SUMOylation of p53 mediates interferon activities

Marcos-Villar, Laura; Pérez-Girón, José; Vilas Martínez, Jessica María; Soto Simón, Atenea; de la Cruz-Herrera, Carlos; Lang, Valerie; Collado Rodríguez, Manuel; Vidal Figueroa, Anxo; Rodríguez, Manuel; Muñoz-Fontela, Cesar; Rivas ?, Carmen

doi:10.4161/cc.25868

Marcos-Villar, Laura; Pérez-Girón, José; Vilas Martínez, Jessica María; Soto Simón, Atenea; de la Cruz-Herrera, Carlos; Lang, Valerie; Collado Rodríguez, Manuel; Vidal Figueroa, Anxo; Rodríguez, Manuel; Muñoz-Fontela, Cesar; Rivas ?, Carmen

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Identifiers

URI: http://hdl.handle.net/20.500.11940/3634

PMID: 23966171

DOI: 10.4161/cc.25868

ISSN: 1538-4101

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Cell Cycle. 2013;12(17): 2809-16 (50.42Kb)

Cell Cycle. 2013;12(17): 2809-16 (2.035Mb)

Date issued

2013

Journal title

CELL CYCLE

Type of content

Artigo

DeCS

Antivirales | Interferón-alfa

MeSH

Antiviral Agents | Interferon-alpha

Abstract

There is growing evidence that many host proteins involved in innate and intrinsic immunity are regulated by SUMOylation, and that SUMO contributes to the regulatory process that governs the initiation of the type I interferon (IFN) response. The tumor suppressor p53 is a modulator of the IFN response that plays a role in virus-induced apoptosis and in IFN-induced senescence. Here we demonstrate that IFN treatment increases the levels of SUMOylated p53 and induces cellular senescence through a process that is partially dependent upon SUMOylation of p53. Similarly, we show that vesicular stomatitis virus (VSV) infection induces p53 SUMOylation, and that this modification favors the control of VSV replication. Thus, our study provides evidence that IFN signaling induces p53 SUMOylation, which results in the activation of a cellular senescence program and contributes to the antiviral functions of interferon.

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