首页> 外文OA文献 >Effect of the Structure of Lipids Favoring Disordered Domain Formation on the Stability of Cholesterol-Containing Ordered Domains (Lipid Rafts): Identification of Multiple Raft-Stabilization Mechanisms
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Effect of the Structure of Lipids Favoring Disordered Domain Formation on the Stability of Cholesterol-Containing Ordered Domains (Lipid Rafts): Identification of Multiple Raft-Stabilization Mechanisms

机译:有利于无序域形成的脂质结构对胆固醇有序域(脂质筏)稳定性的影响:多种筏稳定机制的鉴定

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摘要

Despite the importance of lipid rafts, commonly defined as liquid-ordered domains rich in cholesterol and in lipids with high gel-to-fluid melting temperatures (Tm), the rules for raft formation in membranes are not completely understood. Here, a fluorescence-quenching strategy was used to define how lipids with low Tm, which tend to form disordered fluid domains at physiological temperatures, can stabilize ordered domain formation by cholesterol and high-Tm lipids (either sphingomyelin or dipalmitoylphosphatidylcholine). In bilayers containing mixtures of low-Tm phosphatidylcholines, cholesterol, and high-Tm lipid, the thermal stability of ordered domains decreased with the acyl-chain structure of low-Tm lipids in the following order: diarachadonyl > diphytanoyl > 1-palmitoyl 2-docosahexenoyl = 1,2 dioleoyl = dimyristoleoyl = 1-palmitoyl, 2-oleoyl (PO). This shows that low-Tm lipids with two acyl chains having very poor tight-packing propensities can stabilize ordered domain formation by high-Tm lipids and cholesterol. The effect of headgroup structure was also studied. We found that even in the absence of high-Tm lipids, mixtures of cholesterol with PO phosphatidylethanolamine (POPE) and PO phosphatidylserine (POPS) or with brain PE and brain PS showed a (borderline) tendency to form ordered domains. Because these lipids are abundant in the inner (cytofacial) leaflet of mammalian membranes, this raises the possibility that PE and PS could participate in inner-leaflet raft formation or stabilization. In bilayers containing ternary mixtures of PO lipids, cholesterol, and high-Tm lipids, the thermal stability of ordered domains decreased with the polar headgroup structure of PO lipids in the order PE > PS > phosphatidylcholine (PC). Analogous experiments using diphytanoyl acyl chain lipids in place of PO acyl chain lipids showed that the stabilization of ordered lipid domains by acyl chain and headgroup structure was not additive. This implies that it is likely that there are two largely mutually exclusive mechanisms by which low-Tm lipids can stabilize ordered domain formation by high-Tm lipids and cholesterol: 1), by having structures resulting in immiscibility of low-Tm and high-Tm lipids, and 2), by having structures allowing them to pack tightly within ordered domains to a significant degree.
机译:尽管脂筏很重要,脂筏通常定义为富含胆固醇的脂类和具有高的凝胶-流体熔融温度(Tm)的脂类的有序结构域,但尚未完全理解在膜中形成筏的规则。在这里,荧光猝灭策略用于定义在生理温度下倾向于形成无序流体域的低Tm脂质如何稳定胆固醇和高Tm脂质(鞘磷脂或二棕榈酰磷脂酰胆碱)形成的有序域的形成。在包含低Tm磷脂酰胆碱,胆固醇和高Tm脂质的混合物的双层中,有序域的热稳定性随低Tm脂质的酰基链结构按以下顺序降低:花生四烯酸基>二植烷酰基> 1-棕榈酰基2- docosahexenoyl = 1,2,二油酰基=二肉豆蔻酰基= 1-棕榈酰基,2-油酰基(PO)。这表明具有两个非常弱的紧密堆积倾向的酰基链的低Tm脂质可以稳定高Tm脂质和胆固醇形成的有序结构域。还研究了头部结构的影响。我们发现,即使没有高Tm脂质,胆固醇与PO磷脂酰乙醇胺(POPE)和PO磷脂酰丝氨酸(POPS)或与脑PE和脑PS的混合物也显示出(边界)形成有序域的趋势。由于这些脂质在哺乳动物膜的内部(细胞表面)小叶中含量很高,因此增加了PE和PS参与内部小叶筏形成或稳定的可能性。在包含PO脂质,胆固醇和高Tm脂质的三元混合物的双层中,有序域的热稳定性随PO脂质的极性头基结构而降低,顺序为PE> PS>磷脂酰胆碱(PC)。使用二植烷酰基酰基链脂质代替PO酰基链脂质的类似实验表明,通过酰基链和头基结构对有序脂质结构域的稳定作用不是累加的。这暗示着低Tm脂质可能通过两种相互排斥的机制来稳定高Tm脂质和胆固醇形成的有序结构域的形成:1)通过具有导致低Tm和高Tm不溶混的结构2),通过具有允许它们在有序域内紧密堆积的结构达到显着程度。

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