Irinotecan treatment and senescence failure promote the emergence of more transformed and invasive cells that depend on anti-apoptotic Mcl-1

Jonchère, Barbara; Vétillard, Alexandra; Toutain, Bertrand; Lam, David; Bernard, Anne; Henry, Cécile; Trécesson, Sophie de Carné; Gamelin, Érick; Juin, Philippe; Guette, Catherine; Coqueret, Olivier

doi:10.18632/oncotarget.2774

Cited by 46 publications

(58 citation statements)

References 47 publications

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“…Malheureusement, la sénescence induite par les thérapies anticancéreuses est peu stable. En effet, des cellules cancéreuses traitées à la doxorubicine ou à l'irinotecan, par exemple, entrent en sénescence mais, au cours du temps, certaines d'entre elles échappent à cet état [35][36][37][38].…”

Section: Resultsunclassified

Sénescence et cancer

Goy

Abbadie

2018

Med Sci (Paris)

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When ageing, cells profoundly reprogram to enter a state called senescence. Although the link between senescence and cancer is well established, the nature of this link remains unclear and debated. We will describe in this article the properties of senescent cells and make clear on how they could promote or oppose to cancer initiation and progression. We will also consider senescence as a response to classical anti-cancer therapies and discuss how to take advantage of senescence to improve the efficacy of these therapies while decreasing their toxicity.

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Section: Resultsunclassified

Sénescence et cancer

Goy

Abbadie

2018

Med Sci (Paris)

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“…We and others have shown that this suppression functions as an adaptive mechanism in response to chemotherapy-induced -senescence (CIS) (7,9). We have described that cancer cells can escape senescence and emerge as more transformed cells that resist anoikis and are more invasive (14)(15)(16)(17). In addition, we have also shown that cells having an incomplete senescence response are characterized by a reduced expression of CD47 (17).…”

Section: Introductionmentioning

confidence: 89%

tRNA Biogenesis and Specific Aminoacyl-tRNA Synthetases Regulate Senescence Stability Under the Control of mTOR

Guillon

Toutain

Boissard

et al. 2020

Preprint

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Running title: tRNA deregulation during senescence ABSTRACT Senescence normally prevents the propagation of abnormal cells but is also associated with cancer progression and chemotherapy resistance. These contradictory effects are related to the stability of epigenetic marks and to the senescence-associated secretory phenotype (SASP). The SASP reinforces the proliferative arrest but also induces tumor growth and inflammation during aging. S e n e s c e n c e i s t h e r e f o r e m u c h m o r e heterogeneous than initially thought. How this response varies is not really understood.Using experimental models of senescence escape, we now described that the deregulation of tRNA biogenesis affects the stability of this suppression, leading to chemotherapy resistance. Proteomic analyses showed that several aminoacyl-tRNA synthetases were down-regulated in senescent cells. tRNA transcription was also inhibited as a consequence of a reduced DNA binding of the type III RNA polymerase. Reducing RNA Pol III activity by BRF1 depletion maintained senescence and blocked cell persistence. Results showed that the YA R S 1 a n d L A R S 1 a m i n o a c y l -t R N A synthetases were necessary for cell emergence and that their corresponding tRNA-Leu-CAA and tRNA-Tyr-GTA were up-regulated in persistent cells. On the contrary, the CARS1 ligase had no effect on persistence and the expression of the corresponding tRNA-Cys was not modified. Results also showed that these tRNAs were regulated by mTOR and that this abnormal tRNA biogenesis induced an ER stress which was resolved by the kinase during chemotherapy escape.Overall, these findings highlight a new regulation of tRNA biology during senescence and suggest that specific tRNAs and ligases contribute to the strength and heterogeneity of this suppression and to chemotherapy resistance.

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“…These deleterious effects are not limited to carcinogenesis. We and others have also shown that these arrested cells and the proteins they secrete play a key role in chemotherapy resistance, allowing the generation of more aggressive cells in response to genotoxic treatments . For instance, important results indicate that Wnt activation induces the dedifferentiation of senescent cells, the reactivation of cell cycle progression, and the generation of subpopulations with higher tumor initiation potential .…”

Section: The Senescence‐associated Secretory Phenotypementioning

confidence: 95%

“…In this condition, we and others have shown that senescence relies on p21waf1 and it is not obvious that this protein is always acting as an inhibitor of cancer progression. Using different experimental models, we have shown that cancer cells enter senescence in response to chemotherapy but that persistent cells are able to escape this suppressive arrest . Senescence escape leads to the emergence of more transformed clones with enhanced potential for migration.…”

Section: Different Outcomes For Different Senescence Typesmentioning

confidence: 99%

Proteomics Approaches to Define Senescence Heterogeneity and Chemotherapy Response

et al. 2019

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In primary cells, senescence induces a permanent proliferative arrest to prevent the propagation of malignant cells. However, the outcome of senescence is more complex in advanced cancer cells where senescent states are heterogeneous. Here, this heterogeneity is discussed and it is proposed that proteomic analysis should be used to identify specific signatures of cancer cells that use this pathway as an adaptive mechanism. Since senescent cells produce an inflammatory secretome, MRM approaches and quantification with internal standards might be particularly suited to follow the expression of the corresponding markers in body fluids. Used in combination with imaging medical technics, a better characterization of senescence heterogeneity should help to monitor the response to chemotherapy treatment.

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Irinotecan treatment and senescence failure promote the emergence of more transformed and invasive cells that depend on anti-apoptotic Mcl-1

Cited by 46 publications

References 47 publications

Sénescence et cancer

Sénescence et cancer

tRNA Biogenesis and Specific Aminoacyl-tRNA Synthetases Regulate Senescence Stability Under the Control of mTOR

Proteomics Approaches to Define Senescence Heterogeneity and Chemotherapy Response

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