Abstract

Calcium ions (Ca2+) play critical roles in neuronal processes, such as signaling pathway activation, transcriptional regulation, and synaptic transmission initiation. Therefore, the regulation of Ca2+ homeostasis is one of the most important processes underlying the basic cellular viability and function of the neuron. Multiple components, including intracellular organelles and plasma membrane Ca2+-ATPase, are involved in neuronal Ca2+ control, and recent studies have focused on investigating the roles of mitochondria in synaptic function. Numerous mitochondrial Ca2+ regulatory proteins have been identified in the past decade, with studies demonstrating the tissue- or cell-type-specific function of each component. The mitochondrial calcium uniporter and its binding subunits are major inner mitochondrial membrane proteins contributing to mitochondrial Ca2+ uptake, whereas the mitochondrial Na+/Ca2+ exchanger (NCLX) and mitochondrial permeability transition pore (mPTP) are well-studied proteins involved in Ca2+ extrusion. The level of cytosolic Ca2+ and the resulting characteristics of synaptic vesicle release properties are controlled via mitochondrial Ca2+ uptake and release at presynaptic sites, while in dendrites, mitochondrial Ca2+ regulation affects synaptic plasticity. During brain aging and the progress of neurodegenerative disease, mitochondrial Ca2+ mishandling has been observed using various techniques, including live imaging of Ca2+ dynamics. Furthermore, Ca2+ dysregulation not only disrupts synaptic transmission but also causes neuronal cell death. Therefore, understanding the detailed pathophysiological mechanisms affecting the recently discovered mitochondrial Ca2+ regulatory machineries will help to identify novel therapeutic targets. Here, we discuss current research into mitochondrial Ca2+ regulatory machineries and how mitochondrial Ca2+ dysregulation contributes to brain aging and neurodegenerative disease.

Highlights

  • Mitochondria affect cellular functions via their roles in ATP production, lipid synthesis, reactive oxygen species (ROS) generation, and Ca2+ regulation

  • Recent studies of mitochondria-dependent Ca2+ handling have revealed the molecular identities of Ca2+-control components, including the mitochondrial calcium uniporter (MCU) and its auxiliary subunits (Mammucari et al, 2017)

  • In aged animals and humans, mitochondrial functional impairment is a key hallmark of brain aging (Grimm and Eckert, 2017; Mattson and Arumugam, 2018; Muller et al, 2018)

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Summary

Introduction

Mitochondria affect cellular functions via their roles in ATP production, lipid synthesis, reactive oxygen species (ROS) generation, and Ca2+ regulation. Recent studies of mitochondria-dependent Ca2+ handling have revealed the molecular identities of Ca2+-control components, including the mitochondrial calcium uniporter (MCU) and its auxiliary subunits (Mammucari et al, 2017).

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