Nuclear inclusion bodies of mutant and wild‐type p53 in cancer: a hallmark of p53 inactivation and proteostasis remodelling by p53 aggregation

Smet, Frederik De; Rubio, Mirian Saiz; Hompes, Daphne; Naus, Evelyne; Baets, Greet De; Langenberg, Tobias; Hipp, Mark S.; Houben, Bert; Claes, Filip; Charbonneau, Sarah; Delgado, Javier; Plaisance, Stéphane; Ramkissoon, Shakti; Ramkissoon, Lori; Simons, Colinda C.J.M.; Brandt, Piet A. van den; Weijenberg, Matty; England, Manon Van; Lambrechts, Sandrina; Amant, Frédéric; D’Hoore, André; Ligon, Keith L.; Sagaert, Xavier; Schymkowitz, Joost; Rousseau, Frédéric

doi:10.1002/path.4872

Cited by 57 publications

(79 citation statements)

References 66 publications

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“…HEK293 cells (female) stably expressing UbG76V-GFP (Dantuma et al, 2000; De Smet et al, 2017) were cultured in Dulbecco’s modified Eagle’s medium (DMEM; Biochrom) supplemented with 10 % (v/v) fetal bovine serum (Gibco), 2 mM L-glutamine (Gibco), penicillin-streptomycin (Thermo Fisher) and non-essential amino acids (Gibco). Transfection was carried out using FuGENE 6 (Promega).…”

Section: Star Methodsmentioning

confidence: 99%

In Situ Structure of Neuronal C9orf72 Poly-GA Aggregates Reveals Proteasome Recruitment

Guo

Lehmer

Martínez-Sánchez

et al. 2018

Cell

335

317

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Summary Protein aggregation and dysfunction of the ubiquitin-proteasome system are hallmarks of many neurodegenerative diseases. Here we address the elusive link between these phenomena employing cryo-electron tomography to dissect the molecular architecture of protein aggregates within intact neurons at high resolution. We focus on the poly-Gly-Ala (GA) aggregates resulting from aberrant translation of an expanded GGGGCC repeat in C9orf72, the most common genetic cause of amyotrophic lateral sclerosis and frontotemporal dementia. We find that poly-GA aggregates consist of densely packed twisted ribbons that recruit numerous 26S proteasome complexes, while other macromolecules are largely excluded. Proximity to poly-GA ribbons stabilizes a transient substrate-processing conformation of the 26S proteasome, suggesting stalled degradation. Thus, poly-GA aggregates may compromise neuronal proteostasis by driving the accumulation and functional impairment of a large fraction of cellular proteasomes.

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Section: Star Methodsmentioning

confidence: 99%

In Situ Structure of Neuronal C9orf72 Poly-GA Aggregates Reveals Proteasome Recruitment

Guo

Lehmer

Martínez-Sánchez

et al. 2018

Cell

335

317

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“…HEK293 cells stably expressing Ub G76V ‐GFP (Dantuma et al , ; De Smet et al , ) were transfected with the indicated constructs for co‐culture assays or incubated with conditioned media from GA 175 ‐RFP‐ or RFP‐expressing cells for 48 h. Subsequently, receiver cells were harvested and analyzed by flow cytometry for GFP and RFP fluorescence using an Attune NxT Cytometric Analyser (Thermo Fisher) at the Imaging Facility of the Max Planck Institute of Biochemistry, Martinsried. Fluorescence was detected using the following settings: GFP Ex 488 nm, Em 530/30 nm, tagRFP Ex 561 nm, and Em 586/15 nm.…”

Section: Methodsmentioning

confidence: 99%

Cell‐to‐cell transmission of C9orf72 poly‐(Gly‐Ala) triggers key features of ALS / FTD

et al. 2020

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The C9orf72 repeat expansion causes amyotrophic lateral sclerosis and frontotemporal dementia, but the poor correlation between C9orf72-specific pathology and TDP-43 pathology linked to neurodegeneration hinders targeted therapeutic development.Here, we addressed the role of the aggregating dipeptide repeat proteins resulting from unconventional translation of the repeat in all reading frames. Poly-GA promoted cytoplasmic mislocalization and aggregation of TDP-43 non-cell-autonomously, and anti-GA antibodies ameliorated TDP-43 mislocalization in both donor and receiver cells. Cell-to-cell transmission of poly-GA inhibited proteasome function in neighboring cells. Importantly, proteasome inhibition led to the accumulation of TDP-43 ubiquitinated within the nuclear localization signal (NLS) at lysine 95. Mutagenesis of this ubiquitination site completely blocked poly-GA-dependent mislocalization of TDP-43. Boosting proteasome function with rolipram reduced both poly-GA and TDP-43 aggregation. Our data from cell lines, primary neurons, transgenic mice, and patient tissue suggest that poly-GA promotes TDP-43 aggregation by inhibiting the proteasome cell-autonomously and non-cell-autonomously, which can be prevented by inhibiting poly-GA transmission with antibodies or boosting proteasome activity with rolipram.

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“…Given that mutant p53 is inhibiting the function of TAp63 and TAp73, it has been postulated that through aggregation, mutant p53 might inactivate its family members, preventing them from interacting with their target gene promoters [51,66]. Aggregation was identified as punctate staining for p53 in the cytoplasm or nucleus [67]. A punctate p53 staining has been identified in cancers with mutant or wildtype p53 expression and has been correlated to worse outcomes [67].…”

Section: Mutant P53 Aggregation and Other Binding Partnersmentioning

confidence: 99%

The Diverse Functions of Mutant 53, Its Family Members and Isoforms in Cancer

Hall

Müller

2019

IJMS

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The p53 family of proteins has grown substantially over the last 40 years. It started with p53, then p63, p73, isoforms and mutants of these proteins. The function of p53 as a tumour suppressor has been thoroughly investigated, but the functions of all isoforms and mutants and the interplay between them are still poorly understood. Mutant p53 proteins lose p53 function, display dominant-negative (DN) activity and display gain-of-function (GOF) to varying degrees. GOF was originally attributed to mutant p53′s inhibitory function over the p53 family members p63 and p73. It has become apparent that this is not the only way in which mutant p53 operates as a large number of transcription factors that are not related to p53 are activated on mutant p53 binding. This raises the question to what extent mutant p53 binding to p63 and p73 plays a role in mutant p53 GOF. In this review, we discuss the literature around the interaction between mutant p53 and family members, including other binding partners, the functional consequences and potential therapeutics.

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Nuclear inclusion bodies of mutant and wild‐type p53 in cancer: a hallmark of p53 inactivation and proteostasis remodelling by p53 aggregation

Cited by 57 publications

References 66 publications

In Situ Structure of Neuronal C9orf72 Poly-GA Aggregates Reveals Proteasome Recruitment

In Situ Structure of Neuronal C9orf72 Poly-GA Aggregates Reveals Proteasome Recruitment

Cell‐to‐cell transmission of C9orf72 poly‐(Gly‐Ala) triggers key features of ALS / FTD

The Diverse Functions of Mutant 53, Its Family Members and Isoforms in Cancer

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