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3. Additional file 1 of Dermatologic manifestations in paediatric neurofibromatosis type 2: a cross sectional descriptive multicentric study

Author

Legoupil, S., Bessis, D., Picard, F., Mallet, S., Mazereeuw, J., Phan, A., Dupin-Deguine, D., Kalamarides, M., and Chiaverini, C.

Abstract

Additional file 1: Characteristics of the population, genetic data, and dermatological, ophthalmological, neurological and otolaringeal (ENT) features. yo: years-old; d: deceased; ND: not done; M: male; F: female; CALMs : Café-Au-Lait Macules; HPMs : Hypopigmented Macules.

Published
2022
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8. Surgery of the lateral skull base: A 50-year endeavour

Author

Zanoletti, E., Mazzoni, Alberto, Martini, A., Abbritti, R. V., Albertini, R., Alexandre, E., Baro, V., Bartolini, S., Bernardeschi, D., Bivona, R., Bonali, M., Borghesi, I., Borsetto, D., Bovo, R., Breun, M., Calbucci, F., Carlson, M. L., Caruso, A., Caye-Thomasen, P., Cazzador, D., Champagne, P. -O., Colangeli, R., Conte, G., D'Avella, D., Danesi, G., Deantonio, L., Denaro, L., Berardino, F. D., Draghi, R., Ebner, F. H., Favaretto, N., Ferri, G., Fioravanti, A., Froelich, S., Giannuzzi, A., Girasoli, L., Grossardt, B. R., Guidi, M., Hagen, R., Hanakita, S., Hardy, D. G., Iglesias, V. C., Jefferies, S., Jia, H., Kalamarides, M., Kanaan, I. N., Krengli, M., Landi, A., Lauda, L., Lepera, D., Lieber, S., Lloyd, S. L. K., Lovato, A., Maccarrone, F., Macfarlane, R., Magnan, J., Magnoni, L., Marchioni, D., Marinelli, J. P., Marioni, G., Mastronardi, V., Matthies, C., Moffat, D. A., Munari, S., Nardone, M., Pareschi, R., Pavone, C., Piccirillo, E., Piras, G., Presutti, L., Restivo, G., Reznitsky, M., Roca, E., Russo, A., Sanna, M., Sartori, L., Scheich, M., Shehata-Dieler, W., Soloperto, D., Sorrentino, F., Sterkers, O., Taibah, A., Tatagiba, M., Tealdo, G., Vlad, D., Wu, H., Zanetti, D., Zanoletti E., Mazzoni A., Martini A., Abbritti R.V., Albertini R., Alexandre E., Baro V., Bartolini S., Bernardeschi D., Bivona R., Bonali M., Borghesi I., Borsetto D., Bovo R., Breun M., Calbucci F., Carlson M.L., Caruso A., Caye-Thomasen P., Cazzador D., Champagne P.-O., Colangeli R., Conte G., D'Avella D., Danesi G., Deantonio L., Denaro L., Berardino F.D., Draghi R., Ebner F.H., Favaretto N., Ferri G., Fioravanti A., Froelich S., Giannuzzi A., Girasoli L., Grossardt B.R., Guidi M., Hagen R., Hanakita S., Hardy D.G., Iglesias V.C., Jefferies S., Jia H., Kalamarides M., Kanaan I.N., Krengli M., Landi A., Lauda L., Lepera D., Lieber S., Lloyd S.L.K., Lovato A., Maccarrone F., Macfarlane R., Magnan J., Magnoni L., Marchioni D., Marinelli J.P., Marioni G., Mastronardi V., Matthies C., Moffat D.A., Munari S., Nardone M., Pareschi R., Pavone C., Piccirillo E., Piras G., Presutti L., Restivo G., Reznitsky M., Roca E., Russo A., Sanna M., Sartori L., Scheich M., Shehata-Dieler W., Soloperto D., Sorrentino F., Sterkers O., Taibah A., Tatagiba M., Tealdo G., Vlad D., Wu H., and Zanetti D.

Subjects
Male, medicine.medical_treatment, Schwannoma, Neurosurgical Procedures, Cohort Studies, 0302 clinical medicine, Meningeal Neoplasms, Medicine, 030223 otorhinolaryngology, Skull Base, Benign tumors of the skull base, Lateral approaches to the skull base, Malignant tumors of the skull base, Neuroma, Acoustic, Middle Aged, Magnetic Resonance Imaging, 3. Good health, Chirurgia della base cranio laterale, General Energy, medicine.anatomical_structure, Approcci laterali alla base del cranio, 030220 oncology & carcinogenesis, Head and neck surgery, Female, Neurosurgery, Meningioma, Research Article, Adult, Chirurgia della base del cranio, medicine.medical_specialty, Tumori benigni della base del cranio, Lateral skull base surgery, Tumori maligni della base del cranio, Skull Base Neoplasms, Skull base surgery, Aged, Endoscopy, Hearing Loss, Humans, Mastoid, Retrospective Studies, Temporal Bone, Young Adult, 03 medical and health sciences, otorhinolaryngologic diseases, business.industry, General surgery, medicine.disease, Radiation therapy, Skull, Otorhinolaryngology, business, Jugular foramen
Abstract

Chirurgia della base del cranio laterale: 50 anni di impegno.La base del cranio non è anatomicamente divisa in anteriore e laterale, ma è per semplicità che comunemente si intendono i corridoi chirurgici con direzione antero-laterale, laterale pura e postero laterale come “Approcci chirurgici della base del cranio laterale”. Una relazione con titolo “Cinquant’anni di impegno”, di sforzo o di dedizione, vuole essere il riconoscimento a questa chirurgia che nel corso degli anni ha sviluppato interventi sempre più complessi con una morbidità sempre minore. Il principio della chirurgia della base del cranio laterale si fonda sulla possibilità di “fare spazio”, esporre adeguatamente, rimuovere osso per salvaguardare il cervello, insieme alla possibilità di preservare la funzione e adattare l’approccio chirurgico all’istologia della lesione. Il concetto che l’istologia detta l’entità della resezione chirurgica, bilanciando la morbidità intrinseca di ciascun approccio, è oggetto di trattazione nella prima sezione di questa relazione. Nella seconda sezione sono descritti i principali approcci chirurgici, intesi non come descrizione tecnica di ciascun tempo chirurgico, ma dei principi che sono alla base di ciascun approccio. La terza sezione è dedicata alle questioni aperte, quelle ancora irrisolte, inerenti alcuni tumori ed il loro trattamento. L’argomento del neurinoma sporadico dell’ottavo nervo cranico è trattato riportando l'attuale dibattito sulla osservazione, la chirurgia di preservazione dell’udito, la riabilitazione con l’impianto cocleare, la radioterapia e le ricerche recenti su marcatori tumorali predittivi di crescita. Il paraganglioma del forame giugulare è trattato nel contesto della chirurgia radicale, chirurgia parziale, osservazione e radioterapia. La terapia dei meningiomi della base del cranio analizza il punto di vista specifico dell’otochirurgo e del neurochirurgo. Cordomi e condrosarcomi, tumori del sacco endolinfatico, carcinomi dell’orecchio e colesteatoma della rocca sono le altre lesioni affrontate. Infine, nella quarta sezione è proposto un contributo a libera scelta ad autori di riconosciuta esperienza. Lo scopo di questa relazione è stato quello di fornire un aggiornamento della chirurgia della base del cranio laterale dopo 50 anni di duro lavoro e, o forse soprattutto, di permettere alle tante questioni irrisolte, alle domande che ancora non hanno risposta, di trovare espressione, affinchè il dibattito ed il progresso possano continuare con la condivisione di esperienze. Se al termine della lettura vi saranno più domande che risposte, potremo dirci che l’obiettivo di questa relazione è stato raggiunto.Disregarding the widely used division of skull base into anterior and lateral, since the skull base should be conceived as a single anatomic structure, it was to our convenience to group all those approaches that run from the antero-lateral, pure lateral and postero-lateral side of the skull base as “Surgery of the lateral skull base”. “50 years of endeavour” points to the great effort which has been made over the last decades, when more and more difficult surgeries were performed by reducing morbidity. The principle of lateral skull base surgery, “remove skull base bone to approach the base itself and the adjacent sites of the endo-esocranium”, was then combined with function preservation and with tailoring surgery to the pathology. The concept that histology dictates the extent of resection, balancing the intrinsic morbidity of each approach was the object of the first section of the present report. The main surgical approaches were described in the second section and were conceived not as a step-by-step description of technique, but as the highlighthening of the surgical principles. The third section was centered on open issues related to the tumor and its treatment. The topic of vestibular schwannoma was investigated with the current debate on observation, hearing preservation surgery, hearing rehabilitation, radiotherapy and the recent efforts to detect biological markers able to predict tumor growth. Jugular foramen paragangliomas were treated in the frame of radical or partial surgery, radiotherapy, partial “tailored” surgery and observation. Surgery on meningioma was debated from the point of view of the neurosurgeon and of the otologist. Endolymphatic sac tumors and malignant tumors of the external auditory canal were also treated, as well as chordomas, chondrosarcomas and petrous bone cholesteatomas. Finally, the fourth section focused on free-choice topics which were assigned to aknowledged experts. The aim of this work was attempting to report the state of the art of the lateral skull base surgery after 50 years of hard work and, above all, to raise questions on those issues which still need an answer, as to allow progress in knowledge through sharing of various experiences. At the end of the reading, if more doubts remain rather than certainties, the aim of this work will probably be achieved.

Published
2019

10. Surgery of the lateral skull base:A 50-year endeavour

Author

Zanoletti, E., Mazzoni, A., Martini, A., Abbritti, R. V., Albertini, R., Alexandre, E., Baro, V., Bartolini, S., Bernardeschi, D., Bivona, R., Bonali, M., Borghesi, I., Borsetto, D., Bovo, R., Breun, M., Calbucci, F., Carlson, M. L., Caruso, A., Cayé-Thomasen, P., Cazzador, D., Champagne, P. O., Colangeli, R., Conte, G., D’Avella, D., Danesi, G., Deantonio, L., Denaro, L., Berardino, F. Di, Draghi, R., Ebner, F. H., Favaretto, N., Ferri, G., Fioravanti, A., Froelich, S., Giannuzzi, A., Girasoli, L., Grossardt, B. R., Guidi, M., Hagen, R., Hanakita, S., Hardy, D. G., Iglesias, V. C., Jefferies, S., Jia, H., Kalamarides, M., Kanaan, I. N., Krengli, M., Landi, A., Lauda, L., Lepera, D., Lieber, S., Lloyd, S. L.K., Lovato, A., Maccarrone, F., Macfarlane, R., Magnan, J., Magnoni, L., Marchioni, D., Marinelli, J. P., Marioni, G., Mastronardi, V., Matthies, C., Moffat, D. A., Munari, S., Nardone, M., Pareschi, R., Pavone, C., Piccirillo, E., Piras, G., Presutti, L., Restivo, G., Reznitsky, M., Roca, E., Russo, A., Sanna, M., Sartori, L., Scheich, M., Shehata-Dieler, W., Soloperto, D., Sorrentino, F., Sterkers, O., Taibah, A., Tatagiba, M., Tealdo, G., Vlad, D., Wu, H., and Zanetti, D.

Subjects
Benign tumors of the skull base, Lateral approaches to the skull base, otorhinolaryngologic diseases, Lateral skull base surgery, Malignant tumors of the skull base, Skull base surgery
Abstract

Disregarding the widely used division of skull base into anterior and lateral, since the skull base should be conceived as a single anatomic structure, it was to our convenience to group all those approaches that run from the antero-lateral, pure lateral and postero-lateral side of the skull base as “Surgery of the lateral skull base”. “50 years of endeavour” points to the great effort which has been made over the last decades, when more and more difficult surgeries were performed by reducing morbidity. The principle of lateral skull base surgery, “remove skull base bone to approach the base itself and the adjacent sites of the endo-esocranium”, was then combined with function preservation and with tailoring surgery to the pathology. The concept that histology dictates the extent of resection, balancing the intrinsic morbidity of each approach was the object of the first section of the present report. The main surgical approaches were described in the second section and were conceived not as a step-by-step description of technique, but as the highlighthening of the surgical principles. The third section was centered on open issues related to the tumor and its treatment. The topic of vestibular schwannoma was investigated with the current debate on observation, hearing preservation surgery, hearing rehabilitation, radiotherapy and the recent efforts to detect biological markers able to predict tumor growth. Jugular foramen paragangliomas were treated in the frame of radical or partial surgery, radiotherapy, partial “tailored” surgery and observation. Surgery on meningioma was debated from the point of view of the neurosurgeon and of the otologist. Endolymphatic sac tumors and malignant tumors of the external auditory canal were also treated, as well as chordomas, chondrosarcomas and petrous bone cholesteatomas. Finally, the fourth section focused on free-choice topics which were assigned to aknowledged experts. The aim of this work was attempting to report the state of the art of the lateral skull base surgery after 50 years of hard work and, above all, to raise questions on those issues which still need an answer, as to allow progress in knowledge through sharing of various experiences. At the end of the reading, if more doubts remain rather than certainties, the aim of this work will probably be achieved.

Published
2019

14. Surgery of the lateral skull base: a 50-year endeavour

Author

Zanoletti, E., primary, Mazzoni, A., additional, Martini, A., additional, Abbritti, R. V., additional, Albertini, R., additional, Alexandre, E., additional, Baro, V., additional, Bartolini, S., additional, Bernardeschi, D., additional, Bivona, R., additional, Bonali, M., additional, Borghesi, I., additional, Borsetto, D., additional, Bovo, R., additional, Breun, M., additional, Calbucci, F., additional, Carlson, M. L., additional, Caruso, A., additional, Cayé-Thomasen, P., additional, Cazzador, D., additional, Champagne, P. -O., additional, Colangeli, R., additional, Conte, G., additional, D’Avella, D., additional, Danesi, G., additional, Deantonio, L., additional, Denaro, L., additional, Di Berardino, F., additional, Draghi, R., additional, Ebner, F. H., additional, Favaretto, N., additional, Ferri, G., additional, Fioravanti, A., additional, Froelich, S., additional, Giannuzzi, A., additional, Girasoli, L., additional, Grossardt, B. R., additional, Guidi, M., additional, Hagen, R., additional, Hanakita, S., additional, Hardy, D. G., additional, Iglesias, V. C., additional, Jefferies, S., additional, Jia, H., additional, Kalamarides, M., additional, Kanaan, I. N., additional, Krengli, M., additional, Landi, A., additional, Lauda, L., additional, Lepera, D., additional, Lieber, S., additional, Lloyd, S. L. K., additional, Lovato, A., additional, Maccarrone, F., additional, Macfarlane, R., additional, Magnan, J., additional, Magnoni, L., additional, Marchioni, D., additional, Marinelli, J. P., additional, Marioni, G., additional, Mastronardi, V., additional, Matthies, C., additional, Moffat, D. A., additional, Munari, S., additional, Nardone, M., additional, Pareschi, R., additional, Pavone, C., additional, Piccirillo, E., additional, Piras, G., additional, Presutti, L., additional, Restivo, G., additional, Reznitsky, M., additional, Roca, E., additional, Russo, A., additional, Sanna, M., additional, Sartori, L., additional, Scheich, M., additional, Shehata-Dieler, W., additional, Soloperto, D., additional, Sorrentino, F., additional, Sterkers, O., additional, Taibah, A., additional, Tatagiba, M., additional, Tealdo, G., additional, Vlad, D., additional, Wu, H., additional, and Zanetti, D., additional

Published
2019
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15. Surgical treatment of sporadic vestibular schwannoma in a series of 1006 patients

Author

Zhang Z, Nguyen Y, Daniele De Seta, Fy, Russo, Rey A, Kalamarides M, Sterkers O, Bernardeschi D, CHU Pitié-Salpêtrière [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Xinhua Hospital Shanghai Jiaotong Univerrsity School of Medicine, Hôpital Beaujon, Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Université Paris Diderot - Paris 7 (UPD7)-Hôpital Beaujon [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Université Pierre et Marie Curie - Paris 6 (UPMC), Unité d’Otologie, implants auditifs et chirurgie de la base du crâne [CHU Pitié-Salpêtrière], Service d'Oto-Rhino-Laryngologie [CHU Pitié-Salpêtrière], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-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), Hôpital Beaujon [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Université Paris Diderot - Paris 7 (UPD7), Service de Neurochirurgie [CHU Pitié-Salpêtrière], Service d'Otologie, Implants auditifs et Chirurgie de la base du crâne [CHU Pitié-Salpêtrière], Assistance publique - Hôpitaux de Paris (AP-HP) (APHP)-CHU Pitié-Salpêtrière [APHP], and Assistance publique - Hôpitaux de Paris (AP-HP) (APHP)-Université Paris Diderot - Paris 7 (UPD7)-Hôpital Beaujon

Subjects
Hearing levels, Male, Time Factors, Otology, Neuroma, Acoustic, Middle Aged, Facial nerve, Vestibular schwannoma, Postoperative Complications, Treatment Outcome, Translabyrinthine, Humans, Female, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology, Retrospective Studies
Abstract

International audience; The management of sporadic vestibular schwannoma (VS) has evolved in the last decades. The aim of this study was to analyse the evolution in surgical outcomes of VSs operated by a neurotological team between 1990 and 2006 by different approaches. A monocentric retrospective review of medical charts of 1006 patients was performed. In order to assess eventual changes and progress, the 17-years period was divided in three periods, each one comprehending 268 VS (1990-1996), 299 VS (1997-2001), and 439 VS (2002-2006). Mean follow-up was 5.9 ± 2.4 years. Overall, complete VS removal was achieved in 99.4% of cases. Mortality rate was 0.3%, meningitis and CSF leaks were observed in 1.2 % and 9 % of the cases, respectively. CSF leakage decreased from 11.6% to 7.1% between the first and last period (p < 0.01) as well as revision surgery from 3.4 % to 0.9 % (p < 0.05). Facial nerve was anatomically preserved in 97.7% of cases. At one year, a good facial nerve function was observed in 85.1% of patients (grade I and II of House-Brackmann grading scale), which ranged between the first and last period from 78.4% to 87.6% (p

Published
2016

17. PDGF activation in PGDS-positive arachnoid cells induces meningioma formation in mice promoting tumor progression in combination with Nf2 and Cdkn2ab loss

Author

Peyre, M, Salaud, C, Clermont-Taranchon, E, Niwa-Kawakita, M, Goutagny, S, Mawrin, C, Giovannini, M, and Kalamarides, M

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, Time Factors, Cells, mouse model, Oncology and Carcinogenesis, Inbred C57BL, Cell Transformation, Transfection, meningioma, Transgenic, Mice, Rare Diseases, RCAS, Nf2, otorhinolaryngologic diseases, Meningeal Neoplasms, 2.1 Biological and endogenous factors, Animals, Humans, Aetiology, neoplasms, Cyclin-Dependent Kinase Inhibitor p16, Cancer, Retrospective Studies, Cell Proliferation, Cyclin-Dependent Kinase Inhibitor p15, Neoplastic, Cultured, Neurosciences, Proto-Oncogene Proteins c-sis, PDGF, Platelet-Derived Growth Factor beta, Lipocalins, Brain Disorders, nervous system diseases, Brain Cancer, Intramolecular Oxidoreductases, Gene Expression Regulation, Arachnoid, Neoplasm Grading, Receptor, Signal Transduction
Abstract

The role of PDGF-B and its receptor in meningeal tumorigenesis is not clear. We investigated the role of PDGF-B in mouse meningioma development by generating autocrine stimulation of the arachnoid through the platelet-derived growth factor receptor (PDGFR) using the RCAStv-a system. To specifically target arachnoid cells, the cells of origin of meningioma, we generated the PGDStv-a mouse (Prostaglandin D synthase). Forced expression of PDGF-B in arachnoid cells in vivo induced the formation of Grade I meningiomas in 27% of mice by 8 months of age. In vitro, PDGF-B overexpression in PGDS-positive arachnoid cells lead to increased proliferation. We found a correlation of PDGFR-B expression and NF2 inactivation in a cohort of human meningiomas, and we showed that, in mice, Nf2 loss and PDGF overexpression in arachnoid cells induced meningioma malignant transformation, with 40% of Grade II meningiomas. In these mice, additional loss of Cdkn2ab resulted in a higher incidence of malignant meningiomas with 60% of Grade II and 30% of Grade III meningiomas. These data suggest that chronic autocrine PDGF signaling can promote proliferation of arachnoid cells and is potentially sufficient to induce meningiomagenesis. Loss of Nf2 and Cdkn2ab have synergistic effects with PDGF-B overexpression promoting meningioma malignant transformation.

Published
2015

18. Phase II study of mTORC1 inhibition by everolimus in neurofibromatosis type 2 patients with growing vestibular schwannomas

Author

Goutagny, S, Raymond, E, Esposito-Farese, M, Trunet, S, Mawrin, C, Bernardeschi, D, Larroque, B, Sterkers, O, Giovannini, M, and Kalamarides, M

Subjects
otorhinolaryngologic diseases
Abstract

© 2015 Springer Science+Business Media New York Neurofibromatosis type 2 (NF2) is a genetic disorder with bilateral vestibular schwannomas (VS) as the most frequent manifestation. Merlin, the NF2 tumor suppressor, was identified as a negative regulator of mammalian target of rapamycin complex 1. Pre-clinical data in mice showed that mTORC1 inhibition delayed growth of NF2-schwannomas. We conducted a prospective single-institution open-label phase II study to evaluate the effects of everolimus in ten NF2 patients with progressive VS. Drug activity was monitored every 3 months. Everolimus was administered orally for 12 months and, if the decrease in tumor volume was >20 % from baseline, treatment was continued for 12 additional months. Other patients stopped when completed 12 months of everolimus but were allowed to resume treatment when VS volume was >20 % during 1 year follow-up. Nine patients were evaluable. Safety was evaluated using CTCAE 3.0 criteria. After 12 months of everolimus, no reduction in volume ≥20 % was observed. Four patients had progressive disease, and five patients had stable disease with a median annual growth rate decreasing from 67 %/year before treatment to 0.5 %/year during treatment. In these patients, tumor growth resumed within 3–6 months after treatment discontinuation. Everolimus was then reintroduced and VS decreased by a median 6.8 % at 24 months. Time to tumor progression increased threefold from 4.2 months before treatment to > 12 months. Hearing was stable under treatment. The safety of everolimus was manageable. Although the primary endpoint was not reached, further studies are required to confirm the potential for stabilization of everolimus.

Published
2015

19. ACTA OTORHINOLARYNGOLOGICA ITALICA

Author

Zhang, Z., primary, Nguyen, Y., additional, De Seta, D., additional, Russo, F.Y., additional, Rey, A., additional, Kalamarides, M., additional, Sterkers, O., additional, and Bernardeschi, D., additional

Published
2016
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24. report of 90 personal cases

Author

Sollmann, WP, Laszig, R, Sterkers, O, Rey, A, and Kalamarides, M

Subjects
ddc: 610
Published
2005

27. Neurofibromatosis 2011: a report of the Children's Tumor Foundation annual meeting.

Author

Kalamarides, M, Acosta, MT, Babovic-Vuksanovic, D, Carpen, O, Cichowski, K, Evans, DG, Giancotti, F, Hanemann, CO, Ingram, D, Lloyd, AC, Mayes, DA, Messiaen, L, Morrison, H, North, K, Packer, R, Pan, D, Stemmer-Rachamimov, A, Upadhyaya, M, Viskochil, D, Wallace, MR, Hunter-Schaedle, K, Ratner, N, Kalamarides, M, Acosta, MT, Babovic-Vuksanovic, D, Carpen, O, Cichowski, K, Evans, DG, Giancotti, F, Hanemann, CO, Ingram, D, Lloyd, AC, Mayes, DA, Messiaen, L, Morrison, H, North, K, Packer, R, Pan, D, Stemmer-Rachamimov, A, Upadhyaya, M, Viskochil, D, Wallace, MR, Hunter-Schaedle, K, and Ratner, N

Abstract

The 2011 annual meeting of the Children's Tumor Foundation, the annual gathering of the neurofibromatosis (NF) research and clinical communities, was attended by 330 participants who discussed integration of new signaling pathways into NF research, the appreciation for NF mutations in sporadic cancers, and an expanding pre-clinical and clinical agenda. NF1, NF2, and schwannomatosis collectively affect approximately 100,000 persons in US, and result from mutations in different genes. Benign tumors of NF1 (neurofibroma and optic pathway glioma) and NF2 (schwannoma, ependymoma, and meningioma) and schwannomatosis (schwannoma) can cause significant morbidity, and there are no proven drug treatments for any form of NF. Each disorder is associated with additional manifestations causing morbidity. The research presentations described in this review covered basic science, preclinical testing, and results from clinical trials, and demonstrate the remarkable strides being taken toward understanding of and progress toward treatments for these disorders based on the close interaction among scientists and clinicians.

Published
2012

33. Corticosteroid Effect on Facial Function after Cerebellopontine Angle Tumor Resection: A Double-Blind Study versus Placebo

Author

Bozorg Grayeli, A., primary, Ferrary, E., additional, Tubach, F., additional, Bernat, I., additional, Deguine, O., additional, Darrouzet, V., additional, Robier, A., additional, Zaouche, S., additional, Dubreuil, C., additional, Marx, M., additional, Kalamarides, M., additional, Fraysse, B., additional, and Sterkers, O., additional

Published
2012
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36. Human glioma cells transformed by IGF-I triple helix technology show immune and apoptotic characteristics determining cell selection for gene therapy of glioblastoma

Author

Henin, D., Ly, A., Anthony, D.D., Duc, H.T., Trojan, J., Kalamarides, M., Trojan, L.A., Pan, Y., Shevelev, A., Francois, J-C., Noel, T., and Kane, A.

Abstract

Aims--Insulin-like growth factor type I (IGF-I) antisense cellular gene therapy of tumours is based on the following data: rat glioma or hepatoma cells transfected with the vector encoding IGF-I antisense cDNA lose their tumorigenicity and induce a tumour specific immune response involving CD8+ T cells. Recently, using the IGF-I triple helix approach in studies of tumorigenicity, major histocompatibility complex class I (MHC-I) antigens were demonstrated in rat glioma transfected cells. This study used comparative IGF-I antisense and triple helix technologies in human primary glioma cells to determine the triple helix strategy that would be most appropriate for the treatment of glioblastoma.Methods--The cells were transfected using the IGF-I triple helix expression vector, pMT-AG, derived from the pMT-EP vector. pMT-AG contains a cassette comprising a 23 bp DNA fragment transcribing a third RNA strand, which forms a triple helix structure within a target region of the human IGF-I gene. Using pMT-EP, vectors encoding MHC-I or B7 antisense cDNA were also constructed.Results--IGF-I triple helix transfected glioma cells are characterised by immune and apoptotic phenomena that appear to be related. The expression of MHC-I and B7 in transfected cells (analysed by flow cytometry) was accompanied by programmed cell death (detected by dUTP fluorescein terminal transferase labelling of nicked DNA and electron microscopic techniques). Cotransfection of these cells with MHC-I and B7 antisense vectors suppressed the expression of MHC-I and B7, and was associated with a pronounced decrease in apoptosis.Conclusion--When designing an IGF-I triple helix strategy for the treatment of human glioblastoma, the transfected tumour cells should have the following characteristics: the absence of IGF-I, thepresence of both MHC-I and B7 molecules, and signs of apoptosis.

Published
2001

37. Tumor biological characteristics of Vestibular Schwannoma

Author

Vries, M. de, Hogendoorn, P.C.W., Mey, A.G.L. van der, Benthem, P.P.G. van, Marijnen, C.A.M., Kalamarides, M., Sciot, R., and Leiden University

Subjects
Inflammation, Targeted therapy, Tumor biology, Vestibular schwannoma, otorhinolaryngologic diseases, Growth
Abstract

The aim of this thesis is to shed light on the biological background of progression of sporadic vestibular schwannomas. The results of our studies indicate that, in different ways, intratumoral inflammation seems to be important in the clinical progression of these tumors. By stimulating angiogenesis and through inhibition of antitumor immune responses tumor associated macrophages may allow some tumors to progress faster and reach a larger volume.M-CSF and IL-34 may play a regulatory role when it comes to macrophage activity within vestibular schwannomas, thereby potentially making them targets for therapy. These outcomes must be interpreted with caution. It is important to note that the results of the comparisons we made are observations of association. There is always the possibility that these findings are epiphenomena of a larger biological growth process and therefore not directly related to one another.In the search for new drugs capable of targeting tumor biological factors involved in the progression of vestibular schwannomas it is important to realize that our findings also indicate that these tumors may be protected by barrier proteins such as BCRP.

Published
2019

38. Monitoring Cochlear Nerve Action Potential for Hearing Preservation in Medium/Large Vestibular Schwannoma Surgery: Tips and Pitfalls.

Author

Hochet B, Daoudi H, Lefevre E, Nguyen Y, Bernat I, Sterkers O, Lahlou G, and Kalamarides M

Abstract

The diagnosis of large vestibular schwannomas (VS) with retained useful hearing has become increasingly common. Preservation of facial nerve (FN) function has improved using intraoperative EMG monitoring, hearing preservation remains challenging, with the recent use of cochlear nerve action potential (CNAP) monitoring. This prospective longitudinal series of VS with useful hearing operated on using a retrosigmoid approach included 37 patients with a mean largest extrameatal VS. diameter of 25 ± 8.7 mm (81% of Koos stage 4). CNAP was detected in 51% of patients, while auditory brainstem responses (ABR) were present in 22%. Patients were divided into two groups based on the initial intraoperative CNAP status, whether it was present or absent. FN function was preserved (grade I-II) in 95% of cases at 6 months. Serviceable hearing (class A + B) was preserved in 16% of the cases, while 27% retained hearing with intelligibility (class A-C). Hearing with intelligibility (class A-C) was preserved in 42% of cases when CNAP could be monitored in the early stages of VS resection versus 11% when it was initially absent. Changes in both the approach to the cochlear nerve and VS resection are mandatory in preserving CNAP and improve the rate of hearing preservation.

Published
2023
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39. Super-enhancer hijacking drives ectopic expression of hedgehog pathway ligands in meningiomas.

Author

Youngblood MW, Erson-Omay Z, Li C, Najem H, Coșkun S, Tyrtova E, Montejo JD, Miyagishima DF, Barak T, Nishimura S, Harmancı AS, Clark VE, Duran D, Huttner A, Avşar T, Bayri Y, Schramm J, Boetto J, Peyre M, Riche M, Goldbrunner R, Amankulor N, Louvi A, Bilgüvar K, Pamir MN, Özduman K, Kilic T, Knight JR, Simon M, Horbinski C, Kalamarides M, Timmer M, Heimberger AB, Mishra-Gorur K, Moliterno J, Yasuno K, and Günel M

Subjects
Humans, Hedgehog Proteins genetics, Hedgehog Proteins metabolism, Ligands, Signal Transduction, Meningioma genetics, Meningeal Neoplasms genetics
Abstract

Hedgehog signaling mediates embryologic development of the central nervous system and other tissues and is frequently hijacked by neoplasia to facilitate uncontrolled cellular proliferation. Meningiomas, the most common primary brain tumor, exhibit Hedgehog signaling activation in 6.5% of cases, triggered by recurrent mutations in pathway mediators such as SMO. In this study, we find 35.6% of meningiomas that lack previously known drivers acquired various types of somatic structural variations affecting chromosomes 2q35 and 7q36.3. These cases exhibit ectopic expression of Hedgehog ligands, IHH and SHH, respectively, resulting in Hedgehog signaling activation. Recurrent tandem duplications involving IHH permit de novo chromatin interactions between super-enhancers within DIRC3 and a locus containing IHH. Our work expands the landscape of meningioma molecular drivers and demonstrates enhancer hijacking of Hedgehog ligands as a route to activate this pathway  in neoplasia., (© 2023. Springer Nature Limited.)

Published
2023
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40. The clinical, genetic, and immune landscape of meningioma in patients with NF2-schwannomatosis.

Author

Gregory GE, Islim AI, Hannan CJ, Jones AP, Hammerbeck-Ward C, Rutherford SA, Freeman SR, Lloyd S, Kalamarides M, Smith MJ, Couper K, McBain CA, Jenkinson MD, Brough D, King AT, Evans DG, and Pathmanaban ON

Abstract

NF2-schwannomatosis is the most common genetic predisposition syndrome associated with meningioma. Meningioma in NF2-schwannomatosis is a major source of morbidity and mortality. This is due to accumulative tumor burden in patients with synchronous schwannomas and ependymomas, sometimes including complex collision tumors. Balancing the impact of multiple interventions against the natural history of various index tumors, and the ongoing risk of de novo tumors over an individual's lifetime makes decision-making complex. The management of any given individual meningioma is often different from a comparable sporadic tumor. There is typically a greater emphasis on conservative management and tolerating growth until a risk boundary is reached, whereby symptomatic deterioration or higher risk from anticipated future treatment is threatened. Management by high-volume multidisciplinary teams improves quality of life and life expectancy. Surgery remains the mainstay treatment for symptomatic and rapidly enlarging meningioma. Radiotherapy has an important role but carries a higher risk compared to its use in sporadic disease. Whilst bevacizumab is effective in NF2-associated schwannoma and cystic ependymoma, it has no value in the management of meningioma. In this review, we describe the natural history of the disease, underlying genetic, molecular, and immune microenvironment changes, current management paradigms, and potential therapeutic targets., Competing Interests: G.E.G., A.P.J., K.C., D.B., and O.N.P. have received funding from NF2 BioSolutions UK. A.I.I. is supported by the NIHR Academic Clinical Fellowship Scheme. C.J.H., A.T.K., and O.N.P. are funded by Eleanor Peel Trust, the Royal College of Surgeons of Edinburgh, and the BMA Foundation. S. L. and D.G.E. are supported by the Manchester NIHR Biomedical Research Centre (IS-BRC-1215-20007). O.N.P. is UK Chief Investigator for Recursion Pharma Rec 2282 phase II/III RCT in NF2 mutated meningioma; A.I.I. is sub principal investigator. Supplement sponsorship. This supplement was sponsored by a generous donation from Mr. Paul Mielnik and his family to help raise awareness and advance the care of patients with meningiomas worldwide., (© The Author(s) 2023. Published by Oxford University Press, the Society for Neuro-Oncology and the European Association of Neuro-Oncology.)

Published
2023
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41. Prospective phase II trial of the dual mTORC1/2 inhibitor vistusertib for progressive or symptomatic meningiomas in persons with neurofibromatosis 2.

Author

Jordan JT, Orr CC, Thalheimer RD, Cambillo JV, Beauchamp RL, Shaikh G, Muzikansky A, Stemmer-Rachamimov A, Giovannini M, Kalamarides M, Barker FG 2nd, Ramesh V, and Plotkin SR

Abstract

Background: Meningiomas occur in 80% of persons with neurofibromatosis 2 (NF2) and cause significant mortality and morbidity, yet there are no effective medical treatments. NF2 -deficient tumors have constitutive activation of mammalian/mechanistic target of rapamycin (mTOR), and treatment with mTORC1 inhibitors results in growth arrest in a minority of tumors, with paradoxical activation of the mTORC2/AKT pathway. We studied the effect of vistusertib, a dual mTORC1/mTORC2 inhibitor, in NF2 patients with progressive or symptomatic meningiomas., Methods: Vistusertib was administered orally at 125 mg twice daily for 2 consecutive days each week. The primary endpoint was the imaging response in the target meningioma, defined as a volume decrease of 20% compared with the baseline. Secondary endpoints included toxicity, imaging response of nontarget tumors, quality of life, and genetic biomarkers., Results: Eighteen participants (13 female), median age of 41 (range, 18-61) years, were enrolled. In target meningiomas, the best response was partial response (PR) in 1/18 tumors (6%) and stable disease (SD) in 17/18 tumors (94%). For all measured intracranial meningiomas and vestibular schwannomas, the best imaging response was PR in 6/59 tumors (10%) and SD in 53 (90%). Treatment-related grade 3/4 adverse events occurred in 14 (78%) participants, and 9 participants discontinued treatment due to side effects., Conclusions: Although the study did not meet the primary endpoint, vistusertib treatment was associated with high rates of SD in progressive NF2-related tumors. However, this dosing regimen for vistusertib was poorly tolerated. Future studies of dual mTORC inhibitors for NF2 should focus on optimizing tolerability and evaluating the relevance of tumor stability in participants., Competing Interests: J.T.J.—Paid consulting for NF Network, Recursion Pharmaceuticals, CereXis, Health2047, and Navio Theragnostics. Royalties from Elsevier Publishing. C.C.O.—Paid consulting for AstraZeneca. R.D.T.—No disclosures. J.V.C.—No disclosures. R.L.B.—No disclosures. G.S.—No disclosures. A.M.—No disclosures. A.S.-R.—No disclosures. M.G.—Consults for NF2 Therapeutics and Puma Biotechnology. M.K.—Paid consulting for Recursion Pharmaceuticals. F.G.B.— No disclosures. V.R.—No disclosures. S.R.P.—Dr. Plotkin is co-founder of NFlection Therapeutics and NF2 Therapeutics and consults for AstraZeneca, SonalaSense, and Akouos., (© The Author(s) 2023. Published by Oxford University Press, the Society for Neuro-Oncology and the European Association of Neuro-Oncology.)

Published
2023
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42. Updated diagnostic criteria and nomenclature for neurofibromatosis type 2 and schwannomatosis: An international consensus recommendation.

Author

Plotkin SR, Messiaen L, Legius E, Pancza P, Avery RA, Blakeley JO, Babovic-Vuksanovic D, Ferner R, Fisher MJ, Friedman JM, Giovannini M, Gutmann DH, Hanemann CO, Kalamarides M, Kehrer-Sawatzki H, Korf BR, Mautner VF, MacCollin M, Papi L, Rauen KA, Riccardi V, Schorry E, Smith MJ, Stemmer-Rachamimov A, Stevenson DA, Ullrich NJ, Viskochil D, Wimmer K, Yohay K, Huson SM, Wolkenstein P, and Evans DG

Subjects
Consensus, Humans, Neurilemmoma diagnosis, Neurilemmoma genetics, Neurilemmoma pathology, Neurofibromatoses diagnosis, Neurofibromatoses genetics, Neurofibromatosis 1 genetics, Neurofibromatosis 2 diagnosis, Neurofibromatosis 2 genetics, Skin Neoplasms genetics
Abstract

Purpose: Neurofibromatosis type 2 (NF2) and schwannomatosis (SWN) are genetically distinct tumor predisposition syndromes with overlapping phenotypes. We sought to update the diagnostic criteria for NF2 and SWN by incorporating recent advances in genetics, ophthalmology, neuropathology, and neuroimaging., Methods: We used a multistep process, beginning with a Delphi method involving global disease experts and subsequently involving non-neurofibromatosis clinical experts, patients, and foundations/patient advocacy groups., Results: We reached consensus on the minimal clinical and genetic criteria for diagnosing NF2 and SWN. These criteria incorporate mosaic forms of these conditions. In addition, we recommend updated nomenclature for these disorders to emphasize their phenotypic overlap and to minimize misdiagnosis with neurofibromatosis type 1., Conclusion: The updated criteria for NF2 and SWN incorporate clinical features and genetic testing, with a focus on using molecular data to differentiate the 2 conditions. It is likely that continued refinement of these new criteria will be necessary as investigators study the diagnostic properties of the revised criteria and identify new genes associated with SWN. In the revised nomenclature, the term "neurofibromatosis 2" has been retired to improve diagnostic specificity., Competing Interests: Conflict of Interest R.A.A., C.O.H., and K.A.R declare no conflicts of interest. D.B.-V. is a scientific advisor for AstraZeneca, L.P. and receives grant support from the Department of Defense and SpringWorks Therapeutics. J.B. is a member of the Children’s Tumor Foundation Medical Advisory Committee and the Clinical Care Advisory Board. D.G.E. is a member of the Children’s Tumor Foundation Clinical Care Advisory Board-Europe and has received consultancy fees from AstraZeneca, SpringWorks Therapeutics, and Recursion. R.F. is a member of the Children’s Tumor Foundation Clinical Care Advisory Board-Europe and is a medical advisor for AstraZeneca. M.J.F. is a member of the Children’s Tumor Foundation Medical Advisory Committee. J.M.F. is a member of the Children’s Tumor Foundation Clinical Care Advisory Board. M.G. receives grant support from NF2 Therapeutics, Inc and is a consultant for Puma Biotechnology. D.H.G. declares no conflicts of interest. M.K. is a paid consultant for Regeneron Pharmaceuticals. S.M.H. declares no conflicts of interest. H.K.-S. declares no conflicts of interest. B.R.K is a member of the Children’s Tumor Foundation Medical Advisory Committee (Chair) and is on the medical advisory boards of Genome Medicine and iNfixion Bioscience. E.L. is a member of the Children’s Tumor Foundation Clinical Care Advisory Board-Europe. V.-F.M. is a member of the Children’s Tumor Foundation Clinical Care Advisory Board-Europe. M.M. declares no conflicts of interest. L.P. declares no conflicts of interest. L.M. directed the Medical Genomics Laboratory at University of Alabama, Birmingham, which specializes in genetic testing for all forms of the neurofibromatosis, until April 2021. P.P. is employed by the Children’s Tumor Foundation. S.R.P is a member of the Children’s Tumor Foundation Clinical Care Advisory Board (Chair, United States) and Europe; is cofounder of NFlection Therapeutics, Inc and NF2 Therapeutics, Inc; and is a consultant for Akouos, AstraZeneca, and SonALASense. V.R. declares no conflicts of interest. E.S. is a member of the Children’s Tumor Foundation Clinical Care Advisory Board and receives Department of Defense funding as a site for NF Clinical Trials Consortium. M.J.S declares no conflicts of interest. A.S.-R. declares no conflicts of interest. D.A.S. is a consultant for Alexion Pharmaceuticals, Inc. N.J.U is a member of the Children’s Tumor Foundation Clinical Care Advisory Board, serves on the board of Neurofibromatosis Northeast, and received a consultant fee from Astra Zeneca. D.V. is a member of the Children’s Tumor Foundation Medical Advisory Committee and Clinical Care Advisory Board, is a member of the AstraZeneca speaker’s bureau, and is on the Sanofi-Genzyme—MPS Board of Advisors. K.W. declares no conflicts of interest. P.W. is a member of the Children’s Tumor Foundation Clinical Care Advisory Board-Europe (Chair). K.Y. is a member of the Children’s Tumor Foundation Clinical Care Advisory Board, received a consultant fee from AstraZeneca, is on the Scientific Advisory Board for iNFixion Bioscience, is member of the Programmatic Review Committee for the Department of Defense, Congressionally Directed Medical Research Program, and Neurofibromatosis Research Program., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2022
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43. Conserved meningeal lymphatic drainage circuits in mice and humans.

Author

Jacob L, de Brito Neto J, Lenck S, Corcy C, Benbelkacem F, Geraldo LH, Xu Y, Thomas JM, El Kamouh MR, Spajer M, Potier MC, Haik S, Kalamarides M, Stankoff B, Lehericy S, Eichmann A, and Thomas JL

Subjects
Animals, Humans, Lymphatic System, Magnetic Resonance Imaging, Meninges diagnostic imaging, Mice, Glymphatic System diagnostic imaging, Glymphatic System pathology, Lymphatic Vessels diagnostic imaging
Abstract

Meningeal lymphatic vessels (MLVs) were identified in the dorsal and caudobasal regions of the dura mater, where they ensure waste product elimination and immune surveillance of brain tissues. Whether MLVs exist in the anterior part of the murine and human skull and how they connect with the glymphatic system and extracranial lymphatics remained unclear. Here, we used light-sheet fluorescence microscopy (LSFM) imaging of mouse whole-head preparations after OVA-A555 tracer injection into the cerebrospinal fluid (CSF) and performed real-time vessel-wall (VW) magnetic resonance imaging (VW-MRI) after systemic injection of gadobutrol in patients with neurological pathologies. We observed a conserved three-dimensional anatomy of MLVs in mice and humans that aligned with dural venous sinuses but not with nasal CSF outflow, and we discovered an extended anterior MLV network around the cavernous sinus, with exit routes through the foramina of emissary veins. VW-MRI may provide a diagnostic tool for patients with CSF drainage defects and neurological diseases., (© 2022 Jacob et al.)

Published
2022
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44. ERN GENTURIS clinical practice guidelines for the diagnosis, treatment, management and surveillance of people with schwannomatosis.

Author

Evans DG, Mostaccioli S, Pang D, Fadzil O Connor M, Pittara M, Champollion N, Wolkenstein P, Thomas N, Ferner RE, Kalamarides M, Peyre M, Papi L, Legius E, Becerra JL, King A, Duff C, Stivaros S, and Blanco I

Subjects
Adolescent, Child, Humans, Pain, Transcription Factors genetics, Neurilemmoma diagnosis, Neurilemmoma genetics, Neurilemmoma therapy, Neurofibromatoses diagnosis, Neurofibromatoses genetics, Neurofibromatoses therapy, Skin Neoplasms diagnosis, Skin Neoplasms genetics, Skin Neoplasms therapy
Abstract

A Guideline Group (GG) was convened from multiple specialties and patients to develop the first comprehensive schwannomatosis guideline. The GG undertook thorough literature review and wrote recommendations for treatment and surveillance. A modified Delphi process was used to gain approval for recommendations which were further altered for maximal consensus. Schwannomatosis is a tumour predisposition syndrome leading to development of multiple benign nerve-sheath non-intra-cutaneous schwannomas that infrequently affect the vestibulocochlear nerves. Two definitive genes (SMARCB1/LZTR1) have been identified on chromosome 22q centromeric to NF2 that cause schwannoma development by a 3-event, 4-hit mechanism leading to complete inactivation of each gene plus NF2. These genes together account for 70-85% of familial schwannomatosis and 30-40% of isolated cases in which there is considerable overlap with mosaic NF2. Craniospinal MRI is generally recommended from symptomatic diagnosis or from age 12-14 if molecularly confirmed in asymptomatic individuals whose relative has schwannomas. Whole-body MRI may also be deployed and can alternate with craniospinal MRI. Ultrasound scans are useful in limbs where typical pain is not associated with palpable lumps. Malignant-Peripheral-Nerve-Sheath-Tumour-MPNST should be suspected in anyone with rapidly growing tumours and/or functional loss especially with SMARCB1-related schwannomatosis. Pain (often intractable to medication) is the most frequent symptom. Surgical removal, the most effective treatment, must be balanced against potential loss of function of adjacent nerves. Assessment of patients' psychosocial needs should be assessed annually as well as review of pain/pain medication. Genetic diagnosis and counselling should be guided ideally by both blood and tumour molecular testing., (© 2022. The Author(s).)

Published
2022
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45. Targeting the CSF1/CSF1R axis is a potential treatment strategy for malignant meningiomas.

Author

Yeung J, Yaghoobi V, Miyagishima D, Vesely MD, Zhang T, Badri T, Nassar A, Han X, Sanmamed MF, Youngblood M, Peyre M, Kalamarides M, Rimm DL, Gunel M, and Chen L

Subjects
Animals, Humans, Macrophages, Mice, Tumor Microenvironment, Macrophage Colony-Stimulating Factor, Meningeal Neoplasms drug therapy, Meningioma drug therapy, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor
Abstract

Background: Malignant meningiomas are fatal and lack effective therapy. As M2 macrophages are the most prevalent immune cell type in human meningiomas, we hypothesized that normalizing this immunosuppressive population would be an effective treatment strategy., Methods: We used CIBERSORTx to examine the proportions of 22 immune subsets in human meningiomas. We targeted the colony-stimulating factor 1 (CSF1) or CSF1 receptor (CSF1R) axis, an important regulator of macrophage phenotype, using monoclonal antibodies (mAbs) in a novel immunocompetent murine model (MGS1) for malignant meningioma. RNA sequencing (RNA-seq) was performed to identify changes in gene expression in the tumor microenvironment (TME). Mass cytometry was used to delineate changes in immune subsets after treatment. We measured patients' plasma CSF1 levels using ELISA and CSF1R expression using multiplex quantitative immunofluorescence in a human meningioma tissue microarray., Results: Human meningiomas are heavily enriched for immunosuppressive myeloid cells. MGS1 recapitulates the TME of human meningiomas, including an abundance of myeloid cells, a paucity of infiltrating T cells, and low programmed death ligand 1 (PD-L1) expression. Treatment of murine meningiomas with anti-CSF1/CSF1R, but not programmed cell death receptor 1 (PD-1), mAbs abrogate tumor growth. RNA-seq and mass cytometry analyses reveal a myeloid cell reprogramming with limited effect on T cells in the TME. CSF1 plasma levels are significantly elevated in human patients, and CSF1R is highly expressed on CD163+ macrophages within the human TME., Conclusion: Our findings suggest that anti-CSF1/CSF1R antibody treatment may be an effective normalization cancer immunotherapy for malignant meningiomas., (© The Author(s) 2021. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published
2021
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46. Mouse Models in Meningioma Research: A Systematic Review.

Author

Boetto J, Peyre M, and Kalamarides M

Abstract

Meningiomas are the most frequent primitive central nervous system tumors found in adults. Mouse models of cancer have been instrumental in understanding disease mechanisms and establishing preclinical drug testing. Various mouse models of meningioma have been developed over time, evolving in light of new discoveries in our comprehension of meningioma biology and with improvements in genetic engineering techniques. We reviewed all mouse models of meningioma described in the literature, including xenograft models (orthotopic or heterotopic) with human cell lines or patient derived tumors, and genetically engineered mouse models (GEMMs). Xenograft models provided useful tools for preclinical testing of a huge range of innovative drugs and therapeutic options, which are summarized in this review. GEMMs offer the possibility of mimicking human meningiomas at the histological, anatomical, and genetic level and have been invaluable in enabling tumorigenesis mechanisms, including initiation and progression, to be dissected. Currently, researchers have a range of different mouse models that can be used depending on the scientific question to be answered.

Published
2021
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47. Role of 3D volume growth rate for drug activity evaluation in meningioma clinical trials: the example of the CEVOREM study.

Author

Graillon T, Ferrer L, Siffre J, Sanson M, Peyre M, Peyrière H, Mougel G, Autran D, Tabouret E, Figarella-Branger D, Barlier A, Kalamarides M, Dufour H, Colin T, and Chinot O

Subjects
Humans, Octreotide, Progression-Free Survival, Retrospective Studies, Treatment Outcome, Meningeal Neoplasms drug therapy, Meningioma drug therapy, Pharmaceutical Preparations
Abstract

Background: We aimed to improve the assessment of the drug activity in meningioma clinical trials based on the study of the 3D volume growth rate (3DVGR) in a series of aggressive meningiomas. We secondarily aimed to correlate 3DVGR study with patient outcome., Methods: We performed a post hoc analysis based on volume data and 3DVGR extracted from CEVOREM study including 18 patients with 32 recurrent high-grade meningiomas and treated with everolimus and octreotide. The joint latent class model was used to classify tumor 3DVGR undertreatment., Results: Class 1 includes lesions responding to treatment with decrease in volume in the first 3 months, and then a stabilization thereafter (9.5% of tumors) (mean pretreatment 3DVGR = 6.13%/month; mean undertreatment 3DVGR = -18.7%/month within 3 first months and -0.14%/month after the 3 first months). Class 2 includes lesions considered as stable or with a slight increase in volume undertreatment (65.5%) (mean pretreatment 3DVGR = 6.09%/month; undertreatment 3DVGR = -0.09% within the first 3 months). Class 3 includes lesions without 3DVGR decrease (25%) (mean pretreatment 3DVGR = 46.9%/month; mean undertreatment 3DVGR = 19.2%/month within the first 3 months). Patients with class 3 lesions had a significantly worse progression-free survival (PFS) rate than class 1 and 2 ones., Conclusions: Tumor 3DVGR could be helpful to detect early signal of drugs antitumoral activity or nonactivity. This volume response classification could help in the assessment of drug activity in tumors with mostly volume stabilization and rare response as aggressive meningiomas even with a low number of patients in complement to 6 months PFS., (© The Author(s) 2021. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published
2021
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48. Associations of meningioma molecular subgroup and tumor recurrence.

Author

Youngblood MW, Miyagishima DF, Jin L, Gupte T, Li C, Duran D, Montejo JD, Zhao A, Sheth A, Tyrtova E, Özduman K, Iacoangeli F, Peyre M, Boetto J, Pease M, Avşar T, Huttner A, Bilguvar K, Kilic T, Pamir MN, Amankulor N, Kalamarides M, Erson-Omay EZ, Günel M, and Moliterno J

Subjects
Epigenomics, Genomics, Humans, Kruppel-Like Factor 4, Male, Neoplasm Recurrence, Local genetics, Retrospective Studies, Meningeal Neoplasms genetics, Meningioma genetics
Abstract

Background: We and others have identified mutually exclusive molecular subgroups of meningiomas; however, the implications of this classification for clinical prognostication remain unclear. Integrated genomic and epigenomic analyses implicate unique oncogenic processes associated with each subgroup, suggesting the potential for divergent clinical courses. The aim of this study was to understand the associated clinical outcomes of each subgroup, as this could optimize treatment for patients., Methods: We analyzed outcome data for 469 meningiomas of known molecular subgroup, including extent of resection, postoperative radiation, surveillance imaging, and time to recurrence, when applicable. Statistical relationships between outcome variables and subgroup were assessed. Features previously associated with recurrence were further investigated after stratification by subgroup. We used Kaplan-Meier analyses to compare progression-free survival, and identified factors significantly associated with recurrence using Cox proportional hazards modeling., Results: Meningioma molecular subgroups exhibited divergent clinical courses at 2 years of follow-up, with several aggressive subgroups (NF2, PI3K, HH, tumor necrosis factor receptor-associated factor 7 [TRAF7]) recurring at an average rate of 22 times higher than others (KLF4, POLR2A, SMARCB1). PI3K-activated tumors recurred earlier than other subgroups but had intermediate long-term outcome. Among low-grade tumors, HH and TRAF7 meningiomas exhibited elevated recurrence compared with other subgroups. Recurrence of NF2 tumors was associated with male sex, high grade, and elevated Ki-67. Multivariate analysis identified molecular subgroup as an independent predictor of recurrence, along with grade and previous recurrence., Conclusion: We describe distinct clinical outcomes and recurrence rates associated with meningioma molecular subgroups. Our findings emphasize the importance of genomic characterization to guide postoperative management decisions for meningiomas., (© The Author(s) 2020. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published
2021
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49. Everolimus and Octreotide for Patients with Recurrent Meningioma: Results from the Phase II CEVOREM Trial.

Author

Graillon T, Sanson M, Campello C, Idbaih A, Peyre M, Peyrière H, Basset N, Autran D, Roche C, Kalamarides M, Roche PH, Fuentes S, Tabouret E, Barrie M, Cohen A, Honoré S, Boucekine M, Baumstarck K, Figarella-Branger D, Barlier A, Dufour H, and Chinot OL

Subjects
Adult, Aged, Everolimus administration & dosage, Female, Humans, Male, Meningeal Neoplasms metabolism, Meningeal Neoplasms pathology, Meningioma metabolism, Meningioma pathology, Middle Aged, Neoplasm Recurrence, Local metabolism, Neoplasm Recurrence, Local pathology, Octreotide administration & dosage, Patient Safety, Prospective Studies, Survival Rate, Treatment Outcome, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Meningeal Neoplasms drug therapy, Meningioma drug therapy, Neoplasm Recurrence, Local drug therapy, Receptors, Somatostatin antagonists & inhibitors, TOR Serine-Threonine Kinases antagonists & inhibitors, Tumor Burden drug effects
Abstract

Purpose: Aggressive meningiomas that progress after surgery/radiotherapy represent an unmet medical need. Strong and constant expression of SSTR2A receptors and activation of the Pi3K/Akt/mTOR pathway have been demonstrated in meningiomas. The combination of everolimus, an mTOR inhibitor, and octreotide, a somatostatin agonist, has shown additive antitumor effect in vitro . The phase II CEVOREM trial investigated the efficacy of this combination on recurrent meningiomas., Patients and Methods: Patients with documented recurrent tumor progression ineligible for further surgery/radiotherapy were eligible to receive octreotide (30 mg/d, day 1) and everolimus (10 mg/d, days 1-28). The primary endpoint was the 6-month progression-free survival rate (PFS6). The secondary endpoints were overall survival, response rate, tumor growth rate according to central review, and safety., Results: A total of 20 patients were enrolled, including 2 with World Health Organization (WHO) grade I tumors, 10 with WHO grade II tumors, and 8 with WHO grade III tumors; furthermore, 4 patients harbored NF2 germline mutation. The overall PFS6 was 55% [95% confidence interval (CI), 31.3%-73.5%], and overall 6- and 12-month survival rates were 90% (95% CI, 65.6%-97.4%) and 75% (95% CI, 50.0%-88.7%), respectively. A major decrease (>50%) was observed in the growth rate at 3 months in 78% of tumors. The median tumor growth rate decreased from 16.6%/3 months before inclusion to 0.02%/3 months at 3 months ( P < 0.0002) and 0.48%/3 months at 6 months after treatment ( P < 0.0003)., Conclusions: The combination of everolimus and octreotide was associated with clinical and radiological activity in aggressive meningiomas and warrants further studies. Decrease in the tumor volume growth rate should be considered a complementary and sensitive endpoint to select potentially effective drugs for recurrent meningiomas., (©2020 American Association for Cancer Research.)

Published
2020
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50. How to radiologically identify a spontaneous regression of sporadic vestibular schwannoma?

Author

Lahlou G, Rodallec M, Nguyen Y, Sterkers O, and Kalamarides M

Subjects
Cochlea diagnostic imaging, Cochlea pathology, Cochlea physiopathology, Hearing physiology, Humans, Magnetic Resonance Imaging, Neoplasm Regression, Spontaneous physiopathology, Neuroma, Acoustic pathology, Neuroma, Acoustic physiopathology, Neoplasm Regression, Spontaneous pathology, Neuroma, Acoustic diagnosis, Neuroma, Acoustic diagnostic imaging
Abstract

Background: The natural history of sporadic vestibular schwannoma is unpredictable, with tumors growing, non-growing and even showing spontaneous regression in some rare cases., Objective: This retrospective study aims to describe the radiologic signs characterizing and identifying the shrinking vestibular schwannoma., Methods: Involution was considered to have occurred if tumor size had decreased by 2 mm or more on its largest diameter. All magnetic resonance imaging scans were reviewed for tumor size, internal auditory meatus size, and tumor characteristics. Volumetric measurements were performed on the first and last scan. Audiometric data were collected at the first and last visit., Results: Fourteen patients with a confirmed spontaneous regression were included, with a mean follow-up of 5 ± 2.6 years. The mean shrinkage rate was 0.9 ± 0.59 mm/year on 2D measurements, and 0.2 ± 0.17 cm3/year on volumetric measurements, with a relative shrinkage of 40 ± 16.9%. Two remarkable radiologic features were observed: First, a festooned aspect, defined by multiple curves in the tumor outline, noticed in 12 cases (86%); second, the appearance of cerebrospinal fluid filling the internal auditory meatus, associated with an enlargement of the internal auditory meatus compared to the contralateral side, and observed in 10 out of 13 cases with internal auditory meatus invasion (77%). Those two aspects were associated in 64% of cases., Conclusion: These two newly reported radiologic features could help neurosurgeons, oto-neurosurgeons and neuroradiologists to identify a spontaneous vestibular schwannoma involution at first visit. This could allow any treatment to be postponed, monitoring to be more widely spaced, and patients to be reassured., Competing Interests: The authors have declared that no competing interests exist.

Published
2019
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