Cell Reports (Nov 2017)
ROS Control Mitochondrial Motility through p38 and the Motor Adaptor Miro/Trak
Abstract
Summary: Mitochondrial distribution and motility are recognized as central to many cellular functions, but their regulation by signaling mechanisms remains to be elucidated. Here, we report that reactive oxygen species (ROS), either derived from an extracellular source or intracellularly generated, control mitochondrial distribution and function by dose-dependently, specifically, and reversibly decreasing mitochondrial motility in both rat hippocampal primary cultured neurons and cell lines. ROS decrease motility independently of cytoplasmic [Ca2+], mitochondrial membrane potential, or permeability transition pore opening, known effectors of oxidative stress. However, multiple lines of genetic and pharmacological evidence support that a ROS-activated mitogen-activated protein kinase (MAPK), p38α, is required for the motility inhibition. Furthermore, anchoring mitochondria directly to kinesins without involvement of the physiological adaptors between the organelles and the motor protein prevents the H2O2-induced decrease in mitochondrial motility. Thus, ROS engage p38α and the motor adaptor complex to exert changes in mitochondrial motility, which likely has both physiological and pathophysiological relevance. : Debattisti et al. examine how reactive oxygen species induce dose-dependent and reversible arrest of mitochondrial motility independently of [Ca2+]c in two different mammalian models. The authors argue that ROS target the adaptor complex through p38α to decrease mitochondrial movements. Keywords: reactive oxygen species, mitochondria, movement, calcium, permeability transition, p38, Miro, TRAK
