Biochemistry, Department of Biosciences, Åbo Akademi University, Turku, Finland.
Biophys J. 2011 Jun 8;100(11):2633-41. doi: 10.1016/j.bpj.2011.03.066.
The interaction between cholesterol and phospholipids in bilayer membranes is important for the formation and maintenance of membrane structure and function. However, cholesterol does not interact favorably with all types of phospholipids and, for example, prefers more ordered sphingomyelins (SMs) over phosphatidylcholines (PCs). The reason for this preference is not clear. Here we have studied whether acyl-chain order could be responsible for the preferred sterol interaction with SMs. Acyl-chain order was deduced from diphenylhexatriene anisotropy and from the deuterium order parameter obtained by (2)H-NMR on bilayers made from either 14:0/14:0((d27))-PC, or 14:0((d27))-SM. Sterol/phospholipid interaction was determined from sterol bilayer partitioning. Cholestatrienol (CTL) was used as a fluorescence probe for cholesterol, because its relative membrane partitioning is similar to cholesterol. When CTL was allowed to reach equilibrium partitioning between cyclodextrins and unilamellar vesicles made from either 14:0/14:0-PC or 14:0-SM, the molar-fraction partitioning coefficient (K(x)) was approximately twofold higher for SM bilayers than for PC bilayers. This was even the case when the temperature in the SM samples was raised to achieve equal acyl-chain order, as determined from 1,6-diphenyl-1,3,5-hexatriene (DPH) anisotropy and the deuterium order parameter. Although the K(x) did increase with acyl-chain order, the higher K(x) for SM bilayers was always evident. At equal acyl-chain order parameter (DPH anisotropy), the K(x) was also higher for 14:0-SM bilayers than for bilayers made from either 14:0/15:0-PC or 15:0-/14:0-PC, suggesting that minor differences in chain length or molecular asymmetry are not responsible for the difference in K(x). We conclude that acyl-chain order affects the bilayer affinity of CTL (and thus cholesterol), but that it is not the cause for the preferred affinity of sterols for SMs over matched PCs. Instead, it is likely that the interfacial properties of SMs influence and stabilize interactions with sterols in bilayer membranes.
胆固醇与双层膜中磷脂的相互作用对于膜结构和功能的形成和维持很重要。然而,胆固醇与所有类型的磷脂的相互作用并不理想,例如,它更喜欢更有序的神经鞘磷脂(SM)而不是磷脂酰胆碱(PC)。这种偏好的原因尚不清楚。在这里,我们研究了酰基链有序性是否可能是固醇与 SM 优先相互作用的原因。通过二苯基己三烯各向异性和(2)H-NMR 获得的二氘序参数推导出酰基链有序性,该二氘序参数来自于由 14:0/14:0((d27))-PC 或 14:0((d27))-SM 制成的双层膜。固醇/磷脂相互作用通过固醇双层分配来确定。胆甾烯醇(CTL)被用作胆固醇的荧光探针,因为其相对膜分配与胆固醇相似。当 CTL 被允许在环糊精和由 14:0/14:0-PC 或 14:0-SM 制成的单层囊泡之间达到平衡分配时,SM 双层的摩尔分数分配系数(K(x))大约是 PC 双层的两倍。即使在提高 SM 样品温度以达到相等的酰基链有序性的情况下,也是如此,这可以通过 1,6-二苯基-1,3,5-己三烯(DPH)各向异性和氘序参数来确定。尽管 K(x)随酰基链有序性增加而增加,但 SM 双层的 K(x)总是明显更高。在相等的酰基链有序参数(DPH 各向异性)下,14:0-SM 双层的 K(x)也高于由 14:0/15:0-PC 或 15:0-/14:0-PC 制成的双层,这表明链长或分子不对称性的微小差异不是 K(x)差异的原因。我们得出结论,酰基链有序性影响 CTL(和胆固醇)对双层的亲和力,但它不是固醇优先与 SM 而不是匹配的 PC 相互作用的原因。相反,SM 的界面性质可能影响并稳定双层膜中固醇的相互作用。
