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Structural basis for glycosphingolipid transfer specificity

机译:糖鞘脂转移特异性的结构基础

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Lipid transfer proteins are important in membrane vesicle biogenesis and trafficking, signal transduction and immunological presentation processes(1-3). The conserved and ubiquitous mammalian glycolipid transfer proteins (GLTPs) serve as potential regulators of cell processes mediated by glycosphingolipids, ranging from differentiation and proliferation to invasive adhesion, neurodegeneration and apoptosis(4,5). Here we report crystal structures of apo-GLTP (1.65 Angstrom resolution) and lactosylceramide-bound (1.95 Angstrom) GLTP, in which the bound glycosphingolipid is sandwiched, after adaptive recognition, within a previously unknown two-layer all-alpha-helical topology. Glycosphingolipid binding specificity is achieved through recognition and anchoring of the sugar-amide headgroup to the GLTPlipid recognition centre and within the hydrophobic tunnel support a framework for understanding how GLTPs acquire and release glycosphingolipids during lipid intermembrane transfer and presentation processes.
机译:脂质转移蛋白在膜囊泡的生物发生和运输,信号转导和免疫学呈递过程中很重要(1-3)。保守且普遍存在的哺乳动物糖脂转移蛋白(GLTP)充当糖鞘脂介导的细胞过程的潜在调节剂,范围从分化和增殖到侵袭性粘附,神经变性和凋亡(4,5)。在这里,我们报告apo-GLTP(1.65埃分辨率)和乳糖基神经酰胺结合(1.95埃)GLTP的晶体结构,其中在自适应识别后,结合的糖鞘脂被夹在先前未知的两层全α-螺旋拓扑中。糖鞘脂的结合特异性是通过糖酰胺头基的识别和锚定到GLTP脂质识别中心而实现的,并且在疏水通道内为理解GLTP如何在脂质间膜转移和呈递过程中获取和释放糖鞘脂提供了框架。

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