Resurrecting Golgi proteins to grasp Golgi ribbon formation and self-association under stress

高尔基体 生物 细胞生物学 基因复制 细胞器 分泌途径 抓住 复印件 复印机 基因 遗传学 内质网 计算机科学 程序设计语言
作者
Luís F.S. Mendes,Mariana Batista,Emanuel Kava,Lucas Bleicher,Mariana C. Micheletto,Antonio J. Costa‐Filho
出处
期刊:International Journal of Biological Macromolecules [Elsevier BV]
卷期号:194: 264-275 被引量:6
标识
DOI:10.1016/j.ijbiomac.2021.11.173
摘要

The Golgi complex is an essential organelle of the eukaryotic exocytic pathway. A subfamily of Golgi matrix proteins, called GRASPs, is central in stress-induced unconventional secretion, Golgi dynamics during mitosis/apoptosis, and Golgi ribbon formation. The Golgi ribbon is vertebrate-specific and correlates with the appearance of two GRASP paralogues and two Golgins (GM130/Golgin45), which form specific GRASP-Golgin pairs. The molecular details of their appearance only in Metazoans are unknown. Moreover, despite new functionalities supported by GRASP paralogy, little is known about their structural and evolutionary differences. Here, we used ancestor sequence reconstruction and biophysical/biochemical approaches to assess the evolution of GRASPs structure/dynamics, fibrillation, and how they started anchoring their Golgin partners. Our data showed that a GRASP ancestor anchored Golgins before gorasp gene duplication in Metazoans. After gene duplication, variations within the GRASP binding pocket determined which paralogue would recruit which Golgin. These interactions are responsible for their specific Golgi location and Golgi ribbon appearance. We also suggest that GRASPs have a long-standing capacity to form supramolecular structures, affecting their participation in stress-induced processes.
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