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结构上无关的脂质转运蛋白的构象可塑性与其作用模式相关。

The conformational plasticity of structurally unrelated lipid transport proteins correlates with their mode of action.

机构信息

Department of Biology, University of Fribourg, Fribourg, Switzerland.

Departamento de Química Física y Analítica, Universidad de Oviedo, Oviedo, Spain.

出版信息

PLoS Biol. 2024 Aug 19;22(8):e3002737. doi: 10.1371/journal.pbio.3002737. eCollection 2024 Aug.

Abstract

Lipid transfer proteins (LTPs) are key players in cellular homeostasis and regulation, as they coordinate the exchange of lipids between different cellular organelles. Despite their importance, our mechanistic understanding of how LTPs function at the molecular level is still in its infancy, mostly due to the large number of existing LTPs and to the low degree of conservation at the sequence and structural level. In this work, we use molecular simulations to characterize a representative dataset of lipid transport domains (LTDs) of 12 LTPs that belong to 8 distinct families. We find that despite no sequence homology nor structural conservation, the conformational landscape of LTDs displays common features, characterized by the presence of at least 2 main conformations whose populations are modulated by the presence of the bound lipid. These conformational properties correlate with their mechanistic mode of action, allowing for the interpretation and design of experimental strategies to further dissect their mechanism. Our findings indicate the existence of a conserved, fold-independent mechanism of lipid transfer across LTPs of various families and offer a general framework for understanding their functional mechanism.

摘要

脂质转运蛋白 (LTPs) 是细胞内稳态和调节的关键参与者,因为它们协调脂质在不同细胞器之间的交换。尽管它们很重要,但我们对 LTPs 在分子水平上如何发挥作用的机制理解仍处于起步阶段,主要是由于存在大量的 LTPs 以及在序列和结构水平上的低度保守性。在这项工作中,我们使用分子模拟来表征属于 8 个不同家族的 12 种 LTP 的代表性脂质转运结构域 (LTD) 数据集。我们发现,尽管没有序列同源性或结构保守性,但 LTD 的构象景观显示出共同的特征,其特征是存在至少 2 种主要构象,其种群受结合脂质的存在而调节。这些构象特性与其作用机制的力学模式相关,允许对实验策略进行解释和设计,以进一步剖析其机制。我们的研究结果表明,存在一种保守的、不依赖折叠的脂质跨各种家族 LTP 的转移机制,并为理解其功能机制提供了一个通用框架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bbe6/11361750/be1adf2b2f7c/pbio.3002737.g001.jpg

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