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人类凋亡磷脂翻转酶Xkr4的结构与功能

Structure and function of the human apoptotic scramblase Xkr4.

作者信息

Chakraborty Sayan, Feng Zhang, Lee Sangyun, Alvarenga Omar E, Panda Aniruddha, Bruni Renato, Khelashvili George, Gupta Kallol, Accardi Alessio

机构信息

Department of Anesthesiology, Weill Cornell Medical College.

Physiology, Biophysics and Systems Biology Graduate Program, Weill Cornell Medical College.

出版信息

bioRxiv. 2024 Aug 9:2024.08.07.607004. doi: 10.1101/2024.08.07.607004.

Abstract

Phosphatidylserine externalization on the surface of dying cells is a key signal for their recognition and clearance by macrophages and is mediated by members of the X-Kell related (Xkr) protein family. Defective Xkr-mediated scrambling impairs clearance, leading to inflammation. It was proposed that activation of the Xkr4 apoptotic scramblase requires caspase cleavage, followed by dimerization and ligand binding. Here, using a combination of biochemical approaches we show that purified monomeric, full-length human Xkr4 (hXkr4) scrambles lipids. CryoEM imaging shows that hXkr4 adopts a novel conformation, where three conserved acidic residues create an electronegative surface embedded in the membrane. Molecular dynamics simulations show this conformation induces membrane thinning, which could promote scrambling. Thinning is ablated or reduced in conditions where scrambling is abolished or reduced. Our work provides insights into the molecular mechanisms of hXkr4 scrambling and suggests the ability to thin membranes might be a general property of active scramblases.

摘要

磷脂酰丝氨酸在垂死细胞表面的外化是巨噬细胞识别和清除这些细胞的关键信号,且由X-Kell相关(Xkr)蛋白家族成员介导。Xkr介导的磷脂翻转缺陷会损害清除过程,导致炎症。有人提出,Xkr4凋亡性磷脂翻转酶的激活需要半胱天冬酶切割,随后发生二聚化和配体结合。在这里,我们结合多种生化方法表明,纯化的单体全长人Xkr4(hXkr4)能使脂质发生翻转。冷冻电镜成像显示,hXkr4呈现出一种新的构象,其中三个保守的酸性残基形成了一个嵌入膜内的带负电表面。分子动力学模拟表明,这种构象会导致膜变薄,这可能会促进磷脂翻转。在磷脂翻转被消除或减少的情况下,膜变薄现象会被消除或减轻。我们的工作为hXkr4介导的磷脂翻转分子机制提供了见解,并表明使膜变薄的能力可能是活性磷脂翻转酶的一个普遍特性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/34f2/11326236/96174e8476fb/nihpp-2024.08.07.607004v1-f0001.jpg

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