Kidney cancer PDOXs reveal patient-specific pro-malignant effects of antiangiogenics and its molecular traits

An open debate in antiangiogenic therapies is about their consequence on tumor invasiveness and metastasis, which is undoubtedly relevant for patients currently treated with antiangiogenics, such as renal cell carcinoma patients. To address, this we developed an extensive series of 27 patient biopsy...

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Detalhes bibliográficos
Autores: Moserle, Lidia, Pons, Roser, Martínez-Lozano, Mar, Jiménez Valerio, Gabriela, Vidal, August, Suárez, Cristina, Trilla Herrera, Enrique, Jiménez, José, de Torres, Inés, Carles, Joan, Senserrich, Jordi, Aguilar, Susana, Palomero, Luis, Amadori, Alberto, Casanovas, Oriol
Formato: artículo
Estado:Versión publicada
Fecha de publicación:2020
País:España
Recursos:Universidad de Barcelona
Repositorio:Dipòsit Digital de la UB
OAI Identifier:oai:diposit.ub.edu:2445/213383
Acesso em linha:https://hdl.handle.net/2445/213383
Access Level:acceso abierto
Palavra-chave:Tumors
Càncer de ronyó
Angiogènesi
Animals
Renal cancer
Neovascularization
Descrição
Resumo:An open debate in antiangiogenic therapies is about their consequence on tumor invasiveness and metastasis, which is undoubtedly relevant for patients currently treated with antiangiogenics, such as renal cell carcinoma patients. To address, this we developed an extensive series of 27 patient biopsy-derived orthotopic xenograft models (Ren-PDOX) that represent inter-patient heterogeneity. In specific tumors, antiangiogenics produced increased invasiveness and metastatic dissemination, while in others aggressiveness remained unchanged. Mechanistically, species-discriminative RNA sequencing identified a tumor cell-specific differential expression profile associated with tumor progression and aggressivity in TCGA RCC patients. Gene filtering using an invasion-annotated patient series pinpointed two candidate genes, of which ALDH1A3 differentiated the pro-invasive subtype of Ren-PDOXs. Validation in an independent series of 15 antiangiogenic-treated patients confirmed that pre-treatment ALDH1A3 can significantly discriminate patients with pro-aggressive response upon treatment. Overall, results confirm that effects of antiangiogenic drugs on tumor invasion and metastasis are heterogeneous and may profoundly affect the natural progression of tumors and promote malignancy. Furthermore, we identify a specific molecular biomarker that could be used to select patients that better benefit from treatment.