Your search keyword '"Eduardo Quiroga"' showing total 5 results

1. IMMU-13. Dual CTLA4/ PD-1 blockade improves survival for replication-repair deficient high-grade gliomas failing single agent PD-1 inhibition: An IRRDC study

Author

Das, Anirban, primary, Morgenstern, Daniel, additional, Bianchi, Vanessa, additional, Sudhaman, Sumedha, additional, Edwards, Melissa, additional, Stengs, Lucie, additional, Larouche, Valerie, additional, Samuel, David, additional, Van Damme, An, additional, Gass, David, additional, Ziegler, David, additional, Bielack, Stefan, additional, Zelcer, Shayna, additional, Yalon, Michal, additional, Constantini, Shlomi, additional, Sarosiek, Tomasz, additional, Libionka, Witold, additional, Nichols, Kim, additional, De Mola, Rebecca Loret, additional, Bielamowicz, Kevin, additional, Sabel, Magnus, additional, Frojd, Charlotta, additional, Wood, Matthew D, additional, Migueis, Joana Cristiano Sous, additional, Abongwa, Chenue, additional, Yen, Lee Yi, additional, Stearns, Duncan, additional, Opocher, Enrico, additional, Bhatia, Kanika, additional, Sen, Santanu, additional, Cantero, Eduardo Quiroga, additional, Paez, Palma Solano, additional, Crooks, Bruce, additional, Magimairajan, Vanan, additional, Reddy, Alyssa, additional, Adamski, Jenny, additional, Mason, Gary, additional, Lindhorst, Scott, additional, Aronson, Melyssa, additional, Ertl-Wagner, Birgit, additional, Hawkins, Cynthia, additional, Bouffet, Eric, additional, and Tabori, Uri, additional

Published

2022

2. IMMU-13. Dual CTLA4/ PD-1 blockade improves survival for replication-repair deficient high-grade gliomas failing single agent PD-1 inhibition: An IRRDC study

Author

Anirban Das, Daniel Morgenstern, Vanessa Bianchi, Sumedha Sudhaman, Melissa Edwards, Lucie Stengs, Valerie Larouche, David Samuel, An Van Damme, David Gass, David Ziegler, Stefan Bielack, Shayna Zelcer, Michal Yalon, Shlomi Constantini, Tomasz Sarosiek, Witold Libionka, Kim Nichols, Rebecca Loret De Mola, Kevin Bielamowicz, Magnus Sabel, Charlotta Frojd, Matthew D Wood, Joana Cristiano Sous Migueis, Chenue Abongwa, Lee Yi Yen, Duncan Stearns, Enrico Opocher, Kanika Bhatia, Santanu Sen, Eduardo Quiroga Cantero, Palma Solano Paez, Bruce Crooks, Vanan Magimairajan, Alyssa Reddy, Jenny Adamski, Gary Mason, Scott Lindhorst, Melyssa Aronson, Birgit Ertl-Wagner, Cynthia Hawkins, Eric Bouffet, and Uri Tabori

Subjects

Cancer Research, Oncology, Neurology (clinical)

Abstract

BACKGROUND: High-grade gliomas (HGG) with replication-repair deficiency (RRD) harbour high mutation burden (TMB) and are rapidly fatal following chemo-radiation approaches. Although hypermutation results in objective responses and prolonged survival in >30% of patients undergoing PD1-blockade, salvage following failure of PD1-inhibition remains a challenge. METHODS: We performed a real-world study of Ipilimumab (anti-CTLA4) in combination with Nivolumab/Pembrolizumab for patients failing single-agent PD1-inhibition. RESULTS: Among 68 consortium patients with relapsed HGG treated with single-agent PD1-inhibitors, progression was observed in 43 (63%). Ipilimumab was added to 20/43 (46.5%), 14 (32.5%) received best supportive care (BSC), and 9 (21%) received miscellaneous therapies. For patients receiving CTLA4/PD1-inhibition, median age at progression was 12.3-years (IQR: 9; 15.6). Time from anti-PD1 initiation to progression was 8-months (IQR: 3.8; 18.5). Germline predisposition was observed in all patients (CMMRD: 70%, Lynch: 25%, polymerase-proofreading deficiency: 5%). All HGG were hypermutant (median TMB: 182 mutations/Mb; IQR: 15.6; 369.4). Centralized radiology review revealed objective responses in 3/20 (15%, all ultra-hypermutant: 320, 496, 834 mutations/Mb), stable disease in 5 (25%), and 12 (60%) eventually progressed (iRANO). Following failure of PD1-blockade, estimated progression-free and overall survival at 18-months for patients receiving CTLA4/PD1-inhibition were 11% and 25%, respectively. Importantly, survival was superior to patients receiving BSC (median OS 1-year on the anti-CTLA4/PD1combination (range:1-48 months). The combinational immunotherapy resulted in significant autoimmune toxicity in 11/20 (55%), warranting immunosuppressive therapy in all, and treatment abandonment in 6 patients. CONCLUSION: Combined CTLA4/PD1-blockade after failure of single-agent PD1-inhibition revealed objective responses and prolonged survival in an otherwise rapidly-fatal disease. This needs to be assessed in the context of significant autoimmunity, supporting the need for the current prospective trial (NCT04500548), and novel strategies to limit treatment-related toxicity.

Published

2022

3. LGG-55. OUTCOME OF BRAF V600E PEDIATRIC GLIOMAS TREATED WITH TARGETED BRAF INHIBITION

Author

Ofelia Cruz, Mariana Fernandes, B. Wilson, Abhishek Bavle, Daniel Alderete, Michael D. Taylor, Olaf Witt, Gurcharanjeet Kaur, Jordan R. Hansford, Scott Ryall, Till Milde, Andres Morales La Madrid, Sarah Leary, Zdenek Pavelka, David Sumerauer, Anne Grete Bechensteen, Inga Harting, Liana Nobre, Michal Zapotocky, Eric Bouffet, Jaroslav Sterba, Daniel R. Boue, Jack Su, Scott L. Coven, Maria Luisa Garrè, Matthias A. Karajannis, Helen Toledano, Naureen Mushtaq, Ute Bartels, Sarah Injac, Cecile Faure Conter, Samantha Mascelli, Frank van Landeghem, Annie Huang, Peter Hauser, Derek S Tsang, Helena Mörse, Martin Kyncl, Normad Laperriere, Elizabeth Finch, James T. Rutka, Cornelis M. van Tilburg, Roger J. Packer, Uri Tabori, Julia Balaguer Guill, Magnus Sabel, Jonathan L. Finlay, Peter B. Dirks, Sonika Dahiya, Cynthia Hawkins, Lorena V Baroni, Lili-Naz Hazrati, Eduardo Quiroga-Cantero, Diana S Osorio, Murali Chintagumpala, Palma Solano, Josef Zamecbik, Tara McKeown, Ira J. Dunkel, Alvaro Lassaletta, Julie Bennet, David D. Eisenstat, Valerie Larouche, Karen Gauvain, Lenka Krskova, Duarte Salgado, Vijay Ramaswamy, Giovanni Morana, Frank Lin, Didier Frappaz, Miriam Bornhorst, Adela Cañete, and Valentina Iurilli

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, business.industry, medicine.medical_treatment, Low Grade Glioma, medicine.disease, Chemotherapy regimen, Discontinuation, CDKN2A, Internal medicine, Glioma, Concomitant, Medicine, AcademicSubjects/MED00300, AcademicSubjects/MED00310, Neurology (clinical), Progression-free survival, business, Prospective cohort study

Abstract

Children with pediatric gliomas harboring BRAF V600E mutation have a poor outcome with current chemoradiation strategies. Our aim was to study the role of targeted BRAF inhibition in these tumors. We collected clinical, imaging, molecular and outcome information from BRAF V600E glioma patients treated with BRAFi across 29 centers from multiple countries. Sixty-seven patients were treated with BRAFi (56 pediatric low grade gliomas, PLGG and 11 pediatric high grade gliomas, PHGG) for up to 5.6 years. Objective responses were observed in 80% of PLGGs compared to 28% with conventional chemotherapy (p

Published

2020

4. MBCL-36. MOLECULAR STUDY IN PEDIATRIC MEDULLOBLASTOMA. VALIDATION OF GENETIC MARKERS IN A NATIONAL COHORT OF FORTY YEARS

Author

Alvaro Lassaletta, José Miguel Couselo, Miguel Garcia-Ariza, Ofelia Cruz, Itziar Astigarraga, Olaia Aurtenetxe, Laura Zaldumbide, Eduardo Quiroga, Aurora Navajas, T. Acha, Anna Llort, Idoia Martin-Guerrero, and Carlota Calvo

Subjects

Oncology, Medulloblastoma, Cancer Research, medicine.medical_specialty, business.industry, medicine.disease, National cohort, Abstracts, Genetic marker, Internal medicine, medicine, Neurology (clinical), business

Abstract

OBJECTIVE: To retrospectively assess at national level whether the addition of molecular data to clinical/histopathological factors could have modified the initial risk factors for survival in children with medulloblastoma. METHODS: A 40 years (1975-2015) retrospective study of 218 patients (0-18 years) from 24 national hospitals was performed. Histology and molecular review, including CTNNB1 gene mutations (RT-PCR) p53(immunohistochemistry) and MYCC/MYCN (FISH), was centralized. The patients were reclassified as standard (SR) or high-risk (HR) according to current knowledge. RESULTS: 187 cases had valid data. Median age 6.9 years (76%

Published

2018

5. LGG-16. PREDICTORS OF OUTCOME IN BRAF-V600E PEDIATRIC GLIOMAS TREATED WITH BRAF INHIBITORS: A REPORT FROM THE PLGG TASKFORCE

Author

Vijay Ramaswamy, Miriam Bornhorst, Murali Chintagumpala, Andres Morales La Madrid, Frank van Landeghem, Maria Luisa Garrè, Abhi Bavle, Palma Solano, Bev Wilson, Sarah Leary, Olaf Witt, Liana Nobre, Jean M. Mulcahy Levy, Nicholas K. Foreman, Naureen Mushtaq, Jack Su, Jordan R. Hansford, Diana S Osorio, Julia Balaguer Guill, David D. Eisenstat, Mariana Fernandes, Cornelis Vantilburg, Gurcharanjeet Kaur, Julie Bennett, Ana Guerreiro Stucklin, Valerie Larouche, Sabine Mueller, Till Milde, Inga Harting, Zdenek Pavelka, Scott Ryall, Eduardo Quiroga-Cantero, Jaroslav Sterba, Josef Zamecnik, Helena Mörse, Michal Zapotocky, Lenka Krskova, Anne Grete Bechensteen, Valentina Iurilli, Eric Bouffet, Didier Frappaz, Michael D. Taylor, Elisabeth Finch, Adela Misove, Uri Tabori, Sonika Dahiya, Cynthia Hawkins, Alvaro Lassaletta, Nisreen Amayiri, Peter Hauser, Tara McKeown, Ofelia Cruz, Samatha Mascelli, Scott L. Coven, Magnus Sabel, Adela Cañete, Lorena Baroni, Helen Toledano, Roger J. Packer, Sarah Injac, Ute Bartels, Jonathan L. Finlay, David Sumerauer, Cecile Faure Conter, Karen Gauvain, David W. Ellison, Peter B. Dirks, Theodore Nicolaides, Duarte Salgado, Daniel Alderete, and Matthias A. Karajannis

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, Low Grade Glioma, medicine.disease, Chemotherapy regimen, BRAF V600E, Internal medicine, Glioma, Mutation (genetic algorithm), Medicine, Low-Grade Glioma, Neurology (clinical), business, neoplasms

Abstract

The BRAF-V600E mutation is found in 15–20% of pediatric low grade gliomas (PLGG) and result in worse outcome and higher risk of transformation to high grade gliomas (PHGG). Although ongoing trials are assessing the role of BRAF inhibitors (BRAFi) in these children, data are still limited. We aimed to report overall response rates and predictors of outcome in childhood BRAF-V600E gliomas. We collected clinical, imaging and molecular information of patients treated with BRAFi outside trials from centers participating in the PLGG taskforce. Response was calculated by RANO criteria and follow up data were collected for all patients. Sixty-six patients were treated with BRAFi (55 PLGG and 11 PHGG); median follow-up time was 1.5 years (0.1-5y). In PLGG, objective response (tumor reduction of >25%) was observed in 77% compared to 15% in a cohort treated with conventional chemotherapy (pCDKN2A deletion was not associated with lack of response, while specific enhancing patterns correlated strongly with response to BRAFi. Two-year PFS for the BRAF-V600E PLGG was 74% vs 47% for BRAFi vs chemotherapy, respectively (p=0.02). Our data reveal rapid, dramatic and sustained response of BRAF-V600E PLGG to BRAFi. These are in contrast to BRAF-V600E PHGG and non-enhancing PLGG. Additional molecular analyses are being performed to identify poor responders and emerging mechanisms of resistance in these tumors.

Published

2019