Mitochondrial DNA: Impacting Central and Peripheral Nervous Systems

Creators: Carelli, Valerio; Chan, David C.

Abstract

Because of their high-energy metabolism, neurons are strictly dependent on mitochondria, which generate cellular ATP through oxidative phosphorylation. The mitochondrial genome encodes for critical components of the oxidative phosphorylation pathway machinery, and therefore, mutations in mitochondrial DNA (mtDNA) cause energy production defects that frequently have severe neurological manifestations. Here, we review the principles of mitochondrial genetics and focus on prototypical mitochondrial diseases to illustrate how primary defects in mtDNA or secondary defects in mtDNA due to nuclear genome mutations can cause prominent neurological and multisystem features. In addition, we discuss the pathophysiological mechanisms underlying mitochondrial diseases, the cellular mechanisms that protect mitochondrial integrity, and the prospects for therapy.

Additional Information

© 2014 Elsevier Inc. Available online 17 December 2014. Work in the authors' laboratories is supported by HHMI (D.C.C.); NIH grants GM062967 (D.C.C.) and GM110039 (D.C.C.); Telethon grants GGP11182 (V.C.) and GPP10005 (V.C); the Emilia-Romagna region program ER-MITO (V.C.); support of Fondazione Galletti (V.C.); and support from the patient's associations MITOCON, UMDF, IFOND, Struggling Within Leber's, and The Poincenot Family (V.C.). We are grateful to Maria Lucia Valentino (University of Bologna), Piero Barboni (Università Vita-Salute San Raffaele), Alfredo A. Sadun (Doheny Eye Institute, UCLA), and Fred Ross-Cisneros (Doheny Eye Institute, UCLA) for providing clinical and histological images used in the figures.

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