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Mitochondrial microproteins: critical regulators of protein import, energy production, stress response pathways, and programmed cell death

Journal

AMERICAN JOURNAL OF PHYSIOLOGY-CELL PHYSIOLOGY
Volume 325, Issue 4, Pages C807-C816

Publisher

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/ajpcell.00189.2023

Keywords

cell stress; microproteins; mitochondria; mitochondrial protein import; oxidative phosphorylation

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Mitochondrial microproteins play important roles in maintaining mitochondrial function and regulating cellular stress responses. Despite being a relatively new field, recent studies suggest that there are still many unknown functions of microproteins in the mitochondrial microproteome that require further investigation.
Mitochondria rely upon the coordination of protein import, protein translation, and proper functioning of oxidative phosphorylation (OXPHOS) complexes I-V to sustain the activities of life for an organism. Each process is dependent upon the function of profoundly large protein complexes found in the mitochondria [translocase of the outer mitochondrial membrane (TOMM) complex, translocase of the inner mitochondrial membrane (TIMM) complex, OXPHOS complexes, mitoribosomes]. These massive protein complexes, in some instances more than one megadalton, are built up from numerous protein subunits of varying sizes, including many proteins that are <= 100-150 amino acids. However, these small proteins, termed microproteins, not only act as cogs in large molecular machines but also have important steps in inhibiting or promoting the intrinsic pathway of apoptosis, coordinate responses to cellular stress, and even act as hormones. This review focuses on microproteins that occupy the mitochondria and are critical for its function. Although the microprotein field is relatively new, researchers have long recognized the existence of these mitochondrial proteins as critical components of virtually all aspects of mitochondrial biology. Thus, recent studies estimating that hundreds of new microproteins of unknown function exist and are missing from current genome annotations suggests that the mitochondrial microproteome is a rich area for future biological investigation.

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