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14 results on '"Álvaro Curiel-García"'

1. Somatic genome editing with the RCAS-TVA-CRISPR-Cas9 system for precision tumor modeling

Author

Barbara Oldrini, Álvaro Curiel-García, Carolina Marques, Veronica Matia, Özge Uluçkan, Osvaldo Graña-Castro, Raul Torres-Ruiz, Sandra Rodriguez-Perales, Jason T. Huse, and Massimo Squatrito

Subjects
Science
Abstract

Accurate recapitulation of human disease in animal models requires generation of complex and heterogeneous genetic variation. Here the authors combine RCAS-TVA with CRISPR-Cas9 to generate mouse models of cancer.

Published
2018
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2. Data from Dianhydrogalactitol Overcomes Multiple Temozolomide Resistance Mechanisms in Glioblastoma

Author

Massimo Squatrito, Fátima Al-Shahrour, Scott W. Lowe, Lucía Zhu, Marcos Galán-Ganga, Alberto J. Schuhmacher, Javier Perales-Patón, Paula Nogales, Álvaro Curiel-García, and Miguel Jiménez-Alcázar

Abstract

Glioblastoma (GBM) is the most frequent and aggressive primary tumor type in the central nervous system in adults. Resistance to chemotherapy remains one of the major obstacles in GBM treatment. Identifying and overcoming the mechanisms of therapy resistance is instrumental to develop novel therapeutic approaches for patients with GBM. To determine the major drivers of temozolomide (TMZ) sensitivity, we performed shRNA screenings in GBM lines with different O6-methylguanine-DNA methyl-transferase (MGMT) status. We then evaluated dianhydrogalactitol (Val-083), a small alkylating molecule that induces interstrand DNA crosslinking, as a potential treatment to bypass TMZ-resistance mechanisms. We found that loss of mismatch repair (MMR) components and MGMT expression are mutually exclusive mechanisms driving TMZ resistance in vitro. Treatment of established GBM cells and tumorsphere lines with Val-083 induces DNA damage and cell-cycle arrest in G2–M phase, independently of MGMT or MMR status, thus circumventing conventional resistance mechanisms to TMZ. Combination of TMZ and Val-083 shows a synergic cytotoxic effect in tumor cells in vitro, ex vivo, and in vivo. We propose this combinatorial treatment as a potential approach for patients with GBM.

Published
2023
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5. Pharmacological targeting of the receptor ALK inhibits tumorigenicity and overcomes chemoresistance in pancreatic ductal adenocarcinoma

Author

Beatriz Parejo-Alonso, Alba Royo-García, Pilar Espiau-Romera, Sarah Courtois, Álvaro Curiel-García, Sladjana Zagorac, Isabel Villaoslada, Kenneth P. Olive, Christopher Heeschen, and Patricia Sancho

Subjects
Pharmacology, General Medicine
Abstract

Pancreatic ductal adenocarcinoma (PDAC) is an extremely aggressive disease characterized by its metastatic potential and chemoresistance. These traits are partially attributable to the highly tumorigenic pancreatic cancer stem cells (PaCSCs). Interestingly, these cells show unique features in order to sustain their identity and functionality, some of them amenable for therapeutic intervention. Screening of phospho-receptor tyrosine kinases revealed that PaCSCs harbored increased activation of anaplastic lymphoma kinase (ALK). We subsequently demonstrated that oncogenic ALK signaling contributes to tumorigenicity in PDAC patient-derived xenografts (PDXs) by promoting stemness through ligand-dependent activation. Indeed, the ALK ligands midkine (MDK) or pleiotrophin (PTN) increased self-renewal, clonogenicity and CSC frequency in several in vitro local and metastatic PDX models. Conversely, treatment with the clinically-approved ALK inhibitors Crizotinib and Ensartinib decreased PaCSC content and functionality in vitro and in vivo, by inducing cell death. Strikingly, ALK inhibitors sensitized chemoresistant PaCSCs to Gemcitabine, as the most used chemotherapeutic agent for PDAC treatment. Consequently, ALK inhibition delayed tumor relapse after chemotherapy in vivo by effectively decreasing the content of PaCSCs. In summary, our results demonstrate that targeting the MDK/PTN-ALK axis with clinically-approved inhibitors impairs in vivo tumorigenicity and chemoresistance in PDAC suggesting a new treatment approach to improve the long-term survival of PDAC patients.

Published
2022

6. ALK signaling drives tumorigenicity and chemoresistance of pancreatic ductal adenocarcinoma cells

Author

Beatriz Parejo-Alonso, Alba Royo-García, Pilar Espiau-Romera, Sarah Courtois, Álvaro Curiel-García, Sladjana Zagorac, Isabel Villaoslada, Kenneth P. Olive, Christopher Heeschen, and Patricia Sancho

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is an extremely aggressive disease characterized by its metastatic potential and chemoresistance. These traits are partially attributable to the highly tumorigenic pancreatic cancer stem cells (PaCSCs). Interestingly, these cells show unique features in order to sustain their identity and functionality, some of them amenable for therapeutic intervention. Screening of phospho-receptor tyrosine kinases revealed that PaCSCs harbored increased activation of anaplastic lymphoma kinase (ALK). We subsequently demonstrated that oncogenic ALK signaling drives tumorigenicity in PDAC patient-derived xenografts (PDXs) by promoting stemness through ligand-dependent activation. Indeed, the ALK ligands midkine (MDK) or pleiotrophin (PTN) increased self-renewal, clonogenicity and CSC frequency in several in vitro local and metastatic PDX models. Conversely, treatment with the clinically-approved ALK inhibitors Crizotinib and Ensartinib decreased CSC content and functionality in vitro and in vivo, by inducing cell death. Strikingly, ALK inhibitors sensitized chemoresistant PaCSCs to Gemcitabine, as the most used chemotherapeutic agent for PDAC treatment. Consequently, ALK inhibition delayed tumor relapse after chemotherapy in vivo by effectively decreasing the content of PaCSCs. In summary, our results demonstrate that targeting the MDK/PTN-ALK axis with clinically-approved inhibitors impairs in vivo tumorigenicity and chemoresistance in PDAC suggesting a new treatment approach to improve the long-term survival of PDAC patients.GRAPHICAL ABSTRACT

Published
2022
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7. Dianhydrogalactitol Overcomes Multiple Temozolomide Resistance Mechanisms in Glioblastoma

Author

Marcos Galán-Ganga, Alberto J. Schuhmacher, Paula Nogales, Fatima Al-Shahrour, Miguel Jiménez-Alcázar, Lucía Zhu, Javier Perales-Patón, Scott W. Lowe, Álvaro Curiel-García, and Massimo Squatrito

Subjects
0301 basic medicine, Cancer Research, DNA damage, medicine.medical_treatment, Transfection, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, In vivo, Cell Line, Tumor, Temozolomide, medicine, Animals, Humans, Dianhydrogalactitol, Chemotherapy, business.industry, medicine.disease, Xenograft Model Antitumor Assays, Primary tumor, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, DNA mismatch repair, Glioblastoma, business, Ex vivo, medicine.drug
Abstract

Glioblastoma (GBM) is the most frequent and aggressive primary tumor type in the central nervous system in adults. Resistance to chemotherapy remains one of the major obstacles in GBM treatment. Identifying and overcoming the mechanisms of therapy resistance is instrumental to develop novel therapeutic approaches for patients with GBM. To determine the major drivers of temozolomide (TMZ) sensitivity, we performed shRNA screenings in GBM lines with different O6-methylguanine-DNA methyl-transferase (MGMT) status. We then evaluated dianhydrogalactitol (Val-083), a small alkylating molecule that induces interstrand DNA crosslinking, as a potential treatment to bypass TMZ-resistance mechanisms. We found that loss of mismatch repair (MMR) components and MGMT expression are mutually exclusive mechanisms driving TMZ resistance in vitro. Treatment of established GBM cells and tumorsphere lines with Val-083 induces DNA damage and cell-cycle arrest in G2–M phase, independently of MGMT or MMR status, thus circumventing conventional resistance mechanisms to TMZ. Combination of TMZ and Val-083 shows a synergic cytotoxic effect in tumor cells in vitro, ex vivo, and in vivo. We propose this combinatorial treatment as a potential approach for patients with GBM.

Published
2021
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8. Modeling Pancreatic Cancer through Somatic Editing with AAV

Author

Kenneth P. Olive and Álvaro Curiel-García

Subjects
0301 basic medicine, Somatic cell, Genetic Vectors, Virus, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Pancreatic cancer, medicine, Biomarkers, Tumor, CRISPR, Animals, Humans, Genetic Predisposition to Disease, Molecular Biology, Genetic Association Studies, Gene Editing, business.industry, Cancer, Dependovirus, medicine.disease, Pancreatic Neoplasms, 030104 developmental biology, medicine.anatomical_structure, chemistry, Genetically Engineered Mouse, Cancer research, Molecular Medicine, Pancreas, business, Penetrant (biochemical), 030217 neurology & neurosurgery, Carcinoma, Pancreatic Ductal
Abstract

Genetically engineered mouse models have revolutionized the study of pancreatic cancer, but have several technical and practical limitations. A new adeno-associated virus (AAV)-driven somatic genome-editing model of pancreatic ductal adenocarcinoma reported by Ideno et al. (Lab. Invest. published online February 6, 2019; https://doi.org/10.1038/s41374-018-0171-z) addresses several of these limitations, achieving rapid and penetrant induction of multiple targeted alterations in the adult murine pancreas.

Published
2019

9. EGFR feedback-inhibition by Ran-binding protein 6 is disrupted in cancer

Author

Ingo K. Mellinghoff, Craig M. Bielski, Maryam Pourmaleki, Paolo Codega, Maria Stella Carro, Massimo Squatrito, Barry S. Taylor, Álvaro Curiel-García, Paul Tempst, Daniel Rohle, John Blenis, Travis J. Hollmann, Barbara Oldrini, Igor Vivanco, Carl Campos, Hediye Erdjument-Bromage, Wan-Ying Hsieh, Marc K. Rosenblum, Christian Grommes, National Institutes of Health (Estados Unidos), Geoffrey Beene Foundation, Fundación Seve Ballesteros, and Memorial Sloan Kettering Cancer Center

Subjects
STAT3 Transcription Factor, 0301 basic medicine, Science, Active Transport, Cell Nucleus, General Physics and Astronomy, Mice, SCID, Importin, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Cell Line, Tumor, medicine, Animals, Humans, Gene silencing, Epidermal growth factor receptor, lcsh:Science, STAT3, Cells, Cultured, Feedback, Physiological, Mice, Knockout, Antibiotics, Antineoplastic, Multidisciplinary, biology, Chemistry, Glioma, General Chemistry, beta Karyopherins, Xenograft Model Antitumor Assays, 3. Good health, Cell biology, ErbB Receptors, Gene Expression Regulation, Neoplastic, HEK293 Cells, ran GTP-Binding Protein, 030104 developmental biology, Doxorubicin, Gene Knockdown Techniques, biology.protein, STAT protein, lcsh:Q, Female, Beta Karyopherins, Nuclear transport, Carcinogenesis
Abstract

Transport of macromolecules through the nuclear pore by importins and exportins plays a critical role in the spatial regulation of protein activity. How cancer cells co-opt this process to promote tumorigenesis remains unclear. The epidermal growth factor receptor (EGFR) plays a critical role in normal development and in human cancer. Here we describe a mechanism of EGFR regulation through the importin β family member RAN-binding protein 6 (RanBP6), a protein of hitherto unknown functions. We show that RanBP6 silencing impairs nuclear translocation of signal transducer and activator of transcription 3 (STAT3), reduces STAT3 binding to the EGFR promoter, results in transcriptional derepression of EGFR, and increased EGFR pathway output. Focal deletions of the RanBP6 locus on chromosome 9p were found in a subset of glioblastoma (GBM) and silencing of RanBP6 promoted glioma growth in vivo. Our results provide an example of EGFR deregulation in cancer through silencing of components of the nuclear import pathway., The epidermal growth factor receptor (EGFR) signalling is regulated at multiple levels. Here the authors show that the importin RanBP6 acts as a tumor suppressor in Glioblastoma and regulates EGFR signalling through promoting translocation of STAT3 to the nuclei and repressing EGFR transcription.

Published
2017
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10. Somatic genome editing with the RCAS/TVA-CRISPR/Cas9 system for precision tumor modeling

Author

Álvaro Curiel-García, Carolina Marques, Veronica Matia, Barbara Oldrini, Sandra Rodriguez-Perales, Özge Uluçkan, Massimo Squatrito, Jason T. Huse, and Raúl Torres-Ruiz

Subjects
Homology directed repair, Genetics, Mutation, Genome editing, Cas9, CDKN2A, Somatic cell, medicine, CRISPR, Biology, medicine.disease_cause, Chromosomal Deletion
Abstract

It has been gradually established that the vast majority of human tumors are extraordinarily heterogeneous at a genetic level. To accurately recapitulate this complexity, it is now evident that in vivo animal models of cancers will require to recreate not just a handful of simple genetic alterations, but possibly dozens and increasingly intricate. Here, we have combined the RCAS/TVA system with the CRISPR/Cas9 genome editing tools for precise modeling of human tumors. We show that somatic deletion in neural stem cells (NSCs) of a variety of known tumor suppressor genes (Trp53, Cdkn2a and Pten), in combination with the expression of an oncogene driver, leads to high-grade glioma formation. Moreover, by simultaneous delivery of pairs of guide RNAs (gRNAs) we generated different gene fusions, either by chromosomal deletion (Bcan-Ntrk1) or by chromosomal translocation (Myb-Qk), and we show that they have transforming potential in vitro and in vivo. Lastly, using homology-directed-repair (HDR), we also produced tumors carrying the Braf V600E mutation, frequently identified in a variety of subtypes of gliomas. In summary, we have developed an extremely powerful and versatile mouse model for in vivo somatic genome editing, that will elicit the generation of more accurate cancer models particularly appropriate for pre-clinical testing.

Published
2017
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11. DRES-12. FUNCTIONAL GENETIC APPROACHES TO OVERCOME TEMOZOLOMIDE RESISTANCE IN GLIOBLASTOMA

Author

Fatima Al-Shahrour, Álvaro Curiel-García, Javier Perales-Patón, Alberto Jimenez-Schuhmacher, Paula Nogales-Gomez, and Massimo Squatrito

Subjects
Abstracts, Cancer Research, Temozolomide, Oncology, medicine, O-6-methylguanine-DNA methyltransferase, Tumor cells, Neurology (clinical), Computational biology, Biology, medicine.disease, Glioblastoma, medicine.drug
Abstract

Glioblastoma (GBM), the highest grade of malignant astrocytomas, is the most common and lethal primary central nervous system tumour in the adults. Despite the recent advances in treatment modalities, GBM patients generally respond poorly to all therapeutic approaches and prognosis remain dismal. Radiation and chemo-resistance are characteristic of various cancer types, however it is not clear if this therapy resistance is a consequence of tumour progression or it is intrinsically associated with the genetic events that lead to the tumour formation in the first place. Gaining insights into the pathways that determine this poor treatment response will be instrumental for the development of new therapeutic modalities. Alterations of the DNA damage response (DDR) have been associated with therapy resistance, offering both challenges and opportunities from a treatment prospective. Currently, a number of laboratories are exploring the possibility of manipulating the DDR to cause selective tumour cell death through mitotic catastrophe. In order to identify genes that modulate temozolomide (TMZ) response we have performed a series of in vitro shRNA screenings, using a customized sRNA library against DDR genes and several GBM cell lines with various genetic makeup (e.g.: MGMT+, MGMT-, MMR-proficient and MMR-deficient). Our studies allowed to pinpoint both positive and negative regulators of TMZ sensitivity. Novel approaches to overcome TMZ resistance will be presented.

Published
2018
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12. Functional classification of BRCA2 DNA variants by splicing assays in a large minigene with 9 exons

Author

Alberto Acedo, Álvaro Curiel-García, Beatriz Díez-Gómez, Cristina Hernández-Moro, Eladio Velasco, Ministerio de Economía y Competitividad (España), European Commission, Junta de Castilla y León, Fundación Villalar, and Instituto de Salud Carlos III

Subjects
Hereditary breast and ovarian cancer, Exonic splicing enhancer, ComputingMilieux_LEGALASPECTSOFCOMPUTING, Biology, Splicing, Exon, Genetics, Humans, Protein Isoforms, Vector (molecular biology), Unclassified variants, Gene, Genetics (clinical), Genetic Association Studies, Research Articles, BRCA2 Protein, Alternative splicing, Minigenes, RNA, Exons, BRCA2, Alternative Splicing, RNA splicing, MCF-7 Cells, Hereditary Breast and Ovarian Cancer Syndrome, Minigene, HeLa Cells
Abstract

This is an open access article under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs License., Numerous pathogenic DNA variants impair the splicing mechanism in human genetic diseases. Minigenes are optimal approaches to test variants under the splicing viewpoint without the need of patient samples. We aimed to design a robust minigene construct of the breast cancer gene BRCA2 in order to investigate the impact of variants on splicing. BRCA2 exons 19 to 27 (MGBR2_ex19–27) were cloned in the new vector pSAD. It produced a large transcript of the expected size (2174 nucleotides) and exon structure (V1-ex19-27-V2). Splicing assays showed that 18 (17 splice-site and 1 silencer variants) out of 40 candidate DNA variants induced aberrant patterns. Twenty-four anomalous transcripts were accurately detected by fluorescent-RT-PCR that were generated by exon-skipping, alternative site usage and intron-retention events. Fourteen variants induced major anomalies and were predicted to disrupt protein function so they could be classified as pathogenic. Furthermore, minigene mimicked previously reported patient RNA outcomes of seven variants supporting the reproducibility of minigene assays. Therefore, a relevant fraction of variants are involved in breast cancer through splicing alterations. MGBR2_ex19–27 is the largest reported BRCA2 minigene and constitutes a valuable tool for the functional and clinical classification of sequence variations., Contract grant sponsors: Instituto de Salud Carlos III (Spanish Ministry of Economy and Competitiveness) grants PI10/2910 and PI13/1749, Consejería de Sanidad (Junta de Castilla y León) grant BIO/VA08/13. AA was supported by the European Social Fund and Consejeria de Educación de la Junta de Castilla y León under the P.O. Castilla y León 2007–2013. CHM is supported by Fundación Villalar (Castilla y León, Spain).

Published
2014

13. Generation of orthotopic patient-derived xenograft models for pancreatic cancer using tumor slices

Author

Alvaro Curiel-Garcia, Amanda R. Decker-Farrell, Stephen A. Sastra, and Kenneth P. Olive

Subjects
Cancer, Model Organisms, Science (General), Q1-390
Abstract

Summary: Orthotopic patient-derived xenograft models recapitulate the genomic complexity of the original tumor and some aspects of local microenvironment, useful for rapid development and validation of personalized treatment strategies. Here, we precisely describe a protocol for generating tumor slices from human or murine-derived pancreatic cancer. They are then implanted directly into the murine pancreas, monitored using ultrasound, with a 90% success rate. This assay creates a clinically relevant in vivo model facilitating personalized treatment development. : Publisher’s note: Undertaking any experimental protocol requires adherence to local institutional guidelines for laboratory safety and ethics.

Published
2022
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14. EGFR feedback-inhibition by Ran-binding protein 6 is disrupted in cancer

Author

Barbara Oldrini, Wan-Ying Hsieh, Hediye Erdjument-Bromage, Paolo Codega, Maria Stella Carro, Alvaro Curiel-García, Carl Campos, Maryam Pourmaleki, Christian Grommes, Igor Vivanco, Daniel Rohle, Craig M. Bielski, Barry S. Taylor, Travis J. Hollmann, Marc Rosenblum, Paul Tempst, John Blenis, Massimo Squatrito, and Ingo K. Mellinghoff

Subjects
Science
Abstract

The epidermal growth factor receptor (EGFR) signalling is regulated at multiple levels. Here the authors show that the importin RanBP6 acts as a tumor suppressor in Glioblastoma and regulates EGFR signalling through promoting translocation of STAT3 to the nuclei and repressing EGFR transcription.

Published
2017
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