Alternative Translation and Retrotranslocation of Cytosolic C3 That Detects Cytoinvasive Bacteria

Overview

Journal Cell Mol Life Sci

Publisher Springer

Specialty Biology

Date 2022 May 13

PMID 35546365

Authors

Mariann Kremlitzka

Lucie Colineau

Alicja A Nowacka

Frida C Mohlin

Katarzyna Wozniak

Anna M Blom

Ben C King

Affiliations

Soon will be listed here.

Abstract

Complement C3 was originally regarded as a serum effector protein, although recent data has emerged suggesting that intracellular C3 can also regulate basic cellular processes. Despite the growing interest in intracellular C3 functions, the mechanism behind its generation has not been demonstrated. In this study we show that C3 can be expressed from an alternative translational start site, resulting in C3 lacking the signal peptide, which is therefore translated in the cytosol. In contrast to the secreted form, alternatively translated cytosolic C3 is not glycosylated, is present mainly in a reduced state, and is turned over by the ubiquitin-proteasome system. C3 can also be retrotranslocated from the endoplasmic reticulum into the cytosol, structurally resembling secreted C3. Finally, we demonstrate that intracellular cytosolic C3 can opsonize invasive Staphylococcus aureus within epithelial cell, slowing vacuolar escape as well as impacting bacterial survival on subsequent exposure to phagocytes. Our work therefore reveals the existence and origin of intracellular, cytosolic C3, and demonstrates functions for cytosolic C3 in intracellular detection of cytoinvasive pathogens.

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