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与PI(4)P代谢偶联的ORP介导的脂质交换过程的重构。

Reconstitution of ORP-mediated lipid exchange process coupled to PI(4)P metabolism.

作者信息

Fuggetta Nicolas, Rigolli Nicola, Magdeleine Maud, Seminara Agnese, Drin Guillaume

机构信息

Université Côte d'Azur, Centre National de la Recherche Scientifique, Institut de Pharmacologie Moléculaire et Cellulaire, 660 route des lucioles, 06560 Valbonne, France.

Laboratoire de Physique, École Normale Supérieure (LPENS), 75005 Paris, France.

出版信息

bioRxiv. 2023 Aug 4:2023.08.04.551917. doi: 10.1101/2023.08.04.551917.

Abstract

Lipid distribution in the eukaryotic cells depends on tight couplings between lipid transfer and lipid metabolism. Yet these couplings remain poorly described. Notably, it is unclear to what extent lipid exchangers of the OSBP-related proteins (ORPs) family, coupled to PI(4)P metabolism, contribute to the formation of sterol and phosphatidylserine gradient between the endoplasmic reticulum (ER) and other cell regions. To address this question, we have examined the activity of Osh4p, a representative ORP, between Golgi mimetic membranes in which PI(4)P is produced by a PI 4-kinase and ER mimetic membranes in which PI(4)P is hydrolyzed by the phosphatase Sac1p. Using quantitative, real-time assays, we demonstrate that Osh4p creates a sterol gradient between the two membranes by sterol/PI(4)P exchange as soon as a PI(4)P gradient is generated at this interface following ATP addition, and define how much PI(4)P must be synthesized for this process. Then, using a kinetic model supported by our data, we estimate to what extent PI(4)P metabolism can drive lipid transfer in cells. Finally, we show that Sec14p, by transferring phosphatidylinositol between membranes, can support the synthesis of PI(4)P and the creation of a sterol gradient by Osh4p. These results indicate to what extent ORPs, under the control of PI(4)P metabolism, can distribute lipids in the cell.

摘要

真核细胞中的脂质分布取决于脂质转运与脂质代谢之间的紧密耦合。然而,这些耦合作用仍未得到充分描述。值得注意的是,尚不清楚与PI(4)P代谢相关的OSBP相关蛋白(ORPs)家族的脂质交换体在多大程度上有助于在内质网(ER)和其他细胞区域之间形成固醇和磷脂酰丝氨酸梯度。为了解决这个问题,我们检测了Osh4p(一种代表性的ORP)在由PI 4-激酶产生PI(4)P的高尔基体模拟膜和由磷酸酶Sac1p水解PI(4)P的内质网模拟膜之间的活性。通过定量实时分析,我们证明一旦在添加ATP后该界面处产生PI(4)P梯度,Osh4p就会通过固醇/PI(4)P交换在两个膜之间形成固醇梯度,并确定该过程必须合成多少PI(4)P。然后,使用由我们的数据支持的动力学模型,我们估计PI(4)P代谢在多大程度上可以驱动细胞中的脂质转运。最后,我们表明Sec14p通过在膜之间转移磷脂酰肌醇,可以支持PI(4)P的合成以及Osh4p形成固醇梯度。这些结果表明在PI(4)P代谢的控制下,ORPs在多大程度上可以在细胞中分布脂质。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5453/10418177/b1bd6e93075e/nihpp-2023.08.04.551917v1-f0001.jpg

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