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胆固醇和胆固醇双层结构域抑制 alpha-晶体蛋白与眼晶状体纤维细胞膜主要磷脂组成的膜的结合。

Cholesterol and cholesterol bilayer domains inhibit binding of alpha-crystallin to the membranes made of the major phospholipids of eye lens fiber cell plasma membranes.

机构信息

Department of Physics, Boise State University, Boise, ID, 83725, USA.

Biomolecular Sciences Graduate Program, Boise State University, Boise, ID, 83725, USA.

出版信息

Exp Eye Res. 2021 May;206:108544. doi: 10.1016/j.exer.2021.108544. Epub 2021 Mar 17.

Abstract

The concentration of α-crystallin decreases in the eye lens cytoplasm, with a corresponding increase in membrane-bound α-crystallin during cataract formation. The eye lens's fiber cell plasma membrane consists of extremely high cholesterol (Chol) content, forming cholesterol bilayer domains (CBDs) within the membrane. The role of high Chol content in the lens membrane is unclear. Here, we applied the continuous-wave electron paramagnetic resonance spin-labeling method to probe the role of Chol and CBDs on α-crystallin binding to membranes made of four major phospholipids (PLs) of the eye lens, i.e., phosphatidylcholine (PC), sphingomyelin (SM), phosphatidylserine (PS), and phosphatidylethanolamine (PE). Small unilamellar vesicles (SUVs) of PC, SM*, and PS with 0, 23, 33, 50, and 60 mol% Chol and PE* with 0, 9, and 33 mol% Chol were prepared using the rapid solvent exchange method followed by probe-tip sonication. The 1 mol% CSL spin-labels used during SUVs preparation distribute uniformly within the Chol/PL membrane, enabling the investigation of Chol and CBDs' role on α-crystallin binding to the membrane. For PC, SM*, and PS membranes, the binding affinity (K) and the maximum percentage of membrane surface occupied (MMSO) by α-crystallin decreased with an increase in Chol concentration. The K and MMSO became zero at 50 mol% Chol for PC and 60 mol% Chol for SM* membranes, representing that complete inhibition of α-crystallin binding was possible before the formation of CBDs within the PC membrane but only after the formation of CBDs within the SM* membrane. The K and MMSO did not reach zero even at 60 mol% Chol in the PS membrane, representing CBDs at this Chol concentration were not sufficient for complete inhibition of α-crystallin binding to the PS membrane. Both the K and MMSO were zero at 0, 9, and 33 mol% Chol in the PE* membrane, representing no binding of α-crystallin to the PE* membrane with and without Chol. The mobility parameter profiles decreased with an increase in α-crystallin binding to the membranes; however, the decrease was more pronounced for the membrane with lower Chol concentration. These results imply that the membranes become more immobilized near the headgroup regions with an increase in α-crystallin binding; however, the Chol antagonizes the capacity of α-crystallin to decrease the mobility near the headgroup regions of the membranes. The maximum splitting profiles remained the same with an increase in α-crystallin concentration, but there was an increase in the maximum splitting with an increase in the Chol concentration in the membranes. It implies that membrane order near the headgroup regions does not change with an increase in α-crystallin concentration but increases with an increase in Chol concentration in the membrane. Based on our data, we hypothesize that the Chol and CBDs decrease hydrophobicity (increase polarity) near the membrane surface, inhibiting the hydrophobic binding of α-crystallin to the membranes. Thus, our data suggest that Chol and CBDs play a positive physiological role by preventing α-crystallin binding to lens membranes and possibly protecting against cataract formation and progression.

摘要

晶状体细胞质中 α-晶状体蛋白的浓度降低,同时在白内障形成过程中,膜结合的 α-晶状体蛋白相应增加。晶状体纤维细胞膜的胆固醇(Chol)含量极高,在膜内形成胆固醇双层域(CBD)。高胆固醇在晶状体膜中的作用尚不清楚。在这里,我们应用连续波电子顺磁共振自旋标记法研究胆固醇和 CBD 对四种主要眼晶状体磷脂(PL)(即卵磷脂(PC)、鞘磷脂(SM)、磷脂酰丝氨酸(PS)和磷脂酰乙醇胺(PE))膜中 α-晶状体蛋白结合的作用。采用快速溶剂交换法和探针尖端超声处理,制备了 PC、SM和 PS 的小单层囊泡(SUV),胆固醇含量为 0、23、33、50 和 60mol%,PE的胆固醇含量为 0、9 和 33mol%。在 SUV 制备过程中使用的 1mol%CSL 自旋标记物均匀分布在 Chol/PL 膜内,从而能够研究胆固醇和 CBD 对 α-晶状体蛋白与膜结合的作用。对于 PC、SM和 PS 膜,α-晶状体蛋白的结合亲和力(K)和最大膜表面占有率(MMSO)随胆固醇浓度的增加而降低。在 PC 膜中,K 和 MMSO 在 50mol%胆固醇时降为零,在 SM膜中,K 和 MMSO 在 60mol%胆固醇时降为零,这表明在 PC 膜内形成 CBD 之前,完全抑制 α-晶状体蛋白与膜结合是可能的,但仅在 SM膜内形成 CBD 之后才是可能的。即使在 PS 膜中的胆固醇浓度为 60mol%,K 和 MMSO 也未降为零,这表明在该胆固醇浓度下,CBD 不足以完全抑制 α-晶状体蛋白与 PS 膜结合。PE膜中胆固醇含量为 0、9 和 33mol%时,K 和 MMSO 均为零,这表明没有 α-晶状体蛋白与含有和不含有胆固醇的 PE*膜结合。随着 α-晶状体蛋白与膜结合,迁移率参数谱降低;然而,在胆固醇浓度较低的膜中,降低更为明显。这些结果表明,随着 α-晶状体蛋白与膜结合的增加,膜在靠近头部基团区域变得更加固定;然而,胆固醇拮抗了 α-晶状体蛋白降低膜头部基团区域流动性的能力。随着 α-晶状体蛋白浓度的增加,最大分裂谱保持不变,但随着胆固醇浓度在膜内的增加,最大分裂谱增加。这意味着头部基团区域附近的膜有序性不会随 α-晶状体蛋白浓度的增加而改变,但会随膜内胆固醇浓度的增加而增加。基于我们的数据,我们假设胆固醇和 CBD 降低了靠近膜表面的疏水性(增加极性),从而抑制了 α-晶状体蛋白与膜的疏水结合。因此,我们的数据表明,胆固醇和 CBD 通过防止 α-晶状体蛋白与晶状体膜结合并可能防止白内障形成和进展,从而发挥积极的生理作用。

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