Cargando…
A way to understand idiopathic senescence and apoptosis in primary glioblastoma cells – possible approaches to circumvent these phenomena
BACKGROUND: Glioblastoma (GB) is considered one of the most lethal tumors. Extensive research at the molecular level may enable to gain more profound insight into its biology and thus, facilitate development and testing of new therapeutic approaches. Unfortunately, stable glioblastoma cell lines do...
| Autores principales: | , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
BioMed Central
2019
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6744717/ https://www.ncbi.nlm.nih.gov/pubmed/31521143 http://dx.doi.org/10.1186/s12885-019-6130-2 |
| _version_ | 1783451430835716096 |
|---|---|
| author | Janik, Karolina Treda, Cezary Wlodarczyk, Aneta Peciak, Joanna Rosiak, Kamila Zieba, Jolanta Grot, Dagmara Rutkowska, Adrianna Pawlowska, Roza Och, Waldemar Rieske, Piotr Stoczynska-Fidelus, Ewelina |
| author_facet | Janik, Karolina Treda, Cezary Wlodarczyk, Aneta Peciak, Joanna Rosiak, Kamila Zieba, Jolanta Grot, Dagmara Rutkowska, Adrianna Pawlowska, Roza Och, Waldemar Rieske, Piotr Stoczynska-Fidelus, Ewelina |
| author_sort | Janik, Karolina |
| collection | PubMed |
| description | BACKGROUND: Glioblastoma (GB) is considered one of the most lethal tumors. Extensive research at the molecular level may enable to gain more profound insight into its biology and thus, facilitate development and testing of new therapeutic approaches. Unfortunately, stable glioblastoma cell lines do not reflect highly heterogeneous nature of this tumor, while its primary cultures are difficult to maintain in vitro. We previously reported that senescence is one of the major mechanisms responsible for primary GB cells stabilization failure, to a lesser extent accompanied by apoptosis and mitotic catastrophe-related cell death. METHODS: We made an attempt to circumvent difficulties with glioblastoma primary cultures by testing 3 different approaches aimed to prolong their in vitro maintenance, on a model of 10 patient-derived tumor specimens. RESULTS: Two out of ten analyzed GB specimens were successfully stabilized, regardless of culture approach applied. Importantly, cells transduced with immortalizing factors or cultured in neural stem cell-like conditions were still undergoing senescence/apoptosis. Sequential in vivo/in vitro cultivation turned out to be the most effective, however, it only enabled to propagate cells with preserved molecular profile up to 3(rd) mice transfer. Nevertheless, it was the only method that impeded these phenomena long enough to provide sufficient amount of material for in vitro/in vivo targeted analyses. Interestingly, our data additionally demonstrated that some subpopulations of several stabilized GB cell lines undergo idiopathic senescence, however, it is counterbalanced by simultaneous proliferation of other cell subpopulations. CONCLUSIONS: In the majority of primary glioma cultures, there has to be an imbalance towards apoptosis and senescence, following few weeks of rapid proliferation. Our results indicate that it has to be associated with the mechanisms other than maintenance of glioblastoma stem cells or dependence on proteins controlling cell cycle. |
| format | Online Article Text |
| id | pubmed-6744717 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2019 |
| publisher | BioMed Central |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-67447172019-09-18 A way to understand idiopathic senescence and apoptosis in primary glioblastoma cells – possible approaches to circumvent these phenomena Janik, Karolina Treda, Cezary Wlodarczyk, Aneta Peciak, Joanna Rosiak, Kamila Zieba, Jolanta Grot, Dagmara Rutkowska, Adrianna Pawlowska, Roza Och, Waldemar Rieske, Piotr Stoczynska-Fidelus, Ewelina BMC Cancer Research Article BACKGROUND: Glioblastoma (GB) is considered one of the most lethal tumors. Extensive research at the molecular level may enable to gain more profound insight into its biology and thus, facilitate development and testing of new therapeutic approaches. Unfortunately, stable glioblastoma cell lines do not reflect highly heterogeneous nature of this tumor, while its primary cultures are difficult to maintain in vitro. We previously reported that senescence is one of the major mechanisms responsible for primary GB cells stabilization failure, to a lesser extent accompanied by apoptosis and mitotic catastrophe-related cell death. METHODS: We made an attempt to circumvent difficulties with glioblastoma primary cultures by testing 3 different approaches aimed to prolong their in vitro maintenance, on a model of 10 patient-derived tumor specimens. RESULTS: Two out of ten analyzed GB specimens were successfully stabilized, regardless of culture approach applied. Importantly, cells transduced with immortalizing factors or cultured in neural stem cell-like conditions were still undergoing senescence/apoptosis. Sequential in vivo/in vitro cultivation turned out to be the most effective, however, it only enabled to propagate cells with preserved molecular profile up to 3(rd) mice transfer. Nevertheless, it was the only method that impeded these phenomena long enough to provide sufficient amount of material for in vitro/in vivo targeted analyses. Interestingly, our data additionally demonstrated that some subpopulations of several stabilized GB cell lines undergo idiopathic senescence, however, it is counterbalanced by simultaneous proliferation of other cell subpopulations. CONCLUSIONS: In the majority of primary glioma cultures, there has to be an imbalance towards apoptosis and senescence, following few weeks of rapid proliferation. Our results indicate that it has to be associated with the mechanisms other than maintenance of glioblastoma stem cells or dependence on proteins controlling cell cycle. BioMed Central 2019-09-14 /pmc/articles/PMC6744717/ /pubmed/31521143 http://dx.doi.org/10.1186/s12885-019-6130-2 Text en © The Author(s). 2019 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided 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 Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated. |
| spellingShingle | Research Article Janik, Karolina Treda, Cezary Wlodarczyk, Aneta Peciak, Joanna Rosiak, Kamila Zieba, Jolanta Grot, Dagmara Rutkowska, Adrianna Pawlowska, Roza Och, Waldemar Rieske, Piotr Stoczynska-Fidelus, Ewelina A way to understand idiopathic senescence and apoptosis in primary glioblastoma cells – possible approaches to circumvent these phenomena |
| title | A way to understand idiopathic senescence and apoptosis in primary glioblastoma cells – possible approaches to circumvent these phenomena |
| title_full | A way to understand idiopathic senescence and apoptosis in primary glioblastoma cells – possible approaches to circumvent these phenomena |
| title_fullStr | A way to understand idiopathic senescence and apoptosis in primary glioblastoma cells – possible approaches to circumvent these phenomena |
| title_full_unstemmed | A way to understand idiopathic senescence and apoptosis in primary glioblastoma cells – possible approaches to circumvent these phenomena |
| title_short | A way to understand idiopathic senescence and apoptosis in primary glioblastoma cells – possible approaches to circumvent these phenomena |
| title_sort | way to understand idiopathic senescence and apoptosis in primary glioblastoma cells – possible approaches to circumvent these phenomena |
| topic | Research Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6744717/ https://www.ncbi.nlm.nih.gov/pubmed/31521143 http://dx.doi.org/10.1186/s12885-019-6130-2 |
| work_keys_str_mv | AT janikkarolina awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT tredacezary awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT wlodarczykaneta awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT peciakjoanna awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT rosiakkamila awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT ziebajolanta awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT grotdagmara awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT rutkowskaadrianna awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT pawlowskaroza awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT ochwaldemar awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT rieskepiotr awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT stoczynskafidelusewelina awaytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT janikkarolina waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT tredacezary waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT wlodarczykaneta waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT peciakjoanna waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT rosiakkamila waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT ziebajolanta waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT grotdagmara waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT rutkowskaadrianna waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT pawlowskaroza waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT ochwaldemar waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT rieskepiotr waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena AT stoczynskafidelusewelina waytounderstandidiopathicsenescenceandapoptosisinprimaryglioblastomacellspossibleapproachestocircumventthesephenomena |