mtUPR Modulation as a Therapeutic Target for Primary and Secondary Mitochondrial Diseases

Author:

Cilleros-Holgado Paula,Gómez-Fernández David,Piñero-Pérez Rocío,Reche-López Diana,Álvarez-Córdoba Mónica,Munuera-Cabeza Manuel,Talaverón-Rey Marta,Povea-Cabello Suleva,Suárez-Carrillo Alejandra,Romero-González Ana,Suárez-Rivero Juan Miguel,Romero-Domínguez Jose Manuel,Sánchez-Alcázar Jose AntonioORCID

Abstract

Mitochondrial dysfunction is a key pathological event in many diseases. Its role in energy production, calcium homeostasis, apoptosis regulation, and reactive oxygen species (ROS) balance render mitochondria essential for cell survival and fitness. However, there are no effective treatments for most primary and secondary mitochondrial diseases to this day. Therefore, new therapeutic approaches, such as the modulation of the mitochondrial unfolded protein response (mtUPR), are being explored. mtUPRs englobe several compensatory processes related to proteostasis and antioxidant system mechanisms. mtUPR activation, through an overcompensation for mild intracellular stress, promotes cell homeostasis and improves lifespan and disease alterations in biological models of mitochondrial dysfunction in age-related diseases, cardiopathies, metabolic disorders, and primary mitochondrial diseases. Although mtUPR activation is a promising therapeutic option for many pathological conditions, its activation could promote tumor progression in cancer patients, and its overactivation could lead to non-desired side effects, such as the increased heteroplasmy of mitochondrial DNA mutations. In this review, we present the most recent data about mtUPR modulation as a therapeutic approach, its role in diseases, and its potential negative consequences in specific pathological situations.

Publisher

MDPI AG

Subject

Inorganic Chemistry,Organic Chemistry,Physical and Theoretical Chemistry,Computer Science Applications,Spectroscopy,Molecular Biology,General Medicine,Catalysis

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