Brainstem gliomas in adults: prognostic factors and classification

doi:10.1093/brain/124.12.2528

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Brain, Vol. 124, No. 12, 2528-2539, December 2001
© 2001 Oxford University Press

Brainstem gliomas in adults: prognostic factors and classification

Jean-Sébastien Guillamo¹, Annick Monjour³, Luc Taillandier⁴, Bertrand Devaux², Pascale Varlet², Christine Haie-Meder⁵, Gilles-Louis Defer⁶, Patrick Maison⁷, Jean-Jacques Mazeron¹, Philippe Cornu¹, Jean-Yves Delattre¹ and for the Association des Neuro-Oncologues d'Expression Franciaise (ANOCEF)

¹ Service de Neurologie, Service de Radiothérapie, Service de Neurochirurgie, Hôpital Pitié-Salpêtrière ² Service de Neurochirurgie, Service d'Anatomopathologie, Hôpital Saint-Anne, Paris ³ Service de Neurologie, Hôpital Pasteur, Colmar ⁴ Service de Neurologie, CHU Nancy, Nancy ⁵ Service de Radiothérapie, Institut Gustave Roussy, Villejuif ⁶ Service de Neurologie Dejerine, CHU Côte de Nacre, Caen ⁷ Service de Pharmacologie clinique, CHU Henri Mondor Créteil, France

Correspondence to: Professor J.-Y. Delattre, Service de Neurologie Mazarin, Hôpital Pitié-Salpêtrière, 75651 Paris Cedex 13, Francejean-yves.delattre{at}psl.ap-hop-paris.fr

In contrast to childhood brainstem gliomas, adult brainstemgliomas are rare and poorly understood. The charts of 48 adultssuffering from brainstem glioma were reviewed in order to determineprognostic factors, evaluate the effect of treatment and proposea classification of these tumours. Mean age at onset was 34years (range 16–70 years). The main presenting symptomswere gait disturbance (61%), headache (44%), weakness of thelimbs (42%) and diplopia (40%). Four patterns were identifiedon MRI, representing non-enhancing, diffusely infiltrative tumours(50%), contrast-enhancing localized masses (31%), isolated tectaltumours (8%) and other patterns (11%). Treatment consisted ofpartial resection (8%), radiotherapy (94%) and chemotherapy(56%). Overall median survival was 5.4 years. On univariateanalysis, the following favourable prognostic factors were identified(P< 0.01): age of onset <40 years, duration of symptomsbefore diagnosis >3 months, Karnofski performance status>70, low-grade histology, absence of contrast enhancementand `necrosis' on MRI. On multivariate analysis, the durationof symptoms, the appearance of `necrosis' on MRI and the histologicalgrade of the tumour remained significant and independent prognosticfactors (P< 0.05). Eighty-five percent of the tumours couldbe classified into one of the following three groups on thebasis of clinical, radiological and histological features. (i)Diffuse intrinsic low-grade gliomas (46%) usually occurred inyoung adults with a long clinical history before diagnosis anda diffusely enlarged brainstem on MRI that did not show contrastenhancement. These patients were improved by radiotherapy in62% of cases and had a long survival time (median 7.3 years).Anaplastic transformation (appearance of contrast enhancement,27%) and relentless growth without other changes (23%) werethe main causes of death. (ii) Malignant gliomas (31%) occurredin elderly patients with a short clinical history. Contrastenhancement and necrosis were the rule on MRI. These tumourswere highly resistant to treatment and the patients had a mediansurvival time of 11.2 months. (iii) Focal tectal gliomas (8%)occurred in young patients and were often revealed by isolatedhydrocephalus. The course was indolent and the projected mediansurvival period exceeded 10 years. In conclusion, adult brainstemgliomas are different from the childhood forms and resemblesupratentorial gliomas in adults. Low-grade tumours have a clinicoradiologicalpattern that is so characteristic that the need for a potentiallyharmful biopsy is debatable. The optimum timing of treatmentfor supratentorial low-grade tumours remains unclear. In high-gradegliomas, the prognosis remains extremely poor despite aggressivetreatment with radiotherapy and chemotherapy.

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