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DYRK3通过维持内质网出口位点的类液态状态来实现分泌运输。

DYRK3 enables secretory trafficking by maintaining the liquid-like state of ER exit sites.

作者信息

Gallo Raffaella, Rai Arpan Kumar, McIntyre Alexa B R, Meyer Katrina, Pelkmans Lucas

机构信息

Department of Molecular Life Sciences, University of Zurich, 8046 Zurich, Switzerland.

Department of Molecular Life Sciences, University of Zurich, 8046 Zurich, Switzerland.

出版信息

Dev Cell. 2023 Oct 9;58(19):1880-1897.e11. doi: 10.1016/j.devcel.2023.08.005. Epub 2023 Aug 28.

Abstract

The dual-specificity kinase DYRK3 controls the formation and dissolution of multiple biomolecular condensates, regulating processes including stress recovery and mitotic progression. Here, we report that DYRK3 functionally interacts with proteins associated with endoplasmic reticulum (ER) exit sites (ERESs) and that inhibition of DYRK3 perturbs the organization of the ERES-Golgi interface and secretory trafficking. DYRK3-mediated regulation of ERES depends on the N-terminal intrinsically disordered region (IDR) of the peripheral membrane protein SEC16A, which co-phase separates with ERES components to form liquid-like condensates on the surface of the ER. By modulating the liquid-like properties of ERES, we show that their physical state is essential for functional cargo trafficking through the early secretory pathway. Our findings support a mechanism whereby phosphorylation by DYRK3 and its reversal by serine-threonine phosphatases regulate the material properties of ERES to create a favorable physicochemical environment for directional membrane traffic in eukaryotic cells.

摘要

双特异性激酶DYRK3控制多种生物分子凝聚物的形成和解聚,调节包括应激恢复和有丝分裂进程等过程。在此,我们报道DYRK3与内质网(ER)出口位点(ERESs)相关蛋白发生功能相互作用,并且抑制DYRK3会扰乱ERES - 高尔基体界面的组织以及分泌运输。DYRK3介导的ERES调节依赖于外周膜蛋白SEC16A的N端内在无序区域(IDR),该区域与ERES成分共相分离,在内质网表面形成类似液体的凝聚物。通过调节ERES的类似液体的特性,我们表明它们的物理状态对于通过早期分泌途径的功能性货物运输至关重要。我们的研究结果支持一种机制,即DYRK3的磷酸化及其被丝氨酸 - 苏氨酸磷酸酶的逆转调节ERES的物质特性,为真核细胞中的定向膜运输创造有利的物理化学环境。

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