Proteomics

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A novel transcriptional signalling pathway mediated by the trafficking protein Ambra1 via scaffolding Atf2 complexes


ABSTRACT: Previously, we reported that Ambra1 is a core component of a cytoplasmic trafficking network, acting as a spatial rheostat to control active Src and FAK levels in addition to its critical roles in autophagy during neurogenesis. Here we identify a novel nuclear scaffolding function for Ambra1 that controls gene expression. Ambra1 binds to nuclear pore proteins, to other adaptor proteins like FAK and Akap8 in the nucleus, as well as to chromatin modifiers and transcriptional regulators such as Brg1, Cdk9 and the cAMP-regulated transcription factor Atf2. Ambra1 contributes to their association with chromatin and we identified genes whose transcription is regulated by Ambra1 complexes, likely via histone modifications and phospho-Atf2-dependent transcription. Therefore, Ambra1 scaffolds protein complexes at chromatin, regulating transcriptional signalling in the nucleus; in particular, it recruits chromatin modifiers and transcriptional regulators to control expression of genes such as Angpt1, Tgfb2, Tgfb3, Itga8 and Itgb7 that likely contribute to the role of Ambra1 in cancer cell invasion.

INSTRUMENT(S): Q Exactive HF

ORGANISM(S): Mus Musculus (mouse)

TISSUE(S): Squamous Cell Of Epidermis

DISEASE(S): Skin Cancer

SUBMITTER: Alex von kriegsheim  

LAB HEAD: Alex von kriegsheim

PROVIDER: PXD018745 | Pride | 2021-09-09

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
02_SCC-FAK-WT-Ambra1-1_170515102008.raw Raw
03_SCC-FAK-WT-Ambra1-2.raw Raw
04_SCC-FAK-WT-Ambra1-3.raw Raw
06_SCC-FAK-WT-IgG-1.raw Raw
07_SCC-FAK-WT-IgG-2.raw Raw
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Publications

The autophagy protein Ambra1 regulates gene expression by supporting novel transcriptional complexes.

Schoenherr Christina C   Byron Adam A   Griffith Billie B   Loftus Alexander A   Wills Jimi C JC   Munro Alison F AF   von Kriegsheim Alex A   Frame Margaret C MC  

The Journal of biological chemistry 20200702 34


Ambra1 is considered an autophagy and trafficking protein with roles in neurogenesis and cancer cell invasion. Here, we report that Ambra1 also localizes to the nucleus of cancer cells, where it has a novel nuclear scaffolding function that controls gene expression. Using biochemical fractionation and proteomics, we found that Ambra1 binds to multiple classes of proteins in the nucleus, including nuclear pore proteins, adaptor proteins such as FAK and Akap8, chromatin-modifying proteins, and tra  ...[more]

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