hTERT: a novel endogenous inhibitor of the mitochondrial cell death pathway

Massard, Christophe; Zermati, Yaël; Pauleau, A-L; Larochette, Nathanaël; Métivier, Didier; Sabatier, Laure; Kroemer, Guido; Soria, J-C.

doi:10.1038/sj.onc.1209487

Cited by 132 publications

(144 citation statements)

References 58 publications

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“…The bars in a-c represent standard errors with ** and *** indicating Pr0.01 and Pr0.001, respectively cell death induced by mitomycin C, a potent DNA crosslinker used in cancer treatment to induce mitochondrial apoptosis. 20,21 Figure 1b shows that DN-Aven 180-362 and the bona fide apoptosis inhibitor Bcl-x L both significantly inhibited apoptosis caused by mitomycin C at different concentrations, whereas expression of full-length Aven did not confer protection under this experimental paradigm.…”

Section: Resultsmentioning

confidence: 99%

The Apaf-1-binding protein Aven is cleaved by Cathepsin D to unleash its anti-apoptotic potential

et al. 2012

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The anti-apoptotic molecule Aven was originally identified in a yeast two-hybrid screen for Bcl-x L -interacting proteins and has also been found to bind Apaf-1, thereby interfering with Apaf-1 self-association during apoptosome assembly. Aven is expressed in a wide variety of adult tissues and cell lines, and there is increasing evidence that its overexpression correlates with tumorigenesis, particularly in acute leukemias. The mechanism by which the anti-apoptotic activity of Aven is regulated remains poorly understood. Here we shed light on this issue by demonstrating that proteolytic removal of an inhibitory N-terminal Aven domain is necessary to activate the anti-apoptotic potential of the molecule. Furthermore, we identify Cathepsin D (CathD) as the protease responsible for Aven cleavage. On the basis of our results, we propose a model of Aven activation by which its N-terminal inhibitory domain is removed by CathD-mediated proteolysis, thereby unleashing its cytoprotective function.

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Section: Resultsmentioning

confidence: 99%

The Apaf-1-binding protein Aven is cleaved by Cathepsin D to unleash its anti-apoptotic potential

et al. 2012

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“…In addition, it has been shown that overexpression of hTERT suppresses apoptosis at a premitochondrial step before the release of cytochrome c and apoptosis-inducing factor [32]. Recent studies showed that down-regulation of hTERT expression by hTERT specific interfering RNA (siRNA) sensitizes mitochondrial pathways of apoptosis without apparent involvement of telomere erosion due to telomerase inhibition, rather by post-translational activation of Bax protein which triggers a CD-90 independent mitochondrial pathway of apoptosis [33]. More recent report indicated that TERT promotes cellular and organismal survival independent of telomerase activity [34].…”

Section: Telomerase In Apoptosismentioning

confidence: 99%

Actions of human telomerase beyond telomeres

Cong

Shay²

2008

Cell Res

206

164

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“…It is unlikely that rapid telomere shortening occurred in that cells, and high dose of TELIN may invoke another physiological response of MOLT-4 cells. hTERT is reported to function in mitochondria to suppress the course of apoptosis process, and so is expected as anticancer target (Massard et al 2006), and we have not excluded the possibility that TELIN potentially targets hTERT in mitochondoria.…”

Section: Suppression Of Telomerase Enzyme By Telinmentioning

confidence: 99%

Inhibition of Human Tumor Cell Proliferation by the Telomerase Inhibitor TELIN

et al. 2010

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Summary TELIN, a newly developed catalytic blocker of telomerase, was assessed for its antiproliferative activity against human tumor cells in in vitro cell culture assay. TELIN suppressed cell proliferations of several blood tumor cells with telomere shortening and the appearance of apoptotic small cells, but did not affect hTERT mRNA expression, suggesting that TELIN catalytically inhibited telomerase activity within the cells. TELIN also suppressed cell proliferation of adherent tumor cells, whereas it did not affect the growth of normal fibroblasts. Delivery efficiency of TELIN was significantly different between several delivery carriers, and b-cyclodextrin was found to be a suitable carrier.

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hTERT: a novel endogenous inhibitor of the mitochondrial cell death pathway

Cited by 132 publications

References 58 publications

The Apaf-1-binding protein Aven is cleaved by Cathepsin D to unleash its anti-apoptotic potential

The Apaf-1-binding protein Aven is cleaved by Cathepsin D to unleash its anti-apoptotic potential

Actions of human telomerase beyond telomeres

Inhibition of Human Tumor Cell Proliferation by the Telomerase Inhibitor TELIN

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