info:eu-repo/semantics/article
Alpha-synuclein mitochondrial interaction leads to irreversible translocation and complex I impairment
Fecha
2018-08Registro en:
Martinez, Jimena Hebe; Fuentes, Federico; Vanasco, Virginia; Alvarez, Silvia; Alaimo, Agustina; et al.; Alpha-synuclein mitochondrial interaction leads to irreversible translocation and complex I impairment; Elsevier Science Inc; Archives of Biochemistry and Biophysics; 651; 8-2018; 1-12
0003-9861
CONICET Digital
CONICET
Autor
Martinez, Jimena Hebe
Fuentes, Federico
Vanasco, Virginia
Alvarez, Silvia
Alaimo, Agustina
Cassina, Adriana
Coluccio Leskow, Federico
Velázquez Duarte, Francisco
Resumen
α-synuclein is involved in both familial and sporadic Parkinson's disease. Although its interaction with mitochondria has been well documented, several aspects remains unknown or under debate such as the specific sub-mitochondrial localization or the dynamics of the interaction. It has been suggested that α-synuclein could only interact with ER-associated mitochondria. The vast use of model systems and experimental conditions makes difficult to compare results and extract definitive conclusions. Here we tackle this by analyzing, in a simplified system, the interaction between purified α-synuclein and isolated rat brain mitochondria. This work shows that wild type α-synuclein interacts with isolated mitochondria and translocates into the mitochondrial matrix. This interaction and the irreversibility of α-synuclein translocation depend on incubation time and α-synuclein concentration. FRET experiments show that α-synuclein localizes close to components of the TOM complex suggesting a passive transport of α-synuclein through the outer membrane. In addition, α-synuclein binding alters mitochondrial function at the level of Complex I leading to a decrease in ATP synthesis and an increase of ROS production.