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Structure of apo-phosphatidylinositol transfer protein α provides insight into membrane association

机译:载脂磷脂酰肌醇转移蛋白α的结构为膜结合提供了见识

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摘要

Phosphatidylinositol transfer protein α (PITPα) is a ubiquitous and highly conserved protein in multicellular eukaryotes that catalyzes the exchange of phospholipids between membranes in vitro and participates in cellular phospholipid metabolism, signal transduction and vesicular trafficking in vivo. Here we report the three-dimensional crystal structure of a phospholipid-free mouse PITPα at 2.0 Å resolution. The structure reveals an open conformation characterized by a channel running through the protein. The channel is created by opening the phospholipid-binding cavity on one side by displacement of the C-terminal region and a hydrophobic lipid exchange loop, and on the other side by flattening of the central β-sheet. The relaxed conformation is stabilized at the proposed membrane association site by hydrophobic interactions with a crystallographically related molecule, creating an intimate dimer. The observed open conformer is consistent with a membrane-bound state of PITP and suggests a mechanism for membrane anchoring and the presentation of phosphatidylinositol to kinases and phospholipases after its extraction from the membrane. Coordinates have been deposited in the Protein Data Bank (accession No. 1KCM).
机译:磷脂酰肌醇转移蛋白α(PITPα)是多细胞真核生物中普遍存在且高度保守的蛋白,在体外催化膜之间的磷脂交换,并参与体内的细胞磷脂代谢,信号转导和囊泡运输。在这里我们报告了无磷脂的小鼠PITPα在2.0分辨率下的三维晶体结构。该结构揭示了一个开放构象,其特征是贯穿蛋白质的通道。通过位移C端区域和疏水性脂质交换环,在一侧打开磷脂结合腔,在另一侧通过展平中央β-折叠,形成通道。松弛的构象通过与晶体学相关分子的疏水相互作用而稳定在所提出的膜缔合位点,从而形成紧密的二聚体。观察到的开放构象异构体与PITP的膜结合状态一致,并提出了一种膜锚定的机制以及从膜中提取磷脂酰肌醇后向激酶和磷脂酶呈递的机制。坐标已存放在蛋白质数据库中(登录号1KCM)。

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