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An essential role for the ATG8 ortholog LC3C in antibacterial autophagy
Authors:Natalia von Muhlinen  Masato Akutsu  Benjamin J. Ravenhill   ágnes Foeglein  Stuart Bloor  Trevor J. Rutherford  Stefan M.V. Freund  David Komander  Felix Randow
Affiliation:MRC Laboratory of Molecular Biology; Division of Protein and Nucleic Acid Chemistry; Cambridge UK
Abstract:Autophagy defends the mammalian cytosol against bacterial invasion. Efficient bacterial engulfment by autophagy requires cargo receptors that bind (a) homolog(s) of the ubiquitin-like protein Atg8 on the phagophore membrane. The existence of multiple ATG8 orthologs in higher eukaryotes suggests that they may perform distinct functions. However, no specific role has been assigned to any mammalian ATG8 ortholog. We recently discovered that the autophagy receptor CALCOCO2/NDP52, which detects cytosol-invading Salmonella enterica serovar Typhimurium (S. Typhimurium), preferentially binds LC3C. The CALCOCO2/NDP52-LC3C interaction is essential for cell-autonomous immunity against cytosol-exposed S. Typhimurium, because cells lacking either protein fail to target bacteria into the autophagy pathway. The selectivity of CALCOCO2/NDP52 for LC3C is determined by a novel LC3C interacting region (CLIR), in which the lack of the key aromatic residue of canonical LIRs is compensated by LC3C-specific interactions. Our findings provide a new layer of regulation to selective autophagy, suggesting that specific interactions between autophagy receptors and the ATG8 orthologs are of biological importance.
Keywords:autophagy  Salmonella  ATG8/LC3  LC3C  NDP52  LIR
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