LGG-1/GABARAP lipidation is not required for autophagy and development in Caenorhabditis elegans

The ubiquitin-like proteins Atg8/LC3/GABARAP are required for multiple steps of autophagy, such as initiation, cargo recognition and engulfment, vesicle closure and degradation. Most of LC3/GABARAP functions are considered dependent on their post-translational modifications and their association wit...

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Veröffentlicht in:eLife 2023-07, Vol.12
Hauptverfasser: Leboutet, Romane, Largeau, Céline, Müller, Leonie, Prigent, Magali, Quinet, Grégoire, Rodriguez, Manuel S, Cuif, Marie-Hélène, Hoppe, Thorsten, Culetto, Emmanuel, Lefebvre, Christophe, Legouis, Renaud
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Sprache:eng
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Zusammenfassung:The ubiquitin-like proteins Atg8/LC3/GABARAP are required for multiple steps of autophagy, such as initiation, cargo recognition and engulfment, vesicle closure and degradation. Most of LC3/GABARAP functions are considered dependent on their post-translational modifications and their association with the autophagosome membrane through a conjugation to a lipid, the phosphatidyl-ethanolamine. Contrarily to mammals, possesses single homologs of LC3 and GABARAP families, named LGG-2 and LGG-1. Using site-directed mutagenesis, we inhibited the conjugation of LGG-1 to the autophagosome membrane and generated mutants that express only cytosolic forms, either the precursor or the cleaved protein. LGG-1 is an essential gene for autophagy and development in , but we discovered that its functions could be fully achieved independently of its localization to the membrane. This study reveals an essential role for the cleaved form of LGG-1 in autophagy but also in an autophagy-independent embryonic function. Our data question the use of lipidated GABARAP/LC3 as the main marker of autophagic flux and highlight the high plasticity of autophagy.
ISSN:2050-084X
2050-084X
DOI:10.7554/eLife.85748