵和能源密集型。正丁醇等两亲性溶剂会分割进入发酵微生物的细胞膜,使横向结构变薄,最终导致膜电位丧失和细胞死亡。在这项工作中,我们证明了正丁醇分配对膜结构的横向尺寸的有害影响,称为膜结构域或脂筏。脂筏是细胞膜上富含某些脂质的区域,提供了高温脂质的储存库和膜蛋白分配和寡聚的平台。中子散射实验和分子动力学模拟表明,正丁醇增加了模型膜系统中脂质结构域的大小。数据显示,正丁醇更多地分布在无序的脂质区域,而不是筏状相,导致这些共存相在膜平面上的差异变薄,并增加了疏水错配。界面处线张力的增加有利于畴合并,从而使界面长度与畴面积之比最小。对脂质结构域界面的详细计算研究表明,由于正丁醇的积累,该边界是膜紊乱和变薄的位置。溶剂诱导的结构域形态变化和结构域界面的膜不稳定性是发酵微生物受到溶剂诱导胁迫的未知模式,是提高正丁醇滴度的新溶剂耐受策略的目标。
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来源期刊
Langmuir
Langmuir 化学-材料科学:综合
CiteScore
6.50
自引率
10.30%
发文量
1464
审稿时长
2.1 months
期刊介绍: Langmuir is an interdisciplinary journal publishing articles in the following subject categories: Colloids: surfactants and self-assembly, dispersions, emulsions, foams Interfaces: adsorption, reactions, films, forces Biological Interfaces: biocolloids, biomolecular and biomimetic materials Materials: nano- and mesostructured materials, polymers, gels, liquid crystals Electrochemistry: interfacial charge transfer, charge transport, electrocatalysis, electrokinetic phenomena, bioelectrochemistry Devices and Applications: sensors, fluidics, patterning, catalysis, photonic crystals However, when high-impact, original work is submitted that does not fit within the above categories, decisions to accept or decline such papers will be based on one criteria: What Would Irving Do? Langmuir ranks #2 in citations out of 136 journals in the category of Physical Chemistry with 113,157 total citations. The journal received an Impact Factor of 4.384*. This journal is also indexed in the categories of Materials Science (ranked #1) and Multidisciplinary Chemistry (ranked #5).
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