Merzlyak P G, Yuldasheva L N, Rodrigues C G, Carneiro C M, Krasilnikov O V, Bezrukov S M
Laboratory of Membrane Biophysics, Department of Biophysics and Radiobiology, Federal University of Pernambuco, 50670-901, Recife, PE, Brazil.
Biophys J. 1999 Dec;77(6):3023-33. doi: 10.1016/S0006-3495(99)77133-X.
Asymmetrical (one-sided) application of penetrating water-soluble polymers, polyethylene glycols (PEGs), to a well-defined channel formed by Staphylococcus aureus alpha-toxin is shown to probe channel pore geometry in more detail than their symmetrical (two-sided) application. Polymers added to the cis side of the planar lipid membrane (the side of protein addition) affect channel conductance differently than polymers added to the trans side. Because a satisfactory theory quantitatively describing PEG partitioning into a channel pore does not exist, we apply the simple empirical rules proposed previously (, J. Membr. Biol. 161:83-92) to gauge the size of pore openings as well as the size and position of constrictions along the pore axis. We estimate the radii of the two openings of the channel to be practically identical and equal to 1. 2-1.3 nm. Two apparent constrictions with radii of approximately 0. 9 nm and approximately 0.6-0.7 nm are inferred to be present in the channel lumen, the larger one being closer to the cis side. These structural findings agree well with crystallographic data on the channel structure (, Science. 274:1859-1866) and verify the practicality of polymer probing. The general features of PEG partitioning are examined using available theoretical considerations, assuming there is no attraction between PEG and the channel lumen. It is shown that the sharp dependence of the partition coefficient on polymer molecular weight found under both symmetrical and asymmetrical polymer application can be rationalized within a "hard sphere nonideal solution model." This finding is rather surprising because PEG forms highly flexible coils in water with a Kuhn length of only several Angstroms.
将水溶性渗透聚合物聚乙二醇(PEG)不对称(单侧)应用于由金黄色葡萄球菌α-毒素形成的明确定义的通道,结果表明,与对称(双侧)应用相比,这种方法能更详细地探测通道孔的几何形状。添加到平面脂质膜顺式侧(添加蛋白质的一侧)的聚合物对通道电导的影响与添加到反式侧的聚合物不同。由于不存在能定量描述PEG在通道孔中分配情况的令人满意的理论,我们应用先前提出的简单经验规则(《膜生物学杂志》161:83 - 92)来测量孔开口的大小以及沿孔轴收缩部位的大小和位置。我们估计通道两个开口的半径实际上是相同的,约为1.2 - 1.3纳米。据推断,通道腔内存在两个明显的收缩部位,半径分别约为0.9纳米和约0.6 - 0.7纳米,较大的收缩部位更靠近顺式侧。这些结构发现与关于通道结构的晶体学数据(《科学》274:1859 - 1866)非常吻合,并验证了聚合物探测的实用性。在假设PEG与通道腔之间不存在吸引力的情况下,我们利用现有的理论考量来研究PEG分配的一般特征。结果表明,在聚合物对称和不对称应用情况下发现的分配系数对聚合物分子量的强烈依赖性,可以在“硬球非理想溶液模型”中得到合理的解释。这一发现相当令人惊讶,因为PEG在水中形成高度灵活的线圈,其库恩长度仅为几埃。