Department of Chemical Engineering, Indian Institute of Science, Bangalore-560012, India.
Soft Matter. 2020 May 28;16(20):4840-4857. doi: 10.1039/d0sm00086h. Epub 2020 May 18.
Infections caused by many virulent bacterial strains are triggered by the release of pore forming toxins (PFTs), which form oligomeric transmembrane pore complexes on the target plasma membrane. The spatial extent of the perturbation to the surrounding lipids during pore formation is relatively unexplored. Using all-atom molecular dynamics simulations, we investigate the changes in the structure and dynamics of lipids in a 1,2-dimyristoyl-sn-glycero-3-phosphocholine (DMPC) lipid bilayer in the presence of contrasting PFTs. Cytolysin A (ClyA), an α toxin with its inserted wedge shaped bundle of inserted α helices, induces significant asymmetry across the membrane leaflets in comparison with α hemolysin (AHL), a β toxin. Despite the differences in hydrophobic mismatch and uniquely different topologies of the two oligomers, perturbations to lipid order as reflected in the tilt angle and order parameters and membrane thinning are short ranged, lying within ∼2.5 nm from the periphery of either pore complex, and commensurate with distances typically associated with van der Waals forces. In contrast, the spatial extent of perturbations to the lipid dynamics extends outward to at least 4 nm for both proteins, and the continuous survival probabilities reveal the presence of a tightly bound shell of lipids in this region. Displacement probability distributions show long tails and the distinctly non-Gaussian features reflect the induced dynamic heterogeneity. A detailed profiling of the protein-lipid contacts with tyrosine, tryptophan, lysine and arginine residues shows increased non-polar contacts in the cytoplasmic leaflet for both PFTs, with a higher number of atomic contacts in the case of AHL in the extracellular leaflet due to the mushroom-like topology of the pore complex. The short ranged nature of the perturbations observed in this simple one component membrane suggests inherent plasticity of membrane lipids enabling the recovery of the structure and membrane fluidity even in the presence of these large oligomeric transmembrane protein assemblies. This observation has implications in membrane repair processes such as budding or vesicle fusion events used to mitigate PFT virulence, where the underlying lipid dynamics and fluidity in the vicinity of the pore complex are expected to play an important role.
许多毒性很强的细菌菌株引起的感染是由形成孔的毒素(PFT)释放触发的,这些毒素在靶质膜上形成寡聚跨膜孔复合物。在孔形成过程中,周围脂质的扰动空间范围相对没有得到探索。我们使用全原子分子动力学模拟,研究了在存在对比性 PFT 的情况下,1,2-二肉豆蔻酰基-sn-甘油-3-磷酸胆碱(DMPC)脂质双层中脂质结构和动力学的变化。细胞溶素 A(ClyA)是一种带有插入楔形束插入α螺旋的α毒素,与β毒素α溶血素(AHL)相比,在膜叶之间引起明显的不对称。尽管两种寡聚物的疏水性不匹配和独特的拓扑结构存在差异,但脂质有序性的扰动,如倾斜角和有序参数以及膜变薄,都是短程的,位于两个孔复合物的外围约 2.5nm 范围内,与范德华力通常相关的距离相当。相比之下,脂质动力学的扰动空间范围向外延伸到至少 4nm 对于两种蛋白质都是如此,连续的生存概率表明在该区域存在紧密结合的脂质壳。位移概率分布显示长尾,明显的非高斯特征反映了诱导的动态异质性。对与酪氨酸、色氨酸、赖氨酸和精氨酸残基的蛋白质-脂质接触进行详细分析表明,两种 PFT 细胞质叶都有更多的非极性接触,而由于孔复合物的蘑菇状拓扑结构,AHL 在外质叶中原子接触数量更多。在这种简单的单成分膜中观察到的扰动的短程性质表明,即使存在这些大型跨膜蛋白寡聚物,膜脂质具有固有可塑性,能够恢复结构和膜流动性。这种观察结果对膜修复过程具有启示意义,例如出芽或囊泡融合事件,用于减轻 PFT 的毒力,预计在孔复合物附近的潜在脂质动力学和流动性将发挥重要作用。
