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A molecularly integrated grade for meningioma
Authors:Joseph Driver  Samantha E Hoffman  Sherwin Tavakol  Eleanor Woodward  Eduardo A Maury  Varun Bhave  Noah F Greenwald  Farshad Nassiri  Kenneth Aldape  Gelareh Zadeh  Abrar Choudhury  Harish N Vasudevan  Stephen T Magill  David R Raleigh  Malak Abedalthagafi  Ayal A Aizer  Brian M Alexander  Keith L Ligon  David A Reardon  Patrick Y Wen  Ossama Al-Mefty  Azra H Ligon  Adrian M Dubuc  Rameen Beroukhim  Elizabeth B Claus  Ian F Dunn  Sandro Santagata  Wenya Linda Bi
Abstract:
BackgroundMeningiomas are the most common primary intracranial tumor in adults. Clinical care is currently guided by the World Health Organization (WHO) grade assigned to meningiomas, a 3-tiered grading system based on histopathology features, as well as extent of surgical resection. Clinical behavior, however, often fails to conform to the WHO grade. Additional prognostic information is needed to optimize patient management.MethodsWe evaluated whether chromosomal copy-number data improved prediction of time-to-recurrence for patients with meningioma who were treated with surgery, relative to the WHO schema. The models were developed using Cox proportional hazards, random survival forest, and gradient boosting in a discovery cohort of 527 meningioma patients and validated in 2 independent cohorts of 172 meningioma patients characterized by orthogonal genomic platforms.ResultsWe developed a 3-tiered grading scheme (Integrated Grades 1-3), which incorporated mitotic count and loss of chromosome 1p, 3p, 4, 6, 10, 14q, 18, 19, or CDKN2A. 32% of meningiomas reclassified to either a lower-risk or higher-risk Integrated Grade compared to their assigned WHO grade. The Integrated Grade more accurately identified meningioma patients at risk for recurrence, relative to the WHO grade, as determined by time-dependent area under the curve, average precision, and the Brier score.ConclusionWe propose a molecularly integrated grading scheme for meningiomas that significantly improves upon the current WHO grading system in prediction of progression-free survival. This framework can be broadly adopted by clinicians with relative ease using widely available genomic technologies and presents an advance in the care of meningioma patients.
Keywords:meningioma   copy-number alterations
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