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The ER Thioredoxin-Related Transmembrane Protein TMX2 Controls Redox-Mediated Tethering of ER-Mitochondria Contacts (ERMCS)
by
Bassot, Arthur
, Buzatto, Adriana Zardini
, Morgan, Bruce
, Makio, Tadashi
, Mast, Heather
, Ballanyi, Klaus
, Chen, Junsheng
, Fleury, Samuel G.
, Lemieux, Hélène
, Li, Liang
, Mancini, Grazia M.S.
, Bhat, Rakesh
, Fan, Yuxiang
, Moore, Jack
, Lemieux, M. Joanne
, Tan, Wen-Hann
, Zimmermann, Jannik
, Overduin, Michael
, Marcogliese, Paul C.
, Pascual, Danielle M.
, Simmen, Thomas
, Yap, Megan C.
in
Cell Biology
2024
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The ER Thioredoxin-Related Transmembrane Protein TMX2 Controls Redox-Mediated Tethering of ER-Mitochondria Contacts (ERMCS)
by
Bassot, Arthur
, Buzatto, Adriana Zardini
, Morgan, Bruce
, Makio, Tadashi
, Mast, Heather
, Ballanyi, Klaus
, Chen, Junsheng
, Fleury, Samuel G.
, Lemieux, Hélène
, Li, Liang
, Mancini, Grazia M.S.
, Bhat, Rakesh
, Fan, Yuxiang
, Moore, Jack
, Lemieux, M. Joanne
, Tan, Wen-Hann
, Zimmermann, Jannik
, Overduin, Michael
, Marcogliese, Paul C.
, Pascual, Danielle M.
, Simmen, Thomas
, Yap, Megan C.
in
Cell Biology
2024
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The ER Thioredoxin-Related Transmembrane Protein TMX2 Controls Redox-Mediated Tethering of ER-Mitochondria Contacts (ERMCS)
by
Bassot, Arthur
, Buzatto, Adriana Zardini
, Morgan, Bruce
, Makio, Tadashi
, Mast, Heather
, Ballanyi, Klaus
, Chen, Junsheng
, Fleury, Samuel G.
, Lemieux, Hélène
, Li, Liang
, Mancini, Grazia M.S.
, Bhat, Rakesh
, Fan, Yuxiang
, Moore, Jack
, Lemieux, M. Joanne
, Tan, Wen-Hann
, Zimmermann, Jannik
, Overduin, Michael
, Marcogliese, Paul C.
, Pascual, Danielle M.
, Simmen, Thomas
, Yap, Megan C.
in
Cell Biology
2024
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The ER Thioredoxin-Related Transmembrane Protein TMX2 Controls Redox-Mediated Tethering of ER-Mitochondria Contacts (ERMCS)
Paper
The ER Thioredoxin-Related Transmembrane Protein TMX2 Controls Redox-Mediated Tethering of ER-Mitochondria Contacts (ERMCS)
2024
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Overview
Thioredoxin-related transmembrane proteins (TMX) of the endoplasmic reticulum (ER) have emerged as key regulators of ER membrane properties. Within the ER lumen, TMX proteins and other ER redox enzymes determine oxidative conditions, which control the formation of ER-mitochondria membrane contacts (ERMCS) and determine their function. ERMCS exhibit cytoplasmic redox nanodomains, derived from ER and mitochondrial reactive oxygen species (ROS), whose mechanistic regulation is uncharacterized. Our research has identified the ER protein TMX2, which uses its unique cytosolic thioredoxin domain to prevent cytosolic sulfenylation of mitochondrial outer membrane proteins such as TOM70 through a functional interaction with peroxiredoxin-1 (PRDX1). By doing so, TMX2 interferes with the TOM70 ERMCS tethering function and reduces mitochondrial Ca2+ flux and metabolism. Recently, TMX2 mutations have been identified to cause a neurodevelopmental disorder with microcephaly, cortical malformations, and spasticity (NEDMCMS). Using TMX2-mutated NEDMCMS patient cells, we demonstrate that compromising TMX2 through mutation reproduces mitochondrial defects. In a fly in vivo model, TMX2 knockdown manifests predominantly in glial cells. Our results therefore provide important mechanistic insight into NEDMCMS and mechanistically link TMX2-mediated control of ERMCS to brain development and function.
The transmembrane thioredoxin-related TMX2 prevents TOM70 sulfenylation at ERMCS, thus maintaining normal mitochondria metabolism in wild-type cells. TMX2 knockout leads to TOM70 sulfenylation and tight ERMCS formation. This then increases ROS production, unbalances mitochondrial lipids, and relatively shifts OXPHOS electron supply to complex II.
Publisher
Cold Spring Harbor Laboratory
Subject
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