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Článek

TMEM70 facilitates biogenesis of mammalian ATP synthase by promoting subunit c incorporation into the rotor structure of the enzyme

Kovalčíkova, Jana
Autor Kovalčíkova, Jana Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic
Vrbacký, Marek
Autor Vrbacký, Marek Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic
Pecina, Petr
Autor Pecina, Petr Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic
Tauchmannová, Kateřina
Autor Tauchmannová, Kateřina Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic
Nůsková, Hana
Autor Nůsková, Hana Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic
Kaplanová, Vilma
Autor Kaplanová, Vilma Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic
Brázdová, Andrea
Autor Brázdová, Andrea Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic
Alán, Lukáš
Autor Alán, Lukáš Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic
Eliáš, Jan
Autor Eliáš, Jan Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic
Čunátová, Kristýna
Autor Čunátová, Kristýna Department of Bioenergetics, Institute of Physiology, Prague, Czech Republic

FASEB journal. 2019 Dec ; 33 (12) : 14103-14117. [epub] 20191025

FASEB J
ISSN 1530-6860 | 0892-6638
Zdroj

Biogenesis of F1Fo ATP synthase, the key enzyme of mitochondrial energy provision, depends on transmembrane protein 70 (TMEM70), localized in the inner mitochondrial membrane of higher eukaryotes. TMEM70 absence causes severe ATP-synthase deficiency and leads to a neonatal mitochondrial encephalocardiomyopathy in humans. However, the exact biochemical function of TMEM70 remains unknown. Using TMEM70 conditional knockout in mice, we show that absence of TMEM70 impairs the early stage of enzyme biogenesis by preventing incorporation of hydrophobic subunit c into rotor structure of the enzyme. This results in the formation of an incomplete, pathologic enzyme complex consisting of F1 domain and peripheral stalk but lacking Fo proton channel composed of subunits c and a. We demonstrated direct interaction between TMEM70 and subunit c and showed that overexpression of subunit c in TMEM70-/- cells partially rescued TMEM70 defect. Accordingly, TMEM70 knockdown prevented subunit c accumulation otherwise observed in F1-deficient cells. Altogether, we identified TMEM70 as specific ancillary factor for subunit c. The biologic role of TMEM70 is to increase the low efficacy of spontaneous assembly of subunit c oligomer, the key and rate-limiting step of ATP-synthase biogenesis, and thus to reach an adequately high physiologic level of ATP synthase in mammalian tissues.-Kovalčíková, J., Vrbacký, M., Pecina, P., Tauchmannová, K., Nůsková, H., Kaplanová, V., Brázdová, A., Alán, L., Eliáš, J., Čunátová, K., Kořínek, V., Sedlacek, R., Mráček, T., Houštěk, J. TMEM70 facilitates biogenesis of mammalian ATP synthase by promoting subunit c incorporation into the rotor structure of the enzyme.

Klíčová slova
ATP5G assembly, ancillary factor, mitochondria, mouse knockout,
MeSH
genotyp MeSH
genový knockout metody MeSH
HEK293 buňky MeSH
kultivované buňky MeSH
lidé MeSH
mitochondriální proteiny genetika metabolismus MeSH
mitochondriální protonové ATPasy genetika metabolismus MeSH
myši knockoutované MeSH
myši MeSH
proteolipidy metabolismus MeSH
regulace genové exprese MeSH
tamoxifen farmakologie MeSH
zvířata MeSH
Check Tag
lidé MeSH
myši MeSH
zvířata MeSH
Publikační typ
časopisecké články MeSH
práce podpořená grantem MeSH
Názvy látek
mitochondriální proteiny MeSH
mitochondriální protonové ATPasy MeSH
proteolipidy MeSH
tamoxifen MeSH

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