Mitochondria are vital to the functions of eukaryotic cells. Most mitochondrial proteins are transported into the organelle following their synthesis by cytoplasmic ribosomes. However, precise protein targeting is complex because the two diverse lipid membranes encase mitochondria. Efficient protein translocation across membranes and accurate sorting to specific sub-compartments require the cooperation of multiple factors. Any failure in mitochondrial protein import can disrupt organelle fitness. Proteins intended for mitochondria make up a significant portion of all proteins produced in the cytosol. Therefore, import defects causing their mislocalization can significantly stress cellular protein homeostasis. Recognition of this phenomenon has increased interest in molecular mechanisms that respond to import-related stress and restore proteostasis, which is the focus of this review. Significantly, disruptions in protein homeostasis link strongly to the pathology of several degenerative disorders highly relevant in ageing societies. A comprehensive understanding of protein import quality control will allow harnessing this machinery in therapeutic approaches.
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The versatile programmability of CRISPR system has been utilized in various applications for RNA sensing. In this issue Liu and colleagues review how scientists engineer the guide RNAs (gRNAs) in CRISPR systems and create diverse strategies for designing RNA sensors. These approaches can not only detect target RNA molecules in vitro but also enable the regulation of gene expression in response to specific RNA molecules in vivo. Image provided by Yang Liu.
Mechanisms of stress management in mitochondrial protein import
Maryam Mukhtar, Krutika Thakkur, Agnieszka Chacinska, Piotr Bragoszewski; Mechanisms of stress management in mitochondrial protein import. Biochem Soc Trans 20 December 2023; 51 (6): 2117–2126. doi: https://doi.org/10.1042/BST20230377
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