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http://documenta.ciemat.es/handle/123456789/4341
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| Título : | CDK4/6 Inhibitor as a Novel Therapeutic Approach for Advanced Bladder Cancer Independently of RB1 Status |
| Autor : | Rubio, Carolina
Martínez-Fernández, Mónica
Segovia, Cristina
Lodewijk, Iris
Suárez-Cabrera, Cristina
Segrelles, Carmen
López-Calderon, Fernando
Munera-Maravilla, Ester
Santos, Mirentxu
Bernardini, Alejandra
García-Escudero, Ramón
Lorz, Corina
Gómez-Rodriguez, Maria José
de Velasco, Guillermo
Otero, Irene
Villacamps, Felipe
Guerrero-Ramos, Felix
Ruiz, Sergio
de la Rosa, Federico
Dominguez-Rodriguez, Sara
Real, Francisco X
Malats, Nuria
Castellano, Daniel
Dueñas, Marta
Paramio, Jesus M |
| Palabras clave : | bladder cancer
FOXM1 |
| Fecha de publicación : | 1-ene-2019 |
| Editorial : | Clinical Cancer Research |
| Citación : | Rubio C, Martínez-Fernández M, Segovia C, Lodewijk I, Suarez-Cabrera C, Segrelles C, López-Calderón F, Munera-Maravilla E, Santos M, Bernardini A, García-Escudero R, Lorz C, Gómez-Rodriguez MJ, de Velasco G, Otero I, Villacampa F, Guerrero-Ramos F, Ruiz S, de la Rosa F, Domínguez-Rodríguez S, Real FX, Malats N, Castellano D, Dueñas M, Paramio JM. CDK4/6 Inhibitor as a Novel Therapeutic Approach for Advanced Bladder Cancer Independently of RB1 Status. Clin Cancer Res. 2019 Jan 1;25(1):390-402. doi: 10.1158/1078-0432.CCR-18-0685. |
| Resumen : | Purpose: Bladder cancer is a clinical and social problem due to its high incidence and recurrence rates. It frequently appears in elderly patients showing other medical comorbidities that hamper the use of standard chemotherapy. We evaluated the activity of CDK4/6 inhibitor as a new therapy for patients unfit for cisplatin (CDDP).
Experimental design: Bladder cancer cell lines were tested for in vitro sensitivity to CDK4/6 inhibition. A novel metastatic bladder cancer mouse model was developed and used to test its in vivo activity.
Results: Cell lines tested were sensitive to CDK4/6 inhibition, independent on RB1 gene status. Transcriptome analyses and knockdown experiments revealed a major role for FOXM1 in this response. CDK4/6 inhibition resulted in reduced FOXM1 phosphorylation in vitro and in vivo and showed synergy with CDDP, allowing a significant tumor regression. FOXM1 exerted important oncogenic roles in bladder cancer.
Conclusions: CDK4/6 inhibitors, alone or in combination, are a novel therapeutic strategy for patients with advanced bladder cancer previously classified as unfit for current treatment options. |
| URI : | http://documenta.ciemat.es/handle/123456789/4341 |
| Aparece en las colecciones: | Artículos de Investigación Básica
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