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内质网应激传感器蛋白和内质网-线粒体串扰信号转导超越(内质网)应激反应。

ER Stress-Sensor Proteins and ER-Mitochondrial Crosstalk-Signaling Beyond (ER) Stress Response.

机构信息

Department of Biological Sciences, Birla Institute of Technology and Science (BITS)-Pilani (Hyderabad Campus), Shameerpet-Mandal, Hyderabad, Telangana 500078, India.

出版信息

Biomolecules. 2021 Jan 28;11(2):173. doi: 10.3390/biom11020173.

Abstract

Recent studies undoubtedly show the importance of inter organellar connections to maintain cellular homeostasis. In normal physiological conditions or in the presence of cellular and environmental stress, each organelle responds alone or in coordination to maintain cellular function. The Endoplasmic reticulum (ER) and mitochondria are two important organelles with very specialized structural and functional properties. These two organelles are physically connected through very specialized proteins in the region called the mitochondria-associated ER membrane (MAM). The molecular foundation of this relationship is complex and involves not only ion homeostasis through the shuttling of calcium but also many structural and apoptotic proteins. IRE1alpha and PERK are known for their canonical function as an ER stress sensor controlling unfolded protein response during ER stress. The presence of these transmembrane proteins at the MAM indicates its potential involvement in other biological functions beyond ER stress signaling. Many recent studies have now focused on the non-canonical function of these sensors. In this review, we will focus on ER mitochondrial interdependence with special emphasis on the non-canonical role of ER stress sensors beyond ER stress.

摘要

最近的研究无疑表明了细胞器间连接对于维持细胞内稳态的重要性。在正常生理条件下或细胞和环境应激存在的情况下,每个细胞器都会单独或协调响应以维持细胞功能。内质网 (ER) 和线粒体是两个具有非常特殊结构和功能特性的重要细胞器。这两个细胞器通过称为线粒体相关内质网膜 (MAM) 的区域中的非常特殊的蛋白质物理连接。这种关系的分子基础很复杂,不仅涉及通过钙穿梭实现离子稳态,还涉及许多结构和凋亡蛋白。IRE1alpha 和 PERK 以其作为 ER 应激传感器的经典功能而闻名,在 ER 应激期间控制未折叠蛋白反应。这些跨膜蛋白在 MAM 中的存在表明其可能参与 ER 应激信号以外的其他生物学功能。许多最近的研究都集中在这些传感器的非经典功能上。在这篇综述中,我们将重点关注 ER 与线粒体的相互依存关系,特别强调 ER 应激传感器除 ER 应激以外的非经典作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1fb0/7911976/cef0764052b6/biomolecules-11-00173-g001.jpg

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