Metformin produces growth inhibitory effects in combination with nutlin-3a on malignant mesothelioma through a cross-talk between mTOR and p53 pathways
Abstract Background Mesothelioma is resistant to conventional treatments and is often defective in p53 pathways. We then examined anti-tumor effects of metformin, an agent for type 2 diabetes, and combinatory effects of metformin and nutlin-3a, an inhibitor for ubiquitin-mediated p53 degradation, on...
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2017-05-01
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| Series: | BMC Cancer |
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| Online Access: | http://link.springer.com/article/10.1186/s12885-017-3300-y |
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doaj-1792f90d5cf643a889404e840be146bc2020-11-24T21:10:31ZengBMCBMC Cancer1471-24072017-05-0117111410.1186/s12885-017-3300-yMetformin produces growth inhibitory effects in combination with nutlin-3a on malignant mesothelioma through a cross-talk between mTOR and p53 pathwaysKengo Shimazu0Yuji Tada1Takao Morinaga2Masato Shingyoji3Ikuo Sekine4Hideaki Shimada5Kenzo Hiroshima6Takao Namiki7Koichiro Tatsumi8Masatoshi Tagawa9Department of Respirology, Graduate School of Medicine, Chiba UniversityDepartment of Respirology, Graduate School of Medicine, Chiba UniversityDivision of Pathology and Cell Therapy, Chiba Cancer Center Research InstituteDivision of RespirologyDepartment of Medical Oncology, Faculty of Medicine, University of TsukubaDepartment of Surgery, School of Medicine, Toho UniversityDepartment of Pathology, Tokyo Women’s Medical University Yachiyo Medical CenterDepartment of Japanese-Oriental Medicine, Graduate School of Medicine, Chiba UniversityDepartment of Respirology, Graduate School of Medicine, Chiba UniversityDivision of Pathology and Cell Therapy, Chiba Cancer Center Research InstituteAbstract Background Mesothelioma is resistant to conventional treatments and is often defective in p53 pathways. We then examined anti-tumor effects of metformin, an agent for type 2 diabetes, and combinatory effects of metformin and nutlin-3a, an inhibitor for ubiquitin-mediated p53 degradation, on human mesothelioma. Methods We examined the effects with a colorimetric assay and cell cycle analyses, and investigated molecular events in cells treated with metformin and/or nutlin-3a with Western blot analyses. An involvement of p53 was tested with siRNA for p53. Results Metformin suppressed cell growth of 9 kinds of mesothelioma including immortalized cells of mesothelium origin irrespective of the p53 functional status, whereas susceptibility to nutlin-3a was partly dependent on the p53 genotype. We investigated combinatory effects of metformin and nutlin-3a on, nutlin-3a sensitive MSTO-211H and NCI-H28 cells and insensitive EHMES-10 cells, all of which had the wild-type p53 gene. Knockdown of p53 expression with the siRNA demonstrated that susceptibility of MSTO-211H and NCI-H28 cells to nutlin-3a was p53-dependent, whereas that of EHMES-10 cells was not. Nevertheless, all the cells treated with both agents produced additive or synergistic growth inhibitory effects. Cell cycle analyses also showed that the combination increased sub-G1 fractions greater than metformin or nutlin-3a alone in MSTO-211H and EHMES-10 cells. Western blot analyses showed that metformin inhibited downstream pathways of the mammalian target of rapamycin (mTOR) but did not activate the p53 pathways, whereas nutlin-3a phosphorylated p53 and suppressed mTOR pathways. Cleaved caspase-3 and conversion of LC3A/B were also detected but it was dependent on cells and treatments. The combination of both agents in MSTO-211H cells rather suppressed the p53 pathways that were activated by nutrin-3a treatments, whereas the combination rather augmented the p53 actions in NCI-H28 and EHMES-10 cells. Conclusion These data collectively indicated a possible interactions between mTOR and p53 pathways, and the combinatory effects were attributable to differential mechanisms induced by a cross-talk between the pathways.http://link.springer.com/article/10.1186/s12885-017-3300-yMesotheliomaMetforminNutlin-3ap53Mammalian target of rapamycin |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Kengo Shimazu Yuji Tada Takao Morinaga Masato Shingyoji Ikuo Sekine Hideaki Shimada Kenzo Hiroshima Takao Namiki Koichiro Tatsumi Masatoshi Tagawa |
| spellingShingle |
Kengo Shimazu Yuji Tada Takao Morinaga Masato Shingyoji Ikuo Sekine Hideaki Shimada Kenzo Hiroshima Takao Namiki Koichiro Tatsumi Masatoshi Tagawa Metformin produces growth inhibitory effects in combination with nutlin-3a on malignant mesothelioma through a cross-talk between mTOR and p53 pathways BMC Cancer Mesothelioma Metformin Nutlin-3a p53 Mammalian target of rapamycin |
| author_facet |
Kengo Shimazu Yuji Tada Takao Morinaga Masato Shingyoji Ikuo Sekine Hideaki Shimada Kenzo Hiroshima Takao Namiki Koichiro Tatsumi Masatoshi Tagawa |
| author_sort |
Kengo Shimazu |
| title |
Metformin produces growth inhibitory effects in combination with nutlin-3a on malignant mesothelioma through a cross-talk between mTOR and p53 pathways |
| title_short |
Metformin produces growth inhibitory effects in combination with nutlin-3a on malignant mesothelioma through a cross-talk between mTOR and p53 pathways |
| title_full |
Metformin produces growth inhibitory effects in combination with nutlin-3a on malignant mesothelioma through a cross-talk between mTOR and p53 pathways |
| title_fullStr |
Metformin produces growth inhibitory effects in combination with nutlin-3a on malignant mesothelioma through a cross-talk between mTOR and p53 pathways |
| title_full_unstemmed |
Metformin produces growth inhibitory effects in combination with nutlin-3a on malignant mesothelioma through a cross-talk between mTOR and p53 pathways |
| title_sort |
metformin produces growth inhibitory effects in combination with nutlin-3a on malignant mesothelioma through a cross-talk between mtor and p53 pathways |
| publisher |
BMC |
| series |
BMC Cancer |
| issn |
1471-2407 |
| publishDate |
2017-05-01 |
| description |
Abstract Background Mesothelioma is resistant to conventional treatments and is often defective in p53 pathways. We then examined anti-tumor effects of metformin, an agent for type 2 diabetes, and combinatory effects of metformin and nutlin-3a, an inhibitor for ubiquitin-mediated p53 degradation, on human mesothelioma. Methods We examined the effects with a colorimetric assay and cell cycle analyses, and investigated molecular events in cells treated with metformin and/or nutlin-3a with Western blot analyses. An involvement of p53 was tested with siRNA for p53. Results Metformin suppressed cell growth of 9 kinds of mesothelioma including immortalized cells of mesothelium origin irrespective of the p53 functional status, whereas susceptibility to nutlin-3a was partly dependent on the p53 genotype. We investigated combinatory effects of metformin and nutlin-3a on, nutlin-3a sensitive MSTO-211H and NCI-H28 cells and insensitive EHMES-10 cells, all of which had the wild-type p53 gene. Knockdown of p53 expression with the siRNA demonstrated that susceptibility of MSTO-211H and NCI-H28 cells to nutlin-3a was p53-dependent, whereas that of EHMES-10 cells was not. Nevertheless, all the cells treated with both agents produced additive or synergistic growth inhibitory effects. Cell cycle analyses also showed that the combination increased sub-G1 fractions greater than metformin or nutlin-3a alone in MSTO-211H and EHMES-10 cells. Western blot analyses showed that metformin inhibited downstream pathways of the mammalian target of rapamycin (mTOR) but did not activate the p53 pathways, whereas nutlin-3a phosphorylated p53 and suppressed mTOR pathways. Cleaved caspase-3 and conversion of LC3A/B were also detected but it was dependent on cells and treatments. The combination of both agents in MSTO-211H cells rather suppressed the p53 pathways that were activated by nutrin-3a treatments, whereas the combination rather augmented the p53 actions in NCI-H28 and EHMES-10 cells. Conclusion These data collectively indicated a possible interactions between mTOR and p53 pathways, and the combinatory effects were attributable to differential mechanisms induced by a cross-talk between the pathways. |
| topic |
Mesothelioma Metformin Nutlin-3a p53 Mammalian target of rapamycin |
| url |
http://link.springer.com/article/10.1186/s12885-017-3300-y |
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