Cargando…
A multi-omics integrative approach unravels novel genes and pathways associated with senescence escape after targeted therapy in NRAS mutant melanoma
Therapy Induced Senescence (TIS) leads to sustained growth arrest of cancer cells. The associated cytostasis has been shown to be reversible and cells escaping senescence further enhance the aggressiveness of cancers. Chemicals specifically targeting senescent cells, so-called senolytics, constitute...
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Nature Publishing Group US
2023
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10581906/ https://www.ncbi.nlm.nih.gov/pubmed/37420093 http://dx.doi.org/10.1038/s41417-023-00640-z |
| _version_ | 1785122215661928448 |
|---|---|
| author | Gureghian, Vincent Herbst, Hailee Kozar, Ines Mihajlovic, Katarina Malod-Dognin, Noël Ceddia, Gaia Angeli, Cristian Margue, Christiane Randic, Tijana Philippidou, Demetra Nomigni, Milène Tetsi Hemedan, Ahmed Tranchevent, Leon-Charles Longworth, Joseph Bauer, Mark Badkas, Apurva Gaigneaux, Anthoula Muller, Arnaud Ostaszewski, Marek Tolle, Fabrice Pržulj, Nataša Kreis, Stephanie |
| author_facet | Gureghian, Vincent Herbst, Hailee Kozar, Ines Mihajlovic, Katarina Malod-Dognin, Noël Ceddia, Gaia Angeli, Cristian Margue, Christiane Randic, Tijana Philippidou, Demetra Nomigni, Milène Tetsi Hemedan, Ahmed Tranchevent, Leon-Charles Longworth, Joseph Bauer, Mark Badkas, Apurva Gaigneaux, Anthoula Muller, Arnaud Ostaszewski, Marek Tolle, Fabrice Pržulj, Nataša Kreis, Stephanie |
| author_sort | Gureghian, Vincent |
| collection | PubMed |
| description | Therapy Induced Senescence (TIS) leads to sustained growth arrest of cancer cells. The associated cytostasis has been shown to be reversible and cells escaping senescence further enhance the aggressiveness of cancers. Chemicals specifically targeting senescent cells, so-called senolytics, constitute a promising avenue for improved cancer treatment in combination with targeted therapies. Understanding how cancer cells evade senescence is needed to optimise the clinical benefits of this therapeutic approach. Here we characterised the response of three different NRAS mutant melanoma cell lines to a combination of CDK4/6 and MEK inhibitors over 33 days. Transcriptomic data show that all cell lines trigger a senescence programme coupled with strong induction of interferons. Kinome profiling revealed the activation of Receptor Tyrosine Kinases (RTKs) and enriched downstream signaling of neurotrophin, ErbB and insulin pathways. Characterisation of the miRNA interactome associates miR-211-5p with resistant phenotypes. Finally, iCell-based integration of bulk and single-cell RNA-seq data identifies biological processes perturbed during senescence and predicts 90 new genes involved in its escape. Overall, our data associate insulin signaling with persistence of a senescent phenotype and suggest a new role for interferon gamma in senescence escape through the induction of EMT and the activation of ERK5 signaling. |
| format | Online Article Text |
| id | pubmed-10581906 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2023 |
| publisher | Nature Publishing Group US |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-105819062023-10-19 A multi-omics integrative approach unravels novel genes and pathways associated with senescence escape after targeted therapy in NRAS mutant melanoma Gureghian, Vincent Herbst, Hailee Kozar, Ines Mihajlovic, Katarina Malod-Dognin, Noël Ceddia, Gaia Angeli, Cristian Margue, Christiane Randic, Tijana Philippidou, Demetra Nomigni, Milène Tetsi Hemedan, Ahmed Tranchevent, Leon-Charles Longworth, Joseph Bauer, Mark Badkas, Apurva Gaigneaux, Anthoula Muller, Arnaud Ostaszewski, Marek Tolle, Fabrice Pržulj, Nataša Kreis, Stephanie Cancer Gene Ther Article Therapy Induced Senescence (TIS) leads to sustained growth arrest of cancer cells. The associated cytostasis has been shown to be reversible and cells escaping senescence further enhance the aggressiveness of cancers. Chemicals specifically targeting senescent cells, so-called senolytics, constitute a promising avenue for improved cancer treatment in combination with targeted therapies. Understanding how cancer cells evade senescence is needed to optimise the clinical benefits of this therapeutic approach. Here we characterised the response of three different NRAS mutant melanoma cell lines to a combination of CDK4/6 and MEK inhibitors over 33 days. Transcriptomic data show that all cell lines trigger a senescence programme coupled with strong induction of interferons. Kinome profiling revealed the activation of Receptor Tyrosine Kinases (RTKs) and enriched downstream signaling of neurotrophin, ErbB and insulin pathways. Characterisation of the miRNA interactome associates miR-211-5p with resistant phenotypes. Finally, iCell-based integration of bulk and single-cell RNA-seq data identifies biological processes perturbed during senescence and predicts 90 new genes involved in its escape. Overall, our data associate insulin signaling with persistence of a senescent phenotype and suggest a new role for interferon gamma in senescence escape through the induction of EMT and the activation of ERK5 signaling. Nature Publishing Group US 2023-07-07 2023 /pmc/articles/PMC10581906/ /pubmed/37420093 http://dx.doi.org/10.1038/s41417-023-00640-z Text en © The Author(s) 2023 https://creativecommons.org/licenses/by/4.0/Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) . |
| spellingShingle | Article Gureghian, Vincent Herbst, Hailee Kozar, Ines Mihajlovic, Katarina Malod-Dognin, Noël Ceddia, Gaia Angeli, Cristian Margue, Christiane Randic, Tijana Philippidou, Demetra Nomigni, Milène Tetsi Hemedan, Ahmed Tranchevent, Leon-Charles Longworth, Joseph Bauer, Mark Badkas, Apurva Gaigneaux, Anthoula Muller, Arnaud Ostaszewski, Marek Tolle, Fabrice Pržulj, Nataša Kreis, Stephanie A multi-omics integrative approach unravels novel genes and pathways associated with senescence escape after targeted therapy in NRAS mutant melanoma |
| title | A multi-omics integrative approach unravels novel genes and pathways associated with senescence escape after targeted therapy in NRAS mutant melanoma |
| title_full | A multi-omics integrative approach unravels novel genes and pathways associated with senescence escape after targeted therapy in NRAS mutant melanoma |
| title_fullStr | A multi-omics integrative approach unravels novel genes and pathways associated with senescence escape after targeted therapy in NRAS mutant melanoma |
| title_full_unstemmed | A multi-omics integrative approach unravels novel genes and pathways associated with senescence escape after targeted therapy in NRAS mutant melanoma |
| title_short | A multi-omics integrative approach unravels novel genes and pathways associated with senescence escape after targeted therapy in NRAS mutant melanoma |
| title_sort | multi-omics integrative approach unravels novel genes and pathways associated with senescence escape after targeted therapy in nras mutant melanoma |
| topic | Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10581906/ https://www.ncbi.nlm.nih.gov/pubmed/37420093 http://dx.doi.org/10.1038/s41417-023-00640-z |
| work_keys_str_mv | AT gureghianvincent amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT herbsthailee amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT kozarines amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT mihajlovickatarina amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT maloddogninnoel amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT ceddiagaia amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT angelicristian amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT marguechristiane amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT randictijana amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT philippidoudemetra amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT nomignimilenetetsi amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT hemedanahmed amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT trancheventleoncharles amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT longworthjoseph amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT bauermark amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT badkasapurva amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT gaigneauxanthoula amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT mullerarnaud amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT ostaszewskimarek amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT tollefabrice amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT przuljnatasa amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT kreisstephanie amultiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT gureghianvincent multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT herbsthailee multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT kozarines multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT mihajlovickatarina multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT maloddogninnoel multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT ceddiagaia multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT angelicristian multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT marguechristiane multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT randictijana multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT philippidoudemetra multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT nomignimilenetetsi multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT hemedanahmed multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT trancheventleoncharles multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT longworthjoseph multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT bauermark multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT badkasapurva multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT gaigneauxanthoula multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT mullerarnaud multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT ostaszewskimarek multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT tollefabrice multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT przuljnatasa multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma AT kreisstephanie multiomicsintegrativeapproachunravelsnovelgenesandpathwaysassociatedwithsenescenceescapeaftertargetedtherapyinnrasmutantmelanoma |