Temporal control of contact site formation reveals a relationship between mitochondrial division and Num1-mediated mitochondrial tethering.
Mitochondrial division is critical for maintenance of mitochondrial morphology and cellular homeostasis. Previous studies have suggested that the mitochondria-ER-cortex anchor (MECA), a tripartite membrane contact site between mitochondria, the ER, and the plasma membrane, is involved in mitochondrial division. However, its role is poorly understood. We developed a system to ... control MECA formation and depletion, which allowed us to investigate the relationship between MECA-mediated contact sites and mitochondrial division. Num1 is the protein that mediates mitochondria-ER-plasma membrane tethering at MECA sites. Using both rapamycin-inducible dimerization and auxin-inducible degradation components coupled with Num1, we developed systems to temporally control the formation and depletion of the native contact site. Additionally, we designed a regulatable Num1-independant mitochondria-PM tether. We found that mitochondria-PM tethering alone is not sufficient to rescue mitochondrial division and that a specific feature of Num1-mediated tethering is required. This study demonstrates the utility of systems that regulate contact-site formation and depletion in studying the biological functions of membrane contact sites.
Mesh Terms:
Cell Membrane, Mitochondria, Mitochondrial Membranes, Mitochondrial Proteins, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins
Cell Membrane, Mitochondria, Mitochondrial Membranes, Mitochondrial Proteins, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins
Mol Biol Cell
Date: Oct. 01, 2023
PubMed ID: 37585290
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