iScience. 2024 Aug 16. 27(8): 110560
Kristýna Čunátová,
Marek Vrbacký,
Guillermo Puertas-Frias,
Lukáš Alán,
Marie Vanišová,
María José Saucedo-Rodríguez,
Josef Houštěk,
Erika Fernández-Vizarra,
Jiří Neužil,
Alena Pecinová,
Petr Pecina,
Tomáš Mráček.
Individual complexes of the mitochondrial oxidative phosphorylation system (OXPHOS) are not linked solely by their function; they also share dependencies at the maintenance/assembly level, where one complex depends on the presence of a different individual complex. Despite the relevance of this "interdependence" behavior for mitochondrial diseases, its true nature remains elusive. To understand the mechanism that can explain this phenomenon, we examined the consequences of the aberration of different OXPHOS complexes in human cells. We demonstrate here that the complete disruption of each of the OXPHOS complexes resulted in a decrease in the complex I (cI) level and that the major reason for this is linked to the downregulation of mitochondrial ribosomal proteins. We conclude that the secondary cI defect is due to mitochondrial protein synthesis attenuation, while the responsible signaling pathways could differ based on the origin of the OXPHOS defect.
Keywords: Biochemistry; Cell biology; Molecular biology