Overcoming platinum-acquired resistance in ovarian cancer patient-derived xenografts
Background: Epithelial ovarian cancer is the most lethal gynecological cancer and the high mortality is due to the frequent presentation at advanced stage, and to primary or acquired resistance to platinum-based therapy. Methods: We developed three new models of ovarian cancer patient-derived xenogr...
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SAGE Publishing
2019-06-01
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| Series: | Therapeutic Advances in Medical Oncology |
| Online Access: | https://doi.org/10.1177/1758835919839543 |
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doaj-db1da62259964a9d8e68313c82d64fe92020-11-25T02:59:18ZengSAGE PublishingTherapeutic Advances in Medical Oncology1758-83592019-06-011110.1177/1758835919839543Overcoming platinum-acquired resistance in ovarian cancer patient-derived xenograftsFrancesca RicciLaura BrunelliRoberta AffatatoRosaria ChilàMartina VerzaStefano IndraccoloFrancesca FalcettaMaddalena FratelliRobert FruscioRoberta PastorelliGiovanna DamiaBackground: Epithelial ovarian cancer is the most lethal gynecological cancer and the high mortality is due to the frequent presentation at advanced stage, and to primary or acquired resistance to platinum-based therapy. Methods: We developed three new models of ovarian cancer patient-derived xenografts (ovarian PDXs) resistant to cisplatin (cDDP) after multiple in vivo drug treatments. By different and complementary approaches based on integrated metabolomics (both targeted and untargeted mass spectrometry-based techniques), gene expression, and functional assays (Seahorse technology) we analyzed and compared the tumor metabolic profile in each sensitive and their corresponding cDDP-resistant PDXs. Results: We found that cDDP-sensitive and -resistant PDXs have a different metabolic asset. In particular, we found, through metabolomic and gene expression approaches, that glycolysis, tricarboxylic acid cycle and urea cycle pathways were deregulated in resistant versus sensitive PDXs. In addition, we observed that oxygen consumption rate and mitochondrial respiration were higher in resistant PDXs than in sensitive PDXs under acute stress conditions. An increased oxidative phosphorylation in cDDP-resistant sublines led us to hypothesize that its interference could be of therapeutic value. Indeed, in vivo treatment of metformin and cDDP was able to partially reverse platinum resistance. Conclusions: Our data strongly reinforce the idea that the development of acquired cDDP resistance in ovarian cancer can bring about a rewiring of tumor metabolism, and that this might be exploited therapeutically.https://doi.org/10.1177/1758835919839543 |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Francesca Ricci Laura Brunelli Roberta Affatato Rosaria Chilà Martina Verza Stefano Indraccolo Francesca Falcetta Maddalena Fratelli Robert Fruscio Roberta Pastorelli Giovanna Damia |
| spellingShingle |
Francesca Ricci Laura Brunelli Roberta Affatato Rosaria Chilà Martina Verza Stefano Indraccolo Francesca Falcetta Maddalena Fratelli Robert Fruscio Roberta Pastorelli Giovanna Damia Overcoming platinum-acquired resistance in ovarian cancer patient-derived xenografts Therapeutic Advances in Medical Oncology |
| author_facet |
Francesca Ricci Laura Brunelli Roberta Affatato Rosaria Chilà Martina Verza Stefano Indraccolo Francesca Falcetta Maddalena Fratelli Robert Fruscio Roberta Pastorelli Giovanna Damia |
| author_sort |
Francesca Ricci |
| title |
Overcoming platinum-acquired resistance in ovarian cancer patient-derived xenografts |
| title_short |
Overcoming platinum-acquired resistance in ovarian cancer patient-derived xenografts |
| title_full |
Overcoming platinum-acquired resistance in ovarian cancer patient-derived xenografts |
| title_fullStr |
Overcoming platinum-acquired resistance in ovarian cancer patient-derived xenografts |
| title_full_unstemmed |
Overcoming platinum-acquired resistance in ovarian cancer patient-derived xenografts |
| title_sort |
overcoming platinum-acquired resistance in ovarian cancer patient-derived xenografts |
| publisher |
SAGE Publishing |
| series |
Therapeutic Advances in Medical Oncology |
| issn |
1758-8359 |
| publishDate |
2019-06-01 |
| description |
Background: Epithelial ovarian cancer is the most lethal gynecological cancer and the high mortality is due to the frequent presentation at advanced stage, and to primary or acquired resistance to platinum-based therapy. Methods: We developed three new models of ovarian cancer patient-derived xenografts (ovarian PDXs) resistant to cisplatin (cDDP) after multiple in vivo drug treatments. By different and complementary approaches based on integrated metabolomics (both targeted and untargeted mass spectrometry-based techniques), gene expression, and functional assays (Seahorse technology) we analyzed and compared the tumor metabolic profile in each sensitive and their corresponding cDDP-resistant PDXs. Results: We found that cDDP-sensitive and -resistant PDXs have a different metabolic asset. In particular, we found, through metabolomic and gene expression approaches, that glycolysis, tricarboxylic acid cycle and urea cycle pathways were deregulated in resistant versus sensitive PDXs. In addition, we observed that oxygen consumption rate and mitochondrial respiration were higher in resistant PDXs than in sensitive PDXs under acute stress conditions. An increased oxidative phosphorylation in cDDP-resistant sublines led us to hypothesize that its interference could be of therapeutic value. Indeed, in vivo treatment of metformin and cDDP was able to partially reverse platinum resistance. Conclusions: Our data strongly reinforce the idea that the development of acquired cDDP resistance in ovarian cancer can bring about a rewiring of tumor metabolism, and that this might be exploited therapeutically. |
| url |
https://doi.org/10.1177/1758835919839543 |
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