Secondary coenzyme Q10 deficiencies in oxidative phosphorylation (OXPHOS) and non-OXPHOS disorders.

Yubero,; Montero, R; Martín, Ma; Montoya, J; Ribes, A; Grazina, M; Trevisson, Eva; Rodriguez Aguilera JC,; Hargreaves, Ip; Salviati, Leonardo; Navas, P; Artuch, R; CoQ deficiency study group,; Jou, C; Jimenez Mallebrera, C; Nascimento, A; Pérez Dueñas, B; Ortez C, Ramos F; Colomer, J; O'Callaghan, M; Pineda, M; García Cazorla, A; Espinós, C; Ruiz, A; Macaya, A; Marcé Grau, A; Garcia Villoria, J; Arias, A; Emperador, S; Ruiz Pesini, E; Lopez Gallardo, E; Neergheen, V; Simões, M; Diogo, L; Blázquez, A; González Quintana, A; Delmiro, A; Domínguez González, C; Arenas, J; García Silva MT,; Martín, E; Quijada, P; Hernández Laín, A; Morán, M; Rivas Infante, E; Ávila Polo, R; Paradas Lópe, C; Bautista Lorite, J; Martínez Fernández EM,; Cortés, Ab; Sánchez Cuesta, A; Cascajo, Mv; Alcázar, M; Brea Calvo, G.

doi:10.1016/j.mito.2016.06.007.

We evaluated the coenzyme Q₁₀ (CoQ) levels in patients who were diagnosed with mitochondrial oxidative phosphorylation (OXPHOS) and non-OXPHOS disorders (n=72). Data from the 72 cases in this study revealed that 44.4% of patients showed low CoQ concentrations in either their skeletal muscle or skin fibroblasts. Our findings suggest that secondary CoQ deficiency is a common finding in OXPHOS and non-OXPHOS disorders. We hypothesize that cases of CoQ deficiency associated with OXPHOS defects could be an adaptive mechanism to maintain a balanced OXPHOS, although the mechanisms explaining these deficiencies and the pathophysiological role of secondary CoQ deficiency deserves further investigation.