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Bertran Alamillo, Jordi  
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Giménez Capitán, Ana  
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Román, Ruth  
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Talbot, Sara  
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Whiteley, Rebecca  
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Floch, Nicolas  
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Martinez Perez, Elizabeth  
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Martin, Matthew J.  
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Smith, Paul D.  
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Sullivan, Ivana  
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Terp, Mikkel G.  
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Saeh, Jamal  
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Marino Buslje, Cristina  
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Fabbri, Giulia  
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Guo, Grace  
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Xu, Man  
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Tornador, Cristian  
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Aguilar Hernández, Andrés  
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Reguart, Noemí  
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Ditzel, Henrik J.  
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Martínez Bueno, Alejandro  
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Nabau Moretó, Núria  
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Gascó, Amaya  
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Rosell, Rafael  
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Pease, J. Elizabeth  
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Polanska, Urszula M.  
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Travers, Jon  
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Urosevic, Jelena  
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Molina Vila, Miguel A.  
dc.date.available
2024-03-12T09:46:34Z  
dc.date.issued
2023-12  
dc.identifier.citation
Bertran Alamillo, Jordi; Giménez Capitán, Ana; Román, Ruth; Talbot, Sara; Whiteley, Rebecca; et al.; BID expression determines the apoptotic fate of cancer cells after abrogation of the spindle assembly checkpoint by AURKB or TTK inhibitors; BioMed Central; Molecular Cancer; 22; 1; 12-2023; 1-24  
dc.identifier.issn
1476-4598  
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http://hdl.handle.net/11336/230099  
dc.description.abstract
Background: Drugs targeting the spindle assembly checkpoint (SAC), such as inhibitors of Aurora kinase B (AURKB) and dual specific protein kinase TTK, are in different stages of clinical development. However, cell response to SAC abrogation is poorly understood and there are no markers for patient selection. Methods: A panel of 53 tumor cell lines of different origins was used. The effects of drugs were analyzed by MTT and flow cytometry. Copy number status was determined by FISH and Q-PCR; mRNA expression by nCounter and RT-Q-PCR and protein expression by Western blotting. CRISPR-Cas9 technology was used for gene knock-out (KO) and a doxycycline-inducible pTRIPZ vector for ectopic expression. Finally, in vivo experiments were performed by implanting cultured cells or fragments of tumors into immunodeficient mice. Results: Tumor cells and patient-derived xenografts (PDXs) sensitive to AURKB and TTK inhibitors consistently showed high expression levels of BH3-interacting domain death agonist (BID), while cell lines and PDXs with low BID were uniformly resistant. Gene silencing rendered BID-overexpressing cells insensitive to SAC abrogation while ectopic BID expression in BID-low cells significantly increased sensitivity. SAC abrogation induced activation of CASP-2, leading to cleavage of CASP-3 and extensive cell death only in presence of high levels of BID. Finally, a prevalence study revealed high BID mRNA in 6% of human solid tumors. Conclusions: The fate of tumor cells after SAC abrogation is driven by an AURKB/ CASP-2 signaling mechanism, regulated by BID levels. Our results pave the way to clinically explore SAC-targeting drugs in tumors with high BID expression.  
dc.format
application/pdf  
dc.language.iso
eng  
dc.publisher
BioMed Central  
dc.rights
info:eu-repo/semantics/openAccess  
dc.rights.uri
https://creativecommons.org/licenses/by-nc-sa/2.5/ar/  
dc.subject
ABROGATION  
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AURKB INHIBITOR  
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BID  
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BIOMARKER  
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CASP-2  
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CELL CYCLE  
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SPINDLE ASSEMBLY CHECKPOINT (SAC)  
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TTK INHIBITOR  
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TUMOR  
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Bioquímica y Biología Molecular  
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Ciencias Biológicas  
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CIENCIAS NATURALES Y EXACTAS  
dc.title
BID expression determines the apoptotic fate of cancer cells after abrogation of the spindle assembly checkpoint by AURKB or TTK inhibitors  
dc.type
info:eu-repo/semantics/article  
dc.type
info:ar-repo/semantics/artículo  
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info:eu-repo/semantics/publishedVersion  
dc.date.updated
2024-02-28T10:15:30Z  
dc.journal.volume
22  
dc.journal.number
1  
dc.journal.pagination
1-24  
dc.journal.pais
Reino Unido  
dc.journal.ciudad
Londres  
dc.description.fil
Fil: Bertran Alamillo, Jordi. Quiron Dexeus University Hospital; España  
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Fil: Giménez Capitán, Ana. Quiron Dexeus University Hospital; España  
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Fil: Román, Ruth. Quiron Dexeus University Hospital; España  
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Fil: Talbot, Sara. Quiron Dexeus University Hospital; España  
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Fil: Whiteley, Rebecca. Quiron Dexeus University Hospital; España  
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Fil: Floch, Nicolas. Astrazeneca; Reino Unido  
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Fil: Martinez Perez, Elizabeth. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Parque Centenario. Instituto de Investigaciones Bioquímicas de Buenos Aires. Fundación Instituto Leloir. Instituto de Investigaciones Bioquímicas de Buenos Aires; Argentina  
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Fil: Martin, Matthew J.. Astrazeneca; Reino Unido  
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Fil: Smith, Paul D.. Astrazeneca; Reino Unido  
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Fil: Sullivan, Ivana. Hospital de la Santa Creu I Sant Pau; España. Hospital Universitari Dexeus; España  
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Fil: Terp, Mikkel G.. University of Southern Denmark; Dinamarca  
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Fil: Saeh, Jamal. Astrazeneca; Reino Unido  
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Fil: Marino Buslje, Cristina. Fundación Instituto Leloir; Argentina  
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Fil: Fabbri, Giulia. Astrazeneca; Reino Unido  
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Fil: Guo, Grace. Astrazeneca; Reino Unido  
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Fil: Xu, Man. Astrazeneca; Reino Unido  
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Fil: Tornador, Cristian. Teresa Moretó Foundation And Wholegenix Sl; España  
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Fil: Aguilar Hernández, Andrés. Hospital Universitari Dexeus; España  
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Fil: Reguart, Noemí. Hospital Clinic Barcelona; España  
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Fil: Ditzel, Henrik J.. University of Southern Denmark,; Dinamarca. Odense University Hospital; Dinamarca  
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Fil: Martínez Bueno, Alejandro. Hospital Universitari Dexeus; España  
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Fil: Nabau Moretó, Núria. Teresa Moretó Foundation And Wholegenix Sl; España  
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Fil: Gascó, Amaya. Astrazeneca; Reino Unido  
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Fil: Rosell, Rafael. Germans Trias I Pujol Research Institute; España. Hospital Universitari Dexeus; España  
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Fil: Pease, J. Elizabeth. Astrazeneca; Reino Unido  
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Fil: Polanska, Urszula M.. Astrazeneca; Reino Unido  
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Fil: Travers, Jon. Astrazeneca; Reino Unido  
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Fil: Urosevic, Jelena. Astrazeneca; Reino Unido  
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Fil: Molina Vila, Miguel A.. Hospital Universitari Dexeus; España  
dc.journal.title
Molecular Cancer  
dc.relation.alternativeid
info:eu-repo/semantics/altIdentifier/doi/http://dx.doi.org/10.1186/s12943-023-01815-w  
dc.relation.alternativeid
info:eu-repo/semantics/altIdentifier/url/https://molecular-cancer.biomedcentral.com/articles/10.1186/s12943-023-01815-w  

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