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依赖Pex30的膜接触位点维持内质网脂质稳态。

Pex30-dependent membrane contact sites maintain ER lipid homeostasis.

作者信息

Ferreira Joana Veríssimo, Ahmed Yara, Heunis Tiaan, Jain Aamna, Johnson Errin, Räschle Markus, Ernst Robert, Vanni Stefano, Carvalho Pedro

机构信息

Sir William Dunn School of Pathology, University of Oxford , Oxford, UK.

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

出版信息

J Cell Biol. 2025 Jul 7;224(7). doi: 10.1083/jcb.202409039. Epub 2025 May 23.

Abstract

In eukaryotic cells, communication between organelles and the coordination of their activities depend on membrane contact sites (MCS). How MCS are regulated under the dynamic cellular environment remains poorly understood. Here, we investigate how Pex30, a membrane protein localized to the endoplasmic reticulum (ER), regulates multiple MCS in budding yeast. We show that Pex30 is critical for the integrity of ER MCS with peroxisomes and vacuoles. This requires the dysferlin (DysF) domain on the Pex30 cytosolic tail. This domain binds to phosphatidic acid (PA) both in vitro and in silico, and it is important for normal PA metabolism in vivo. The DysF domain is evolutionarily conserved and may play a general role in PA homeostasis across eukaryotes. We further show that the ER-vacuole MCS requires a Pex30 C-terminal domain of unknown function and that its activity is controlled by phosphorylation in response to metabolic cues. These findings provide new insights into the dynamic nature of MCS and their coordination with cellular metabolism.

摘要

在真核细胞中,细胞器之间的通讯及其活动的协调依赖于膜接触位点(MCS)。在动态细胞环境下,MCS 是如何被调控的仍知之甚少。在此,我们研究了定位在内质网(ER)的膜蛋白 Pex30 如何调控出芽酵母中的多个 MCS。我们发现 Pex30 对于 ER 与过氧化物酶体和液泡的 MCS 的完整性至关重要。这需要 Pex30 胞质尾部的dysferlin(DysF)结构域。该结构域在体外和计算机模拟中均能结合磷脂酸(PA),并且对体内正常的 PA 代谢很重要。DysF 结构域在进化上是保守的,可能在真核生物的 PA 稳态中发挥普遍作用。我们进一步表明,ER - 液泡 MCS 需要一个功能未知的 Pex30 C 末端结构域,并且其活性受代谢信号响应的磷酸化作用控制。这些发现为 MCS 的动态性质及其与细胞代谢的协调提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9fbe/12232902/24b5cce3a63f/jcb_202409039_fig1.jpg

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