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3 research outputs found

Parkin-independent mitophagy controls chemotherapeutic response in cancer cells

Author: Bossowski Jozef P.
Chiche Johanna
Marchetti Sandrine
Mondragón Laura
Obba Sandrine
Proïcs Emma
Ricci Jean-Ehrland
Riley Joel S.
Rozier Romain M.
Rubio-Patiño Camila
Tait Stephen W.G.
Verhoeyen Els
Villa Elodie
Zunino Barbara
Publication venue: 'Elsevier BV'
Publication date: 01/09/2017
Field of study

Mitophagy is an evolutionarily conserved process that selectively targets impaired mitochondria for degradation. Defects in mitophagy are often associated with diverse pathologies, including cancer. Because the main known regulators of mitophagy are frequently inactivated in cancer cells, the mechanisms that regulate mitophagy in cancer cells are not fully understood. Here, we identified an E3 ubiquitin ligase (ARIH1/HHARI) that triggers mitophagy in cancer cells in a PINK1-dependent manner. We found that ARIH1/HHARI polyubiquitinates damaged mitochondria, leading to their removal via autophagy. Importantly, ARIH1 is widely expressed in cancer cells, notably in breast and lung adenocarcinomas; ARIH1 expression protects against chemotherapy-induced death. These data challenge the view that the main regulators of mitophagy are tumor suppressors, arguing instead that ARIH1-mediated mitophagy promotes therapeutic resistance

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Mitochondrial permeabilization engages NF-κB-dependent anti-tumour activity under caspase deficiency

Author: Albert Matthew L.
Blyth Karen
Bock Florian
Cao Kai
Cloix Catherine
Dhayade Sandeep
Fort Loic
Giampazolias Evangelos
Ichim Gabriel
Lecis Daniele
Lopez Jonathan
Machesky Laura
Milling Simon
Oberst Andrew
Orozco Susana
Peltzer Nieves
Proïcs Emma
Ricci Jean-Ehrland
Roca Alba
Rubio-Patiño Camila
Ryan Kevin M.
Tait Stephen W.G.
Taraborrelli Lucia
Walczak Henning
Woodham Emma
Yatim Nader
Zunino Barbara
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/09/2017
Field of study

Apoptosis represents a key anti-cancer therapeutic effector mechanism. During apoptosis, mitochondrial outer membrane permeabilization (MOMP) typically kills cells even in the absence of caspase activity. Caspase activity can also have a variety of unwanted consequences that include DNA damage. We therefore investigated whether MOMP-induced caspase-independent cell death (CICD) might be a better way to kill cancer cells. We find that cells undergoing CICD display potent pro-inflammatory effects relative to apoptosis. Underlying this, MOMP was found to stimulate NF-κB activity through the downregulation of inhibitor of apoptosis proteins. Strikingly, engagement of CICD displays potent anti-tumorigenic effects, often promoting complete tumour regression in a manner dependent on intact immunity. Our data demonstrate that by activating NF-κB, MOMP can exert additional signalling functions besides triggering cell death. Moreover, they support a rationale for engaging caspase-independent cell death in cell-killing anti-cancer therapies

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GAPDH Overexpression in the T Cell Lineage Promotes Angioimmunoblastic T Cell Lymphoma through an NF-κB-Dependent Mechanism

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