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Immunohistochemical and molecular genetic study on epithelioid glioblastoma: Series of seven cases with review of literature
Authors:Gaurav Khanna  Pankaj Pathak  Vaishali Suri  Mehar Chand Sharma  Sujata Chaturvedi  Arvind Ahuja  M. Bhardwaj  Ajay Garg  Chitra Sarkar  Rajeev Sharma
Affiliation:1. Department of Pathology, All India Institute of Medical Sciences (AIIMS), New Delhi 110029, India;2. Department of Pathology, Institute of Human Behaviour and Allied Sciences, New Delhi, India;3. Department of Pathology, PGIMER & Dr. RML Hospital, New Delhi, India;4. Department of Neuroradiology,All India Institute of Medical Sciences (AIIMS), New Delhi, India;5. Department of Neurosurgery, All India Institute of Medical Sciences (AIIMS), New Delhi, India
Abstract:Epithelioid glioblastoma (e-gbm) is a recently described variant of glioblastoma (GBM) which is associated with short survival and now added as a provisional entity to WHO 2016 classification of CNStumors. About half of these tumors show characteristic BRAF-V600E mutation. However, unlike conventional GBMs, e-gbm lack specific diagnostic and prognostic markers. Hence, we aimed to molecularly characterize these tumors. An extensive review of literature was performed.In a multi-institutional effort, all the cases of glioblastoma of year 2017 were reviewed. Cases with predominant epithelioid morphology were analysed. Seven cases of e-gbm (adults:4 and pediatric: 3) were identified. Duration of symptoms varied from 2 weeks to one month. Radiologically, all cases were supratentorial, contrast enhancing with solid and cystic appearance. Majority of the cases were immunopositive for GFAP (71%), EMA (71%), S100 (71%) and vimentin (85%). All the cases showed ATRX, INI-1 and H3K27me3 expression. BRAFV600Emutation was seen in 28% of cases. TERT mutation was seen in 40% cases, while one case showed EGFR amplification. H3F3A mutations and PTEN deletions were seen in none. Although e-gbms are rare, epithelioid morphology of a CNS tumor in a young adult or children with areas of necrosis needs thorough histomorphological and genetic workup.
Keywords:BRAFV600E  Epithelioid glioblastoma  EGFR amplification  TERT
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