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模型磷脂酰胆碱翻转酶的结构特性。

Structural properties of model phosphatidylcholine flippases.

作者信息

Langer Marcella, Sah Rashmi, Veser Anika, Gütlich Markus, Langosch Dieter

机构信息

Lehrstuhl für Chemie der Biopolymere, Department für biowissenschaftliche Grundlagen, Technische Universität München, Weihenstephaner Berg 3, 85354 Freising and Munich Center For Integrated Protein Science (CIPS(M)), Germany.

出版信息

Chem Biol. 2013 Jan 24;20(1):63-72. doi: 10.1016/j.chembiol.2012.11.006.

Abstract

Lipid translocation from one lipid bilayer leaflet to the other, termed flip-flop, is required for the distribution of newly synthesized phospholipids during membrane biogenesis. However, a dedicated biogenic lipid flippase has not yet been identified. Here, we show that the efficiency by which model transmembrane peptides facilitate flip of reporter lipids with different headgroups critically depends on their content of helix-destabilizing residues, the charge state of polar flanking residues, and the composition of the host membrane. In particular, increased backbone dynamics of the transmembrane helix relates to its increased ability to flip lipids with phosphatidylcholine and phosphatidylserine headgroups, whereas a more rigid helix favors phosphatidylethanolamine flip. Further, the transmembrane domains of many SNARE protein subtypes share essential features with the dynamic model peptides. Indeed, recombinant SNAREs possess significant lipid flippase activity.

摘要

脂质从一个脂质双分子层小叶转移到另一个小叶,即所谓的翻转,是膜生物合成过程中新合成磷脂分布所必需的。然而,尚未鉴定出专门的生物合成脂质翻转酶。在此,我们表明,模型跨膜肽促进具有不同头部基团的报告脂质翻转的效率关键取决于其螺旋不稳定残基的含量、极性侧翼残基的电荷状态以及宿主膜的组成。特别是,跨膜螺旋主链动力学的增加与其翻转具有磷脂酰胆碱和磷脂酰丝氨酸头部基团的脂质的能力增加有关,而更刚性的螺旋有利于磷脂酰乙醇胺的翻转。此外,许多SNARE蛋白亚型的跨膜结构域与动态模型肽具有共同的基本特征。事实上,重组SNARE具有显著的脂质翻转酶活性。

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