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Lamellar Phases Composed of Phospholipid Cholesterol and Ceramide as Studied by 2H NMR

机译:由磷脂胆固醇和神经酰胺组成的层状相如2h NMR所研究

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摘要

Sphingolipids constitute a significant fraction of cellular plasma membrane lipid content. Among sphingolipids, ceramide levels are usually very low. However, in some cell processes like apoptosis, cell membrane ceramide levels increase markedly because of the activation of enzymes like acid sphingomyelinase. This increase can change the physical state of the membrane by promoting molecular order and inducing solid-ordered (So) phase domains. This effect has been observed in a previous 2H NMR study on membranes consisting of palmitoyl sphingomyelin (PSM) and palmitoyl ceramide (PCer). Cholesterol (Chol), too, is present at high concentrations in mammalian plasma membranes and has a favorable interaction with sphingomyelin (SM), together forming domains in the liquid-ordered phase in model membranes. There are reports that Chol is able to displace ceramide (Cer) in SM bilayers and abolish the So phase domains formed by SM:Cer. This ability of Chol appears to be concentration dependent; in membranes with low Chol and high Cer contents, So phase domains rich in Cer coexist with the continuous fluid phase of the membrane. Here, we studied the effect of increasing PCer concentration in PSM:Chol bilayers, using 2H NMR. Chol:PCer mole ratios were 3:1, 3:2, and 3:3, at a fixed 7:3 phospholipid:cholesterol mol ratio. Both PSM and PCer were monitored in separate samples for changes in their physical state by introducing a perdeuterated palmitoyl chain in either molecule. Moreover, the effect of replacing PSM with DPPC was investigated to test the impact on membrane phase behavior of replacing the sphingosine with a palmitoylated glycerol backbone. We found that PCer can increase acyl chain order in both PSM:Chol and DPPC:Chol bilayers. Especially in bilayers with Chol:PCer 1:1 molar ratios, PCer induces highly stable So phase domains in both PSM and DPPC bilayers near 37°C. However, PCer has a more pronounced ordering effect on PSM compared to DPPC bilayers.
机译:鞘脂素构成细胞血浆膜脂质含量的显着分数。在鞘脂层中,神经酰胺水平通常非常低。然而,在细胞凋亡的一些细胞过程中,由于酸鞘磷脂酶等酶活化,细胞膜神经酰胺水平显着增加。通过促进分子阶和诱导固体有序(SO)相域来改变膜的物理状态。在先前的2H NMR研究中已经观察到这种效果,该研究是由Palmitoyl鞘磷脂(PSM)和Palmitoyl神经酰胺(PCER)组成的膜。胆固醇(CHOL)也存在于哺乳动物血浆膜的高浓度下存在,并且具有与鞘磷脂(SM)的良好相互作用,在模型膜中的液体有序相中形成域。有报道称,CHOL能够在SM双层中移位神经酰胺(CER),并取代SM:CER形成的所以相位域。这种CHOL的能力似乎是浓度依赖性;在具有低Chol和High Cer含量的膜中,使得CER在CER共存的相位域与膜的连续流体相。在此,我们研究了使用2H NMR的PSM:Chol双层在PSM中提高PCer浓度的影响。 CHOL:PCER摩尔比为3:1,3:2和3:3,固定的7:3磷脂:胆固醇摩尔比。在单独的样品中监测PSM和PCER,通过在任何一种分子中引入丙二酸棕榈酰基链来改变其物理状态。此外,研究了用DPPC替代PSM的效果,以测试用棕榈酰胺甘油骨架替换鞘氨醇的膜相行为的影响。我们发现PCer可以在PSM中增加酰基链顺序:CHOL和DPPC:CHOL双层。特别是在具有CHOL的双层:PCER 1:1摩尔比,PPer在PSM和DPPC双层附近的PSM和DPPC双层中诱导高度稳定的所以相位畴。然而,与DPPC双层相比,PCer对PSM有一个更明显的订购效果。

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