Akt Is S-Palmitoylated: A New Layer of Regulation for Akt

The protein kinase Akt/PKB participates in a great variety of processes, including translation, cell proliferation and survival, as well as malignant transformation and viral infection. In the last few years, novel Akt posttranslational modifications have been found. However, how these modification...

Full description

Saved in:
Bibliographic Details
Published in:Frontiers in cell and developmental biology 2021-02, Vol.9, p.626404-626404
Main Authors: Blaustein, Matías, Piegari, Estefanía, Martínez Calejman, Camila, Vila, Antonella, Amante, Analía, Manese, María Victoria, Zeida, Ari, Abrami, Laurence, Veggetti, Mariela, Guertin, David A, van der Goot, F Gisou, Corvi, María Martha, Colman-Lerner, Alejandro
Format: Article
Language:English
Subjects:
Akt
Cell and Developmental Biology
cell signaling
Golgi
lysosomes
S-palmitoylation
subcellular localization
Citations: Items that this one cites
Items that cite this one
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:The protein kinase Akt/PKB participates in a great variety of processes, including translation, cell proliferation and survival, as well as malignant transformation and viral infection. In the last few years, novel Akt posttranslational modifications have been found. However, how these modification patterns affect Akt subcellular localization, target specificity and, in general, function is not thoroughly understood. Here, we postulate and experimentally demonstrate by acyl-biotin exchange (ABE) assay and H-palmitate metabolic labeling that Akt is S-palmitoylated, a modification related to protein sorting throughout subcellular membranes. Mutating cysteine 344 into serine blocked Akt S-palmitoylation and diminished its phosphorylation at two key sites, T308 and T450. Particularly, we show that palmitoylation-deficient Akt increases its recruitment to cytoplasmic structures that colocalize with lysosomes, a process stimulated during autophagy. Finally, we found that cysteine 344 in Akt1 is important for proper its function, since Akt1-C344S was unable to support adipocyte cell differentiation These results add an unexpected new layer to the already complex Akt molecular code, improving our understanding of cell decision-making mechanisms such as cell survival, differentiation and death.
ISSN:2296-634X
2296-634X
DOI:10.3389/fcell.2021.626404