首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >CRAC motif peptide of the HIV-1 gp41 protein thins SOPC membranes and interacts with cholesterol
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CRAC motif peptide of the HIV-1 gp41 protein thins SOPC membranes and interacts with cholesterol

机译:HIV-1 gp41蛋白的CRAC基序肽使SOPC膜变薄并与胆固醇相互作用

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This study uses low-angle (LAXS) and wide-angle (WAXS) X-ray synchrotron scattering, volume measurements and thin layer chromatography to determine the structure and interactions of SOPC, SOPC/cholesterol mixtures, SOPC/peptide and SOPC/cholesterol/peptide mixtures. N-acetyl-LWYIK-amide (LWYIK) represents the naturally-occurring CRAC motif segment in the pretransmembrane region of the gp41 protein of HIV-1, and N-acetyl-IWYIK-amide (IWYIK), an unnatural isomer, is used as a control. Both peptides thin the SOPC bilayer by similar to 3 angstrom, and cause the area/unit cell (peptide + SOPC) to increase by similar to 9 angstrom(2) from the area/lipid of SOPC at 30 degrees C (67.0 +/- 0.9 angstrom(2)). Model fitting suggests that LWYlK's average position is slightly closer to the bilayer center than IWYIK's, and both peptides are just inside of the phosphate headgroup. Both peptides increase the wide-angle spacing d of SOPC without cholesterol, whereas with 50% cholesterol LWYIK increases d but IWYIK decreases d. TLC shows that LWYIK is more hydrophobic than IWYIK; this difference persists in peptide/SOPC 1:9 mole ratio mixtures. Both peptides counteract the chain ordering effect of cholesterol to roughly the same degree, and both decrease K-C, the bending modulus, thus increasing the SOPC membrane fluidity. Both peptides nucleate crystals of cholesterol, but the LWYIK-induced crystals are weaker and dissolve more easily. (C) 2008 Elsevier B.V. All rights reserved.
机译:这项研究使用低角度(LAXS)和广角(WAXS)X射线同步加速器散射,体积测量和薄层色谱法确定SOPC,SOPC /胆固醇混合物,SOPC /肽和SOPC /胆固醇/的结构和相互作用肽混合物。 N-乙酰基-LWYIK-酰胺(LWYIK)代表HIV-1 gp41蛋白跨膜前区域中天然存在的CRAC基序片段,N-乙酰基-IWYIK-酰胺(IWYIK)是一种非天然异构体,被用作控件。两种肽都使SOPC双层变薄约3埃,并导致面积/单位细胞(肽+ SOPC)在30摄氏度时从SOPC的面积/脂质增加约9埃(2)(67.0 +/- 0.9埃(2))。模型拟合表明,LWYlK的平均位置比IWYIK的平均位置稍微靠近双层中心,并且这两种肽都位于磷酸根基中。两种肽均增加不含胆固醇的SOPC的广角间隔d,而含有50%胆固醇的LWYIK则增加d,而IWYIK则减少d。 TLC显示LWYIK比IWYIK更疏水。这种差异在肽/ SOPC 1:9摩尔比的混合物中仍然存在。两种肽都在大致相同的程度上抵消了胆固醇的链序作用,并且都降低了K-C(弯曲模量),从而增加了SOPC膜的流动性。两种肽都使胆固醇晶体成核,但LWYIK诱导的晶体较弱且更易于溶解。 (C)2008 Elsevier B.V.保留所有权利。

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