Your search keyword '"Taillandier, L"' showing total 127 results

1. Systemic relapses of primary CNS lymphomas (PCNSL): a LOC network study

Author

Dufour, J., Choquet, S., Hoang-Xuan, K., Schmitt, A., Ahle, G., Houot, R., Taillandier, L., Gressin, R., Casasnovas, O., Marolleau, J.P., Tamburini, J., Serrier, C., Perez, E., Paillassa, J., Gyan, E., Chauchet, A., Ursu, R., Kas, A., Soussain, C., and Houillier, C.

Published

2023

2. Molecular and clinical diversity in primary central nervous system lymphoma

Author

Hernández-Verdin, I., Kirasic, E., Wienand, K., Mokhtari, K., Eimer, S., Loiseau, H., Rousseau, A., Paillassa, J., Ahle, G., Lerintiu, F., Uro-Coste, E., Oberic, L., Figarella-Branger, D., Chinot, O., Gauchotte, G., Taillandier, L., Marolleau, J.-P., Polivka, M., Adam, C., Ursu, R., Schmitt, A., Barillot, N., Nichelli, L., Lozano-Sánchez, F., Ibañez-Juliá, M.-J., Peyre, M., Mathon, B., Abada, Y., Charlotte, F., Davi, F., Stewart, C., de Reyniès, A., Choquet, S., Soussain, C., Houillier, C., Chapuy, B., Hoang-Xuan, K., and Alentorn, A.

Published

2023

3. Impact of fractionated stereotactic radiotherapy on activity of daily living and performance status in progressive/recurrent glioblastoma: a retrospective study

Author

Demogeot, Nicolas, Salleron, J., Rech, F., Taillandier, L., Royer, P., and Vogin, G.

Published

2022

4. Randomized phase II trial of irinotecan and bevacizumab as neo-adjuvant and adjuvant to temozolomide-based chemoradiation compared with temozolomide-chemoradiation for unresectable glioblastoma: final results of the TEMAVIR study from ANOCEF

Author

Chauffert, B., Feuvret, L., Bonnetain, F., Taillandier, L., Frappaz, D., Taillia, H., Schott, R., Honnorat, J., Fabbro, M., Tennevet, I., Ghiringhelli, F., Guillamo, J.S., Durando, X., Castera, D., Frenay, M., Campello, C., Dalban, C., Skrzypski, J., and Chinot, O.

Published

2014

5. P14.48 Extracerebral relapses of primary CNS lymphoma (PCNSL): a LOC network retrospective study

Author

Dufour, J, primary, Choquet, S, additional, Schmitt, A, additional, Ahle, G, additional, Houot, R, additional, Taillandier, L, additional, Ursu, R, additional, Hoang-Xuan, K, additional, Soussain, C, additional, and Houillier, C, additional

Published

2021

6. Concomitant bone marrow metastasis of a glioblastoma multiforme revealed at the diagnosis

Author

Didelot, A., Taillandier, L., Grignon, Y., Vespignani, H., and Beauchesne, P.

Published

2006

7. Improving the time-machine: estimating date of birth of grade II gliomas

Author

Gerin, C., Pallud, J., Grammaticos, B., Mandonnet, E., Deroulers, C., Varlet, P., Capelle, L., Taillandier, L., Bauchet, L., Duffau, H., and Badoual, M.

Published

2012

8. OS3.4 Karnofsky and WHO performance scores of brain tumour patients may limit inclusion in protocols though they depend on clinician status

Author

Frappaz, D, primary, Taillandier, L, additional, Bonneville Levard, A, additional, Sorre, J, additional, Ricard, D, additional, Carrie, S, additional, Schiffler, C, additional, and Weller, M, additional

Published

2019

9. Haemangioblastoma of the central nervous system in von Hippel-Lindau disease

Author

RICHARD, S., CAMPELLO, C., TAILLANDIER, L., PARKER, F., and RESCHE, F.

Published

1998

10. P05.28 Karnofsky performance score of brain tumor patients depends on clinician status

Author

Frappaz, D, primary, Taillandier, L, additional, Levard-Bonneville, A, additional, Sore, J, additional, Ricard, D, additional, Schiffler, C, additional, and Weller, M, additional

Published

2018

11. P01.034 Prospective evaluation of alternative therapies in glioma patients in France

Author

Le Rhun, E, primary, Lebrun Frenay, C, additional, Devos, P, additional, Darlix, A, additional, Lorgis, V, additional, Ahle, G, additional, Boone, M, additional, Taillandier, L, additional, Curtit, E, additional, Gras, L, additional, Bourg, V, additional, Ramirez, C, additional, Reyns, N, additional, Weller, M, additional, and Simon, N, additional

Published

2018

12. Personal exercise training in patients with gliomas: Preliminary results of feasibility and effectiveness

Author

Moreau, G., primary, Khalil, N., additional, Blonski, M., additional, Poussel, M., additional, Chenuel, B., additional, Taillandier, L., additional, and Paysant, J., additional

Published

2018

13. Temozolomide and Bevacizumab Induction before Chemoradiotherapy in Patients with Bulky Glioblastoma and/or with Severe Neurological Impairment

Author

Christine Desenclos, M C Morisse, Taillandier L, S. Trudel, Le Rhun E, Roufai Db, Blanchard N, Bruno Chauffert, Coutte A, Mathieu Boone, Faivre Jc, Blonski M, I. Darmon, CHU Amiens-Picardie, Centre Hospitalier Régional Universitaire de Nancy (CHRU Nancy), Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille), Centre Alexis Vautrin (CAV), Centre hospitalier régional Metz-Thionville (CHR Metz-Thionville), Clinique des Dentellières [Valenciennes, France], and SALZET, Michel

Subjects

medicine.medical_specialty, Bevacizumab, medicine.drug_class, medicine.medical_treatment, [SDV]Life Sciences [q-bio], multifocal glioblastoma, temozolomide, bevacizumab, Gastroenterology, 03 medical and health sciences, radiotherapy, 0302 clinical medicine, Internal medicine, medicine, Temozolomide, Performance status, business.industry, 3. Good health, [SDV] Life Sciences [q-bio], Radiation therapy, Oncology, 030220 oncology & carcinogenesis, Cohort, Toxicity, bulky glioblastoma, Corticosteroid, business, 030217 neurology & neurosurgery, Chemoradiotherapy, Research Paper, medicine.drug

Abstract

International audience; Background. New approaches are needed for patients newly diagnosed with bulky glioblastoma (GB) and/or with severe neurological impairment that cannot benefit from first line temozolomide (TMZ)-based chemoradiotherapy. Bevacizumab (BEV), an antiangiogenic anti-VEGF-R monoclonal antibody, has a rapid impact on tumor-related brain edema in recurrent GB. The present study reports the feasibility and efficacy of an induction treatment with TMZ and BEV to alleviate the initial neurological impairment and/or to reduce the tumor volume before a delayed chemoradiotherapy. Methods. We retrospectively analyzed tumor and target volumes and clinical neurological status in 39 patients with bulky GB and/or with severe neurological impairment after an induction treatment combining TMZ and BEV. Neurological and radiological responses were assessed according to RANO criteria. Calculating gross tumor and clinical target volumes (GTV and CTV) was done at diagnosis and before radiotherapy. Progression-free survival (PFS) and overall survival (OS) were determined by Kaplan Meier methods. Safety was reported according to NCTCAE. Results. A cohort of 39 patients was analyzed between December 2010 and April 2014. Upfront standard TMZ-based chemoradiotherapy was recused due either to tumor volume or impairment of neurological status and/or performance status. After TMZ/BEV induction (median time of 3 months), 6 (15%) patients achieved a partial response (PR), and 17 (44%) had a stable disease. 24 patients (62%) received a radical-intent chemoradiotherapy. TMZ-BEV induced median reduction of the clinical target volume (CTV) was 25.9% [-84.4%; - 4.8%]. The median PFS and OS were 8.4 months [95% CI: (6.6 - 9.9)] and 11.0 months [95% CI: (9.3 - 13.7)], respectively in the whole cohort and 10.8 [95% CI: (9.3 - 12.9)] and 15.0 [95% CI: (13.2 - 17.8)] for irradiated patients. Induction treatment led to corticosteroid dose reduction or cessation in 21 patients (54%). KPS improvement was observed in 38% of patients. Toxicity was mild with only 7/39 (18%) grade III-IV toxicity, including 1 digestive bleeding and 1 epistaxis. Conclusion. TMZ-BEV induction led to CTV reduction allowing for optimal chemoradiotherapy in a majority (62%) of patients for which radiotherapy was initially recused. A clinical benefit was obtained with improved KPS and a decrease in steroid dose.

Published

2017

14. MANAGEMENT PATTERNS AND OUTCOME OF PATIENTS WITH PRIMARY CNS LYMPHOMA (PCNSL) IN FRANCE DURING 2011-2016. A LOC NETWORK STUDY

Author

Houillier, C., Soussain, C., Ghesquieres, H., Soubeyran, P., Chinot, O., Taillandier, L., Houot, R., Ahle, G., Gyan, E., Hoang-Xuan, K., Service de neurologie 2 [CHU Pitié-Salpêtrière], CHU Pitié-Salpêtrière [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), CRLCC René Huguenin, Microenvironnement et cancer (MiCa), Université de Rennes 1 (UR1), Université de Rennes (UNIV-RENNES)-Université de Rennes (UNIV-RENNES)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), Centre Hospitalier Régional Universitaire de Tours (CHRU Tours), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Université de Rennes (UR)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-CHU Pitié-Salpêtrière [AP-HP], and Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)

Subjects

[SDV.CAN]Life Sciences [q-bio]/Cancer, ComputingMilieux_MISCELLANEOUS

Abstract

International audience; no abstract

Published

2016

15. Patterns of response and relapse in primary CNS lymphomas after first-line chemotherapy: imaging analysis of the ANOCEF-GOELAMS prospective randomized trial

Author

Tabouret, E., primary, Houillier, C., additional, Martin-Duverneuil, N., additional, Blonski, M., additional, Soussain, C, additional, Ghesquières, H., additional, Houot, R., additional, Larrieu, D., additional, Soubeyran, P., additional, Gressin, R., additional, Gyan, E., additional, Chinot, O., additional, Taillandier, L., additional, Choquet, S., additional, Alentorn, A., additional, Leclercq, D., additional, Omuro, A., additional, Tanguy, M.L., additional, and Hoang-Xuan, K., additional

Published

2016

16. OS7.6 Management patterns and outcome of patients with primary CNS lymphoma (PCNSL) in France during 2011–2016. A LOC network study

Author

Houillier, C., primary, Soussain, C., additional, Ghesquières, H., additional, Soubeyran, P., additional, Chinot, O., additional, Taillandier, L., additional, Houot, R., additional, Ahle, G., additional, Gyan, E., additional, and Hoang-Xuan, K., additional

Published

2016

17. Effectiveness of a personalized rehabilitation-reconditioning program in brain tumors

Author

Khalil, N., primary, Leyes-Bret, L., additional, Marcon, D., additional, Ferry, M.F., additional, Blonski, M., additional, Poussel, M., additional, Chenuel, B., additional, Taillandier, L., additional, and Paysant, J., additional

Published

2015

18. P17.09 * PCV CHEMOTHERAPY IMMEDIATELY FOLLOWED BY RADIOTHERAPY IN DIFFUSE LOW GRADE GLIOMAS - ABOUT A SERIES OF 12 PATIENTS

Author

Blonski, M., primary, Lacroix, C., additional, Thi-Lambert, P. N., additional, Gauchotte, G., additional, Hassani, K., additional, Manceau, P., additional, Ben Abdallah, M., additional, Moureaux, J., additional, Bastogne, T., additional, and Taillandier, L., additional

Published

2014

19. P08.02 * IDENTIFICATION AND QUANTIFICATION OF CSF MALIGNANT CELLS BY THE CELLSEARCH(R) TECHNOLOGY IN PATIENTS WITH LUNG LEPTOMENINGEAL METASTASIS

Author

Blonski, M., primary, Wittwer, B., additional, Faure, G., additional, Simon, L., additional, Bittencourt, M. D. C., additional, Tu, Q., additional, Larrieu, D., additional, Le Rhun, E., additional, and Taillandier, L., additional

Published

2014

20. P17.08 * RENAL THROMBOTIC MICROANGIOPATHY INDUCED BY BEVACIZUMAB IN HIGH GRADE GLIOMA PATIENTS - ABOUT SIX CASES

Author

Blonski, M., primary, Simon, L., additional, Houillier, C., additional, Idbaih, A., additional, Wittwer, B., additional, Beauchesne, P., additional, Hoang-Xuan, K., additional, and Taillandier, L., additional

Published

2014

21. New concepts in the management of diffuse low-grade glioma: Proposal of a multistage and individualized therapeutic approach

Author

Duffau, H., primary and Taillandier, L., additional

Published

2014

22. Imaging growth and isocitrate dehydrogenase 1 mutation are independent predictors for diffuse low-grade gliomas

Author

Goze, C., primary, Blonski, M., additional, Le Maistre, G., additional, Bauchet, L., additional, Dezamis, E., additional, Page, P., additional, Varlet, P., additional, Capelle, L., additional, Devaux, B., additional, Taillandier, L., additional, Duffau, H., additional, and Pallud, J., additional

Published

2014

23. Assessment and treatment relevance in elderly glioblastoma patients

Author

Bauchet, L., primary, Zouaoui, S., additional, Darlix, A., additional, Menjot de Champfleur, N., additional, Ferreira, E., additional, Fabbro, M., additional, Kerr, C., additional, and Taillandier, L., additional

Published

2014

24. Besoins de rééducation en onco-cancérologie – collaboration à multiples facettes

Author

Taillandier, L., primary

Published

2013

25. Physical medicine, rehabilitation and neuro-oncology interfaces to develop

Author

Taillandier, L., primary

Published

2013

26. Brainstem gliomas in adults: prognostic factors and classification.

Author

Guillamo J, Monjour A, Taillandier L, Devaux B, Varlet P, Haie-Meder C, Defer G, Maison P, Mazeron J, Cornu P, Delattre J, Guillamo, J S, Monjour, A, Taillandier, L, Devaux, B, Varlet, P, Haie-Meder, C, Defer, G L, Maison, P, and Mazeron, J J

Published

2001

27. CLIN-SYMPTOM MANAGEMENT/QUALITY OF LIFE

Author

Habets, E. J., primary, Taphoorn, M. J., additional, Nederend, S., additional, Klein, M., additional, Delgadillo, D., additional, Hoang-Xuan, K., additional, Bottomley, A., additional, Allgeier, A., additional, Seute, T., additional, Gijtenbeek, A. M., additional, De Gans, J., additional, Enting, R. H., additional, Tijssen, C. C., additional, Van den Bent, M. J., additional, Reijneveld, J. C., additional, Xu, H., additional, Halbert, K., additional, Bliss, R., additional, Trusheim, J., additional, Hunt, M. A., additional, Bunevicius, A., additional, Tamasauskas, S., additional, Tamasauskas, A., additional, Deltuva, V., additional, Field, K. M., additional, Guyatt, N., additional, Fleet, M., additional, Rosenthal, M. A., additional, Drummond, K. J., additional, Oliver, H., additional, Tobias, M., additional, Eva, V., additional, Matthias, S., additional, Johannes, S., additional, Oliver, S., additional, Christian, T. J., additional, Dietmar, K., additional, Gabriele, S., additional, Thomas, R., additional, Nikkhah, G., additional, Uwe, S., additional, Markus, L., additional, Michael, W., additional, Manfred, W., additional, Strowd, R. E., additional, Swett, K., additional, Harmon, M., additional, Pop-Vicas, A., additional, Chan, M., additional, Tatter, S. B., additional, Ellis, T. L., additional, Blevins, M., additional, High, K., additional, Lesser, G. J., additional, Benouaich-Amiel, A., additional, Taillandier, L., additional, Vercueil, L., additional, Valton, L., additional, Szurhaj, W., additional, Idbaih, A., additional, Delattre, J.-Y., additional, Loiseau, H., additional, Klein, I., additional, Block, V., additional, Ramirez, C., additional, Laigle-Donadey, F., additional, Le Rhun, E., additional, Harrison, C., additional, Van Horn, A., additional, Sapienza, C., additional, Schlimper, C., additional, Schlag, H., additional, Weber, F., additional, Acquaye, A. A., additional, Gilbert, M. R., additional, Armstrong, T. S., additional, Vera-Bolanos, E., additional, Walbert, T., additional, Elizabeth, V.-B., additional, Gilbert, M., additional, Affronti, M. L., additional, Woodring, S., additional, Allen, K., additional, Herndon, J. E., additional, McSherry, F., additional, Peters, K. B., additional, Friedman, H. S., additional, Desjardins, A., additional, Freeman, W., additional, Cheshire, S., additional, Cone, C., additional, Kalinowski, K. H., additional, Kim, J.-Y., additional, Lay, H. H., additional, Poillucci, V., additional, Southerland, C., additional, Tetterton, J., additional, Kirkpatrick, J., additional, Vredenburgh, J. J., additional, Edelstein, K., additional, Coate, L., additional, Mason, W. P., additional, Jewitt, N. C., additional, Massey, C., additional, Devins, G. M., additional, Lin, L., additional, Chiang, H.-H., additional, Cahill, J. E., additional, Amidei, C. M., additional, Lovely, M., additional, Page, M. D., additional, Mogensen, K., additional, Arzbaecher, J., additional, Lupica, K., additional, Maher, M. E., additional, Duong, H. T., additional, Kelly, D. F., additional, Gning, I., additional, Wefel, J. S., additional, Mendoza, T. R., additional, Cleeland, C. S., additional, Guthikonda, B., additional, Thakur, J. D., additional, Banerjee, A., additional, Shorter, C., additional, Sonig, A., additional, Khan, I. S., additional, Gardner, G. L., additional, Nanda, A., additional, Reddy, K., additional, Gaspar, L., additional, Kavanagh, B., additional, Waziri, A., additional, Chen, C., additional, Boele, F., additional, Hoeben, W., additional, Hilverda, K., additional, Lenting, J., additional, Calis, A.-L., additional, Sizoo, E., additional, Collette, E., additional, Heimans, J., additional, Postma, T., additional, Taphoorn, M., additional, and Reijneveld, J., additional

Published

2012

28. Randomized Multicenter Phase II Trial of Irinotecan and Bevacizumab as Neo-Adjuvant and Adjuvant to Temozolomide-Based Chemoradiation Versus Chemoradiation for Unresectable Glioblastoma (DEFINITIVE RESULTS OF THE TEMAVIR ANOCEF STUDY)

Author

Chauffert, B., primary, Feuvret, L., additional, Bonnetain, F., additional, Taillandier, L., additional, Frappaz, D., additional, Honnorat, J., additional, Fabbro, M., additional, Frenay, M., additional, Durando, X., additional, Tennevet, I., additional, Guillamo, J.S., additional, Tailla, H., additional, Schott, R., additional, Ghiringhelli, F., additional, Campello, C., additional, Tubiana-Mathieu, N., additional, Dalban, C., additional, Skrzypski, J., additional, and Chinot, O., additional

Published

2012

29. Intensive chemotherapy with thiotepa, busulfan and cyclophosphamide and hematopoietic stem cell rescue in relapsed or refractory primary central nervous system lymphoma and intraocular lymphoma: a retrospective study of 79 cases

Author

Soussain, C., primary, Choquet, S., additional, Fourme, E., additional, Delgadillo, D., additional, Bouabdallah, K., additional, Ghesquieres, H., additional, Damaj, G., additional, Dupriez, B., additional, Vargaftig, J., additional, Gonzalez, A., additional, Houillier, C., additional, Taillandier, L., additional, Hoang-Xuan, K., additional, and Leblond, V., additional

Published

2012

30. Improving the time-machine: estimating date of birth of grade II gliomas

Author

Gerin, C., primary, Pallud, J., additional, Grammaticos, B., additional, Mandonnet, E., additional, Deroulers, C., additional, Varlet, P., additional, Capelle, L., additional, Taillandier, L., additional, Bauchet, L., additional, Duffau, H., additional, and Badoual, M., additional

Published

2011

31. Peri-ictal pseudoprogression in patients with brain tumor

Author

Rheims, S., primary, Ricard, D., additional, van den Bent, M., additional, Taillandier, L., additional, Bourg, V., additional, Desestret, V., additional, Cartalat-Carel, S., additional, Hermier, M., additional, Monjour, A., additional, Delattre, J.-Y., additional, Sanson, M., additional, Honnorat, J., additional, and Ducray, F., additional

Published

2011

32. Ongoing Clinical Trials

Author

Clarke, J. L., primary, Ennis, M. M., additional, Lamborn, K. R., additional, Prados, M. D., additional, Puduvalli, V. K., additional, Penas-Prado, M., additional, Gilbert, M. R., additional, Groves, M. D., additional, Hess, K. R., additional, Levin, V. A., additional, de Groot, J., additional, Colman, H., additional, Conrad, C. A., additional, Loghin, M. E., additional, Hunter, K., additional, Yung, W. K., additional, Chen, C., additional, Damek, D., additional, Liu, A., additional, Gaspar, L. E., additional, Waziri, A., additional, Lillehei, K., additional, Kavanagh, B., additional, Finlay, J. L., additional, Haley, K., additional, Dhall, G., additional, Gardner, S., additional, Allen, J., additional, Cornelius, A., additional, Olshefski, R., additional, Garvin, J., additional, Pradhan, K., additional, Etzl, M., additional, Goldman, S., additional, Atlas, M., additional, Thompson, S., additional, Hirt, A., additional, Hukin, J., additional, Comito, M., additional, Bertolone, S., additional, Torkildson, J., additional, Joyce, M., additional, Moertel, C., additional, Letterio, J., additional, Kennedy, G., additional, Walter, A., additional, Ji, L., additional, Sposto, R., additional, Dorris, K., additional, Wagner, L., additional, Hummel, T., additional, Drissi, R., additional, Miles, L., additional, Leach, J., additional, Chow, L., additional, Turner, R., additional, Gragert, M. N., additional, Pruitt, D., additional, Sutton, M., additional, Breneman, J., additional, Crone, K., additional, Fouladi, M., additional, Friday, B. B., additional, Buckner, J., additional, Anderson, S. K., additional, Giannini, C., additional, Kugler, J., additional, Mazurczac, M., additional, Flynn, P., additional, Gross, H., additional, Pajon, E., additional, Jaeckle, K., additional, Galanis, E., additional, Badruddoja, M. A., additional, Pazzi, M. A., additional, Stea, B., additional, Lefferts, P., additional, Contreras, N., additional, Bishop, M., additional, Seeger, J., additional, Carmody, R., additional, Rance, N., additional, Marsella, M., additional, Schroeder, K., additional, Sanan, A., additional, Swinnen, L. J., additional, Rankin, C., additional, Rushing, E. J., additional, Hutchins, L. F., additional, Damek, D. M., additional, Barger, G. R., additional, Norden, A. D., additional, Lesser, G., additional, Hammond, S. N., additional, Drappatz, J., additional, Fadul, C. E., additional, Batchelor, T. T., additional, Quant, E. C., additional, Beroukhim, R., additional, Ciampa, A., additional, Doherty, L., additional, LaFrankie, D., additional, Ruland, S., additional, Bochacki, C., additional, Phan, P., additional, Faroh, E., additional, McNamara, B., additional, David, K., additional, Rosenfeld, M. R., additional, Wen, P. Y., additional, Phuphanich, S., additional, Reardon, D., additional, Wong, E. T., additional, Plotkin, S. R., additional, Mintz, A., additional, Raizer, J. J., additional, Kaley, T. J., additional, Smith, K. H., additional, Chamberlain, M. C., additional, Graham, C., additional, Mrugala, M., additional, Johnston, S., additional, Kreisl, T. N., additional, Smith, P., additional, Iwamoto, F., additional, Sul, J., additional, Butman, J. A., additional, Fine, H. A., additional, Westphal, M., additional, Heese, O., additional, Warmuth-Metz, M., additional, Pietsch, T., additional, Schlegel, U., additional, Tonn, J.-C., additional, Schramm, J., additional, Schackert, G., additional, Melms, A., additional, Mehdorn, H. M., additional, Seifert, V., additional, Geletneky, K., additional, Reuter, D., additional, Bach, F., additional, Khasraw, M., additional, Abrey, L. E., additional, Lassman, A. B., additional, Hormigo, A., additional, Nolan, C., additional, Gavrilovic, I. T., additional, Mellinghoff, I. K., additional, Reiner, A. S., additional, DeAngelis, L., additional, Omuro, A. M., additional, Burzynski, S. R., additional, Weaver, R. A., additional, Janicki, T. J., additional, Burzynski, G. S., additional, Szymkowski, B., additional, Acelar, S. S., additional, Mechtler, L. L., additional, O'Connor, P. C., additional, Kroon, H.-A., additional, Vora, T., additional, Kurkure, P., additional, Arora, B., additional, Gupta, T., additional, Dhamankar, V., additional, Banavali, S., additional, Moiyadi, A., additional, Epari, S., additional, Merchant, N., additional, Jalali, R., additional, Moller, S., additional, Grunnet, K., additional, Hansen, S., additional, Schultz, H., additional, Holmberg, M., additional, Sorensen, M. M., additional, Poulsen, H. S., additional, Lassen, U., additional, Reardon, D. A., additional, Vredenburgh, J. J., additional, Desjardins, A., additional, Janney, D. E., additional, Peters, K., additional, Sampson, J., additional, Gururangan, S., additional, Friedman, H. S., additional, Jeyapalan, S., additional, Constantinou, M., additional, Evans, D., additional, Elinzano, H., additional, O'Connor, B., additional, Puthawala, M. Y., additional, Goldman, M., additional, Oyelese, A., additional, Cielo, D., additional, Dipetrillo, T., additional, Safran, H., additional, Anan, M., additional, Seyed Sadr, M., additional, Alshami, J., additional, Sabau, C., additional, Seyed Sadr, E., additional, Siu, V., additional, Guiot, M.-C., additional, Samani, A., additional, Del Maestro, R., additional, Bogdahn, U., additional, Stockhammer, G., additional, Mahapatra, A. K., additional, Venkataramana, N. K., additional, Oliushine, V. E., additional, Parfenov, V. E., additional, Poverennova, I. E., additional, Hau, P., additional, Jachimczak, P., additional, Heinrichs, H., additional, Schlingensiepen, K.-H., additional, Shibui, S., additional, Kayama, T., additional, Wakabayashi, T., additional, Nishikawa, R., additional, de Groot, M., additional, Aronica, E., additional, Vecht, C. J., additional, Toering, S. T., additional, Heimans, J. J., additional, Reijneveld, J. C., additional, Batchelor, T., additional, Mulholland, P., additional, Neyns, B., additional, Nabors, L. B., additional, Campone, M., additional, Wick, A., additional, Mason, W., additional, Mikkelsen, T., additional, Ashby, L. S., additional, DeGroot, J. F., additional, Gattamaneni, H. R., additional, Cher, L. M., additional, Rosenthal, M. A., additional, Payer, F., additional, Xu, J., additional, Liu, Q., additional, van den Bent, M., additional, Nabors, B., additional, Fink, K., additional, Chan, M., additional, Trusheim, J., additional, Raval, S., additional, Hicking, C., additional, Henslee-Downey, J., additional, Picard, M., additional, Schiff, D., additional, Karimi, S., additional, DeAngelis, L. M., additional, Nolan, C. P., additional, Omuro, A., additional, Gavrilovic, I., additional, Norden, A., additional, Purow, B. W., additional, Lieberman, F. S., additional, Hariharan, S., additional, Perez-Larraya, J. G., additional, Honnorat, J., additional, Chinot, O., additional, Catry-Thomas, I., additional, Taillandier, L., additional, Guillamo, J. S., additional, Campello, C., additional, Monjour, A., additional, Tanguy, M. L., additional, Delattre, J. Y., additional, Franz, D. N., additional, Krueger, D. A., additional, Care, M. M., additional, Holland-Bouley, K., additional, Agricola, K., additional, Tudor, C., additional, Mangeshkar, P., additional, Byars, A. W., additional, Sahmoud, T., additional, Alonso-Basanta, M., additional, Lustig, R. A., additional, Dorsey, J. F., additional, Lai, R. K., additional, Recht, L. D., additional, Paleologos, N., additional, Groves, M., additional, Meech, S., additional, Davis, T., additional, Pavlov, D., additional, Marshall, M. A., additional, Slot, M., additional, Peerdeman, S. M., additional, Beauchesne, P. D., additional, Faure, G., additional, Noel, G., additional, Schmitt, T., additional, Kerr, C., additional, Jadaud, E., additional, Martin, L., additional, Carnin, C., additional, Peters, K. B., additional, Herndon, J. E., additional, Kirkpatrick, J. P., additional, Nayak, L., additional, Panageas, K. S., additional, and Deangelis, L. M., additional

Published

2010

33. Prolonged survival for patients with newly diagnosed, inoperable glioblastoma with 3-times daily ultrafractionated radiation therapy

Author

Beauchesne, P., primary, Bernier, V., additional, Carnin, C., additional, Taillandier, L., additional, Djabri, M., additional, Martin, L., additional, Michel, X., additional, Maire, J.-P., additional, Khalil, T., additional, Kerr, C., additional, Gorlia, T., additional, Stupp, R., additional, and Pedeux, R., additional

Published

2010

34. Correlation between genetic alterations and growth of human malignant glioma xenografted in nude mice

Author

Leuraud, P, primary, Taillandier, L, additional, Aguirre-Cruz, L, additional, Medioni, J, additional, Crinière, E, additional, Marie, Y, additional, Dutrillaux, A M, additional, Kujas, M, additional, Duprez, A, additional, Delattre, J-Y, additional, Poupon, M-F, additional, and Sanson, M, additional

Published

2003

35. LBA15 - Randomized Multicenter Phase II Trial of Irinotecan and Bevacizumab as Neo-Adjuvant and Adjuvant to Temozolomide-Based Chemoradiation Versus Chemoradiation for Unresectable Glioblastoma (DEFINITIVE RESULTS OF THE TEMAVIR ANOCEF STUDY)

Author

Chauffert, B., Feuvret, L., Bonnetain, F., Taillandier, L., Frappaz, D., Honnorat, J., Fabbro, M., Frenay, M., Durando, X., Tennevet, I., Guillamo, J.S., Tailla, H., Schott, R., Ghiringhelli, F., Campello, C., Tubiana-Mathieu, N., Dalban, C., Skrzypski, J., and Chinot, O.

Published

2012

36. P01.034 Prospective evaluation of alternative therapies in glioma patients in France.

Author

Rhun, E Le, Frenay, C Lebrun, Devos, P, Darlix, A, Lorgis, V, Ahle, G, Boone, M, Taillandier, L, Curtit, E, and Gras, L

Published

2018

37. A neuroimmunological aproach to CNS neoplastic disease: the way to immunotherapy - OC40.

Author

Tanasescu, R., Ticmeanu, M., Beauchesne, P., and Taillandier, L.

Subjects

*CENTRAL nervous system diseases

Abstract

An abstract of the article "A neuroimmunological aproach to CNS neoplastic disease: the way to immunotherapy," by R. Tanasescu and colleagues is presented.

Published

2008

38. Descriptive epidemiology of 399 histologically confirmed newly diagnosed meningeal solitary fibrous tumours and haemangiopericytomas in France: 2006-2015.

Author

Champeaux Depond C, Zouaoui S, Darlix A, Rigau V, Mathieu-Daudé H, Bauchet F, Khettab M, Trétarre B, Figarella-Branger D, Taillandier L, Boetto J, Pallud J, Peyre M, Lottin M, and Bauchet L

Subjects

Humans, France epidemiology, Female, Male, Middle Aged, Adult, Aged, Incidence, Young Adult, Meningioma epidemiology, Meningioma pathology, Meningioma surgery, Meningioma diagnosis, Adolescent, Aged, 80 and over, Child, Hemangiopericytoma epidemiology, Hemangiopericytoma pathology, Hemangiopericytoma surgery, Hemangiopericytoma diagnosis, Meningeal Neoplasms epidemiology, Meningeal Neoplasms pathology, Meningeal Neoplasms surgery, Meningeal Neoplasms diagnosis, Solitary Fibrous Tumors epidemiology, Solitary Fibrous Tumors pathology, Solitary Fibrous Tumors surgery, Solitary Fibrous Tumors diagnosis

Abstract

Purpose: Meningeal solitary fibrous tumour (SFT) and haemangiopericytoma (HPC) are uncommon tumours that have been merged into a single entity in the last 2021 WHO Classification of Tumors of the Central Nervous System. To describe the epidemiology of SFT/HPC operated in France and, to assess their incidence., Methods: We processed the French Brain Tumour Database (FBTDB) to conduct a nationwide population-based study of all histopathologically confirmed SFT/HPC between 2006 and 2015., Results: Our study included 399 SFT/HPC patients, operated in France between 2006 and 2015, in one of the 46 participating neurosurgical centres. The incidence reached 0.062, 95% CI[0.056-0.068] for 100,000 person-years. SFT accounted for 35.8% and, HPC for 64.2%. The ratio of SFT/HPC over meningioma operated during the same period was 0.013. SFT/HPC are about equally distributed in women and men (55.9% vs. 44.1%). For the whole population, mean age at surgery was 53.9 (SD ± 15.8) years. The incidence of SFT/HPC surgery increases with the age and, is maximal for the 50-55 years category. Benign SFT/HPC accounted for 65.16%, SFT/HPC of uncertain behaviour for 11.53% and malignant ones for 23.31%. The number of resection progresses as the histopathological behaviour became more aggressive. 6.7% of the patients with a benign SFT/HPC had a second surgery vs.16.6% in case of uncertain behaviour and, 28.4% for malignant SFT/HPC patients., Conclusion: Meningeal SFT and HPC are rare CNS mesenchymal tumours which both share common epidemiological characteristics, asserting their merging under a common entity. SFT/HPC incidence is less that one case for 1 billion per year and, for around 100 meningiomas-like tumours removed, one SFT/HPC may be diagnosed. SFT/HPC are equally distributed in women and men and, are mainly diagnosed around 50-55 years. The more aggressive the tumour, the higher the probability of recurrence., (© 2024. The Author(s), under exclusive licence to Springer-Verlag GmbH Austria, part of Springer Nature.)

Published

2024

39. Descriptive epidemiology of 30,223 histopathologically confirmed meningiomas in France: 2006-2015.

Author

Depond CC, Zouaoui S, Darlix A, Rigau V, Mathieu-Daudé H, Bauchet F, Khettab M, Trétarre B, Figarella-Branger D, Taillandier L, Boetto J, Pallud J, Zemmoura I, Roche PH, and Bauchet L

Subjects

Humans, France epidemiology, Female, Male, Middle Aged, Aged, Adult, Incidence, Aged, 80 and over, Neoplasm Grading, Young Adult, Adolescent, Databases, Factual, Meningioma epidemiology, Meningioma pathology, Meningioma surgery, Meningeal Neoplasms epidemiology, Meningeal Neoplasms pathology, Meningeal Neoplasms surgery

Abstract

Background and Objectives: Meningioma is one of the most common neoplasm of the central nervous system. To describe the epidemiology of meningioma operated in France and, to assess grading and histopathological variability among the different neurosurgical centres., Methods: We processed the French Brain Tumour Database (FBTDB) to conduct a nationwide population-based study of all histopathologically confirmed meningiomas between 2006 and 2015., Results: 30,223 meningiomas cases were operated on 28,424 patients, in 61 centres. The average number of meningioma operated per year in France was 3,022 (SD ± 122). Meningioma was 3 times more common in women (74.1% vs. 25.9%). The incidence of meningioma increased with age and, mean age at surgery was 58.5 ± 13.9 years. Grade 1, 2, and 3 meningiomas accounted for 83.9%, 13.91% and, 2.19% respectively. There was a significant variability of meningioma grading by institutions, especially for grade 2 which spanned from 5.1% up to 22.4% (p < 0.001). Moreover, the proportion of grade 2 significantly grew over the study period (p < 0.001). There was also a significant variation in grade 1 subtypes diagnosis among the institutions (p < 0.001). 89.05% of the patients had solely one meningioma surgery, 8.52% two and, 2.43% three or more. The number of surgeries was associated to the grade of malignancy (p < 0.001)., Conclusion: The incidence of meningioma surgery increased with age and, peaked at 58.5 years. They were predominantly benign with meningothelial subtype being the most common. However, there was a significant variation of grade 1 subtypes diagnosis among the centres involved. The proportion of grade 2 meningioma significantly grew over the study time, on contrary to malignant meningioma proportion, which remained rare and, stable over time around 2%. Likewise, there was a significant variability of grade 2 meningioma rate among the institutions., (© 2024. The Author(s), under exclusive licence to Springer-Verlag GmbH Austria, part of Springer Nature.)

Published

2024

40. Anti-Hu Antibodies in Patients With Neurologic Side Effects of Immune Checkpoint Inhibitors.

Author

Farina A, Villagrán-García M, Ciano-Petersen NL, Vogrig A, Muñiz-Castrillo S, Taillandier L, Michaud M, Lefilliatre M, Wang A, Lepine Z, Picard G, Wucher V, Dhairi M, Fabien N, Goncalves D, Rogemond V, Joubert B, and Honnorat J

Subjects

Humans, Male, Female, Immune Checkpoint Inhibitors adverse effects, Peripheral Nervous System, Antibodies, Antinuclear, Drug-Related Side Effects and Adverse Reactions, Lung Neoplasms

Abstract

Background and Objectives: To clinically characterize post-immune checkpoint inhibitor (ICI) Hu antibody (Ab) neurologic disorders, we analyzed Hu-Ab-positive patients with neurologic immune-related adverse events (n-irAEs) and compared them with patients with other n-irAEs, ICI-naive patients with Hu-Ab paraneoplastic neurologic syndromes (PNSs) identified in the same study center, and those with Hu-Ab n-irAEs reported elsewhere., Methods: Patients whose samples were sent to the French reference center for a suspicion of n-irAE (2015-2021) were identified; those with a final diagnosis of n-irAE and Hu-Ab were included. Control groups included patients with a final diagnosis of n-irAE occurring during the same period as the patients included (2018-2021) but without Hu-Ab, and ICI-naive patients with Hu-Ab PNS diagnosed during the same period; a systematic review was performed to identify previous reports., Results: Eleven patients with Hu-Ab and n-irAEs were included (median age, 66 years, range 44-76 years; 73% men). Ten patients had small cell lung cancer, and 1 had lung adenocarcinoma. The median follow-up from onset was 3 months (range 0.5-18 months). Compared with those with other n-irAEs (n = 63), Hu-Ab-positive patients had more frequently co-occurring involvement of both central and peripheral nervous systems (36% vs 8%, p = 0.02) and limbic (54% vs 14%, p < 0.01), brainstem (27% vs 5%, p = 0.02), and dorsal root ganglia (45% vs 5%, p < 0.01) involvement. The proportion of patients with severe disability (modified Rankin Scale score >3) at diagnosis was higher among Hu-Ab n-irAEs (91% vs 52%, p = 0.02). Patients with Hu-Ab had also poorer outcome (100% vs 28%, p < 0.01) and higher mortality (91% vs 46%, p < 0.01). There was no significant difference in terms of clinical features between Hu-Ab n-irAEs and ICI-naive Hu-Ab PNS (n = 92), but there was a poorer outcome (56/78, 71%, p < 0.01) and higher mortality (26%, p < 0.01) among the former. No significant difference was found between the patients reported herein and those in the literature., Discussion: The presence of Hu-Ab identifies a subgroup of n-irAEs that consistently reproduce the phenotypes of Hu-Ab-related PNS, supporting the hypothesis of ICI triggering or unmasking PNS. As these patients show high disability and mortality, further studies are required to investigate the underlying immunopathogenic mechanisms and to improve the outcome of Hu-Ab n-irAEs., (Copyright © 2022 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Academy of Neurology.)

Published

2022

41. Characteristics of Anaplastic Oligodendrogliomas Short-Term Survivors: A POLA Network Study.

Author

Garnier L, Vidal C, Chinot O, Cohen-Jonathan Moyal E, Djelad A, Bronnimann C, Bekaert L, Taillandier L, Frenel JS, Langlois O, Colin P, Menei P, Dhermain F, Carpentier C, Gerazime A, Curtit E, Figarella-Branger D, Dehais C, and Ducray F

Subjects

Chromosome Aberrations, Humans, Retrospective Studies, Survivors, Temozolomide therapeutic use, Brain Neoplasms pathology, Oligodendroglioma genetics

Abstract

Background: Anaplastic oligodendrogliomas IDH-mutant and 1p/19q codeleted (AO) occasionally have a poor outcome. Herein we aimed at analyzing their characteristics., Methods: We retrospectively analyzed the characteristics of 44 AO patients with a cancer-specific survival <5 years (short-term survivors, STS) and compared them with those of 146 AO patients with a survival ≥5 years (classical survivors, CS) included in the POLA network., Results: Compared to CS, STS were older (P = .0001), less frequently presented with isolated seizures (P < .0001), more frequently presented with cognitive dysfunction (P < .0001), had larger tumors (P = .= .003), a higher proliferative index (P = .= .0003), and a higher number of chromosomal arm abnormalities (P = .= .02). Regarding treatment, STS less frequently underwent a surgical resection than CS (P = .= .0001) and were more frequently treated with chemotherapy alone (P = .= .009) or with radiotherapy plus temozolomide (P = .= .05). Characteristics independently associated with STS in multivariate analysis were cognitive dysfunction, a number of mitosis > 8, and the absence of tumor resection. Based on cognitive dysfunction, type of surgery, and number of mitosis, patients could be classified into groups of standard (18%) and high (62%) risk of <5 year survival., Conclusion: The present study suggests that although STS poor outcome appears to largely result from a more advanced disease at diagnosis, surgical resection may be particularly important in this population., (© The Author(s) 2022. Published by Oxford University Press.)

Published

2022

42. Initial PCV Chemotherapy Followed by Radiotherapy Is Associated With a Prolonged Response But Late Neurotoxicity in 20 Diffuse Low-Grade Glioma Patients.

Author

Blonski M, Obara T, Brzenczek C, Pouget C, Dillier C, Meyer M, Lavigne L, Forthoffer N, Broussois A, Gauchotte G, Baron MH, Rech F, Mézières S, Gaudeau Y, Verger A, Vogin G, Anxionnat R, Moureaux JM, and Taillandier L

Abstract

Background: Study RTOG 9802 in high-risk diffuse low-grade gliomas (DLGGs) showed the potential synergistic effect on survival of the procarbazine, CCNU, and vincristine (PCV) radiotherapy (RT) combination. Limited data on long-term neurocognitive impact and quality of life (QoL) have yet been reported., Patients and Methods: We described a monocentric series of patients treated at first line by the combination of PCV immediately followed by RT between January 01, 1982 and January 01, 2017. Radiological data were collected and included volume, velocity of diametric expansion (VDE), and MRI aspects. Long-term neurocognitive and QoL were analyzed., Results: Twenty patients fulfilled the eligibility criteria. The median response rate was 65.1% (range, 9.6%-99%) at the time of maximal VDE decrease corresponding to a median volume reduction of 79.7 cm 3 (range, 3.1 to 174.2 cm 3 ), which occurred after a median period of 7.2 years (range, 0.3-21.9) after the end of RT. An ongoing negative VDE was measured in 13/16 patients after the end of RT, with a median duration of 6.7 years (range, 9 months-21.9 years). The median follow-up since radiological diagnosis was 17.5 years (range, 4.8 to 29.5). Estimated median survival was 17.4 years (95% CI: 12; NR). After a long-term follow-up, substantial neurotoxicity was noticed with dementia in six progression-free patients (30%), leading to ventriculo-peritoneal shunt procedures in three, and premature death in five. Thirteen patients (65%) were unable to work with disability status. Successive longitudinal neurocognitive assessments for living patients showed verbal episodic memory deterioration., Conclusions: PCV-RT combination seems to have not only an oncological synergy but also a long-term neurotoxic synergy to consider before initial therapeutic decision., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Blonski, Obara, Brzenczek, Pouget, Dillier, Meyer, Lavigne, Forthoffer, Broussois, Gauchotte, Baron, Rech, Mézières, Gaudeau, Verger, Vogin, Anxionnat, Moureaux and Taillandier.)

Published

2022

43. 18 F-FDOPA PET for the Noninvasive Prediction of Glioma Molecular Parameters: A Radiomics Study.

Author

Zaragori T, Oster J, Roch V, Hossu G, Chawki MB, Grignon R, Pouget C, Gauchotte G, Rech F, Blonski M, Taillandier L, Imbert L, and Verger A

Subjects

Adult, Aged, Female, Humans, Male, Middle Aged, Image Processing, Computer-Assisted methods, Machine Learning, Mutation, Retrospective Studies, Brain Neoplasms diagnostic imaging, Brain Neoplasms genetics, Dihydroxyphenylalanine analogs & derivatives, Glioma diagnostic imaging, Glioma genetics, Isocitrate Dehydrogenase genetics, Positron-Emission Tomography

Abstract

The assessment of gliomas by 18 F-FDOPA PET imaging as an adjunct to MRI showed high performance by combining static and dynamic features to noninvasively predict the isocitrate dehydrogenase (IDH) mutations and the 1p/19q codeletion, which the World Health Organization classified as significant parameters in 2016. The current study evaluated whether other 18 F-FDOPA PET radiomics features further improve performance and the contributions of each of these features to performance. Methods: Our study included 72 retrospectively selected, newly diagnosed glioma patients with 18 F-FDOPA PET dynamic acquisitions. A set of 114 features, including conventional static features and dynamic features, as well as other radiomics features, were extracted and machine-learning models trained to predict IDH mutations and the 1p/19q codeletion. Models were based on a machine-learning algorithm built from stable, relevant, and uncorrelated features selected by hierarchic clustering followed by a bootstrapped feature selection process. Models were assessed by comparing area under the curve using a nested cross-validation approach. Feature importance was assessed using Shapley additive explanations values. Results: The best models were able to predict IDH mutations (logistic regression with L2 regularization) and the 1p/19q codeletion (support vector machine with radial basis function kernel) with an area under the curve of 0.831 (95% CI, 0.790-0.873) and 0.724 (95% CI, 0.669-0.782), respectively. For the prediction of IDH mutations, dynamic features were the most important features in the model (time to peak, 35.5%). In contrast, other radiomics features were the most useful for predicting the 1p/19q codeletion (up to 14.5% of importance for the small-zone low-gray-level emphasis). Conclusion: 18 F-FDOPA PET is an effective tool for the noninvasive prediction of glioma molecular parameters using a full set of amino-acid PET radiomics features. The contribution of each feature set shows the importance of systematically integrating dynamic acquisition for prediction of the IDH mutations as well as developing the use of radiomics features in routine practice for prediction of the 1p/19q codeletion., (© 2022 by the Society of Nuclear Medicine and Molecular Imaging.)

Published

2022

44. Effects of Carbidopa Premedication on 18 F-FDOPA PET Imaging of Glioma: A Multiparametric Analysis.

Author

Bros M, Zaragori T, Rech F, Blonski M, Hossu G, Taillandier L, Marie PY, and Verger A

Abstract

Purpose: This study aimed to determine the impact of carbidopa premedication on static, dynamic and radiomics parameters of 18 F-FDOPA PET in brain tumors., Methods: The study included 54 patients, 18 of whom received carbidopa, who underwent 18 F-FDOPA PET for newly diagnosed gliomas. SUV-derived, 105 radiomics features and TTP dynamic parameters were extracted from volumes of interest in healthy brains and tumors. Simulation of the effects of carbidopa on time-activity curves were generated., Results: All static and TTP dynamic parameters were significantly higher in healthy brain regions of premedicated patients (ΔSUV mean = +53%, ΔTTP = +48%, p < 0.001). Furthermore, carbidopa impacted 81% of radiomics features, of which 92% correlated with SUV mean (absolute correlation coefficient ≥ 0.4). In tumors, premedication with carbidopa was an independent predictor of SUV mean (ΔSUV mean = +52%, p < 0.001) and TTP (ΔTTP = +24%, p = 0.025). All parameters were no longer significantly modified by carbidopa premedication when using ratios to healthy brain. Simulated data confirmed that carbidopa leads to higher tumor TTP values, corrected by the ratios., Conclusion: In 18 F-FDOPA PET, carbidopa induces similarly higher SUV and TTP dynamic parameters and similarly impacts SUV-dependent radiomics in healthy brain and tumor regions, which is compensated for by correcting for the tumor-to-healthy-brain ratio. This is a significant advantage for multicentric study harmonization.

Published

2021

45. Dynamic 18 F-FDopa PET Imaging for Newly Diagnosed Gliomas: Is a Semiquantitative Model Sufficient?

Author

Zaragori T, Doyen M, Rech F, Blonski M, Taillandier L, Imbert L, and Verger A

Abstract

Purpose: Dynamic amino acid positron emission tomography (PET) has become essential in neuro-oncology, most notably for its prognostic value in the noninvasive prediction of isocitrate dehydrogenase (IDH) mutations in newly diagnosed gliomas. The 6-[ 18 F]fluoro-l-DOPA ( 18 F-FDOPA) kinetic model has an underlying complexity, while previous studies have predominantly used a semiquantitative dynamic analysis. Our study addresses whether a semiquantitative analysis can capture all the relevant information contained in time-activity curves for predicting the presence of IDH mutations compared to the more sophisticated graphical and compartmental models., Methods: Thirty-seven tumour time-activity curves from 18 F-FDOPA PET dynamic acquisitions of newly diagnosed gliomas (median age = 58.3 years, range = 20.3-79.9 years, 16 women, 16 IDH-wild type) were analyzed with a semiquantitative model based on classical parameters, with (SQ) or without (Ref SQ) a reference region, or on parameters of a fit function (SQ Fit), a graphical Logan model with input function (Logan) or reference region (Ref Logan), and a two-tissue compartmental model previously reported for 18 F-FDOPA PET imaging of gliomas (2TCM). The overall predictive performance of each model was assessed with an area under the curve (AUC) comparison using multivariate analysis of all the parameters included in the model. Moreover, each extracted parameter was assessed in a univariate analysis by a receiver operating characteristic curve analysis., Results: The SQ model with an AUC of 0.733 for predicting IDH mutations showed comparable performance to the other models with AUCs of 0.752, 0.814, 0.693, 0.786, and 0.863, respectively corresponding to SQ Fit, Ref SQ, Logan, Ref Logan, and 2TCM ( p ≥ 0.10 for the pairwise comparisons with other models). In the univariate analysis, the SQ time-to-peak parameter had the best diagnostic performance (75.7% accuracy) compared to all other individual parameters considered., Conclusions: The SQ model circumvents the complexities of the 18 F-FDOPA kinetic model and yields similar performance in predicting IDH mutations when compared to the other models, most notably the compartmental model. Our study provides supportive evidence for the routine clinical application of the SQ model for the dynamic analysis of 18 F-FDOPA PET images in newly diagnosed gliomas., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Zaragori, Doyen, Rech, Blonski, Taillandier, Imbert and Verger.)

Published

2021

46. TEMOBIC: Phase II Trial of Neoadjuvant Chemotherapy for Unresectable Anaplastic Gliomas: An ANOCEF Study.

Author

Tabouret E, Fabbro M, Autran D, Hoang-Xuan K, Taillandier L, Ducray F, Barrie M, Sanson M, Kerr C, Cartalat-Carel S, Loundou A, Guillevin R, Mokhtari K, Figarella-Branger D, Delattre JY, and Chinot O

Subjects

Adult, Aged, Antineoplastic Agents, Alkylating adverse effects, Dacarbazine therapeutic use, Humans, Middle Aged, Neoadjuvant Therapy, Young Adult, Brain Neoplasms drug therapy, Brain Neoplasms radiotherapy, Glioma drug therapy, Glioma radiotherapy

Abstract

Lessons Learned: Treatment with temozolomide and BCNU was associated with substantial response and survival rates for patients with unresectable anaplastic glioma, suggesting potential therapeutic alternative for these patients. The optimal treatment for unresectable large anaplastic gliomas remains debated., Background: The optimal treatment for unresectable large anaplastic gliomas remains debated., Methods: Adult patients with histologically proven unresectable anaplastic oligodendroglioma or mixed gliomas (World Health Organization [WHO] 2007) were eligible. Treatment consisted of BCNU (150 mg/m 2 ) and temozolomide (110 mg/m 2 for 5 days) every 6 weeks for six cycles before radiotherapy., Results: Between December 2005 and December 2009, 55 patients (median age of 53.1 years; range, 20.5-70.2) were included. Forty percent of patients presented with wild-type IDH1 gliomas, and 30% presented with methylated MGMT promoter. Median progression-free survival (PFS), centralized PFS, and overall survival (OS) were 16.6 (95% confidence interval [CI], 12.8-20.3), 15.4 (95% CI, 10.0-20.8), and 25.4 (95% CI, 17.5-33.2) months, respectively. Complete and partial responses under chemotherapy were observed for 28.3% and 17% of patients, respectively. Radiotherapy completion was achieved for 75% of patients. Preservation of functional status and self-care capability (Karnofsky performance status [KPS] ≥70) were preserved until disease progression for 69% of patients. Grade ≥ 3 toxicities were reported for 52% of patients, and three deaths were related to treatment. By multivariate analyses including age and KPS, IDH mutation was associated with better prognostic for both PFS and OS, whereas MGMT promoter methylation was associated with better OS., Conclusion: The association of BCNU and temozolomide upfront is active for patients with unresectable anaplastic gliomas, but toxicity limits its use., (© AlphaMed Press; the data published online to support this summary are the property of the authors.)

Published

2021

47. What Does Quality of Care Mean in Lower-Grade Glioma Patients: A Precision Molecular-Based Management of the Tumor or an Individualized Medicine Centered on Patient's Choices?

Author

Taillandier L, Obara T, and Duffau H

Abstract

Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Published

2021

48. Adult Diffuse Low-Grade Gliomas: 35-Year Experience at the Nancy France Neurooncology Unit.

Author

Obara T, Blonski M, Brzenczek C, Mézières S, Gaudeau Y, Pouget C, Gauchotte G, Verger A, Vogin G, Moureaux JM, Duffau H, Rech F, and Taillandier L

Abstract

Background: To report survival, spontaneous prognostic factors, and treatment efficacy in a French monocentric cohort of diffuse low-grade glioma (DLGG) patients over 35 years of follow-up., Methods: A monocentric retrospective study of 339 patients diagnosed with a new DLGG between 01/01/1982 and 01/01/2017 was created. Inclusion criteria were patient age ≥18 years at diagnosis and histological diagnosis of WHO grade II glioma (according to 1993, 2007, and 2016 WHO classifications). The survival parameters were estimated using the Kaplan-Meier method with a 95% confidence interval. Differences in survival were tested for statistical significance by the log-rank test. Factors were considered significant when p ≤ 0.1 and p ≤ 0.05 in the univariate and multivariate analyses, respectively., Results: A total of 339 patients were included with a median follow-up of 8.7 years. The Kaplan-Meier median overall survival was 15.7 years. At the time of radiological diagnosis, Karnofsky Performance Status score and initial tumor volume were significant independent prognostic factors. Oncological prognostic factors were the extent of resection for patients who underwent surgery and the timing of radiotherapy for those concerned. In this study, patients who had delayed radiotherapy (provided remaining low grade) did not have worse survival compared with patients who had early radiotherapy. The functional capabilities of the patients were preserved enough so that they could remain independent during at least three quarters of the follow-up., Conclusion: This large monocentric series spread over a long time clarifies the effects of different therapeutic strategies and their combination in the management of DLGG., (Copyright © 2020 Obara, Blonski, Brzenczek, Mézières, Gaudeau, Pouget, Gauchotte, Verger, Vogin, Moureaux, Duffau, Rech and Taillandier.)

Published

2020

49. Use of static and dynamic [ 18 F]-F-DOPA PET parameters for detecting patients with glioma recurrence or progression.

Author

Zaragori T, Ginet M, Marie PY, Roch V, Grignon R, Gauchotte G, Rech F, Blonski M, Lamiral Z, Taillandier L, Imbert L, and Verger A

Abstract

Background: Static [ 18 F]-F-DOPA PET images are currently used for identifying patients with glioma recurrence/progression after treatment, although the additional diagnostic value of dynamic parameters remains unknown in this setting. The aim of this study was to evaluate the performances of static and dynamic [ 18 F]-F-DOPA PET parameters for detecting patients with glioma recurrence/progression as well as assess further relationships with patient outcome., Methods: Fifty-one consecutive patients who underwent an [ 18 F]-F-DOPA PET for a suspected glioma recurrence/progression at post-resection MRI, were retrospectively included. Static parameters, including mean and maximum tumor-to-normal-brain (TBR) ratios, tumor-to-striatum (TSR) ratios, and metabolic tumor volume (MTV), as well as dynamic parameters with time-to-peak (TTP) values and curve slope, were tested for predicting the following: (1) glioma recurrence/progression at 6 months after the PET exam and (2) survival on longer follow-up., Results: All static parameters were significant predictors of glioma recurrence/progression (accuracy ≥ 94%) with all parameters also associated with mean progression-free survival (PFS) in the overall population (all p < 0.001, 29.7 vs. 0.4 months for TBR max , TSR max , and MTV). The curve slope was the sole dynamic PET predictor of glioma recurrence/progression (accuracy = 76.5%) and was also associated with mean PFS (p < 0.001, 18.0 vs. 0.4 months). However, no additional information was provided relative to static parameters in multivariate analysis., Conclusion: Although patients with glioma recurrence/progression can be detected by both static and dynamic [ 18 F]-F-DOPA PET parameters, most of this diagnostic information can be achieved by conventional static parameters.

Published

2020

50. Ki-67 and MCM6 labeling indices are correlated with overall survival in anaplastic oligodendroglioma, IDH1-mutant and 1p/19q-codeleted: a multicenter study from the French POLA network.

Author

Pouget C, Hergalant S, Lardenois E, Lacomme S, Houlgatte R, Carpentier C, Dehais C, Rech F, Taillandier L, Sanson M, Appay R, Colin C, Figarella-Branger D, Battaglia-Hsu SF, and Gauchotte G

Subjects

Adult, Aged, Aged, 80 and over, Brain Neoplasms genetics, Brain Neoplasms mortality, Brain Neoplasms pathology, Female, France, Gene Expression Profiling, Humans, Isocitrate Dehydrogenase metabolism, Male, Middle Aged, Mitotic Index, Oligodendroglioma genetics, Oligodendroglioma mortality, Oligodendroglioma pathology, Prognosis, Survival Rate, Young Adult, Brain Neoplasms metabolism, Gene Deletion, Isocitrate Dehydrogenase genetics, Ki-67 Antigen metabolism, Minichromosome Maintenance Complex Component 6 metabolism, Mutation, Oligodendroglioma metabolism

Abstract

Anaplastic oligodendroglioma (AO), IDH-mutant and 1p/19q codeleted (IDHmut+/1p19qcodel), is a high-grade glioma with only limited prognostic markers. The primary objective of this study was to evaluate, by immunohistochemistry, the prognostic value of two proliferation markers, MCM6 and Ki-67, in a large series of IDHmut+/1p19qcodel AO included in the POLA ("Prise en charge des Oligodendrogliomes Anaplasiques") French national multicenter network. We additionally examined the transcriptome obtained from this series to understand the functional pathways dysregulated with the mRNA overexpression of these two markers. The labeling indices (LI) of MCM6 and Ki-67 were obtained via computer-assisted color image analyses on immunostained AO tissues of the cohort (n = 220). Furthermore, a subgroup of AO (n = 68/220) was used to perform transcriptomic analyses. A high LI of either MCM6 (≥50%) or Ki-67 (≥15%) correlated with shorter overall survival, both in univariate (P = 0.013 and P = 0.004, respectively) and multivariate analyses (P = 0.027; multivariate Cox model including age, mitotic index, MCM6 and Ki-67). MCM6 and Ki-67 LI also correlated with overall survival in an additional retrospective cohort of 30 grade II IDHmut+/1p19qcodel oligodendrogliomas. The prognostic value of MCM6 mRNA level was confirmed in The Cancer Genome Atlas (TCGA) IDHmut+/1p19qcodel gliomas. The transcriptomic approach revealed that high transcriptional expressions of MCM6 and MKI67 were both linked positively with cell cycle progression, DNA replication, mitosis, pro-neural phenotype as well as neurogenesis, and negatively with microglial cell activation, immune response, positive regulation of myelination, oligodendrocyte development, beta-amyloid binding and postsynaptic specialization. In conclusion, the overexpression of MCM6 and/or Ki-67 is independently associated to shorter overall survival in IDHmut+/1p19qcodel AO. These two easy-to-use and cost-effective markers could thus be used concurrently in routine pathology practice. Additionally, the transcriptomic analyses showed that AO with high proliferation index have down-regulated immune response and lower microglial cells activation, and bears pro-neural phenotype., (© 2019 International Society of Neuropathology.)

Published

2020