Malignant and benign ganglioglioma: A pathological and molecular study

doi:10.1215/15228517-2006-029

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First published on January 26, 2007
A more recent version of this article appeared on April 1, 2007
Neuro Oncol 2007, DOI:10.1215/15228517-2006-029

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Basic and Translational Investigations

Malignant and benign ganglioglioma: A pathological and molecular study

Ajay Pandita ¹, Anandh Balasubramaniam ¹, Richard Perrin ², Patrick Shannon ³, Abhijit Guha ⁴^*

¹ Arthur and Sonia Labatt Brain Tumour Research Centre, Hospital for Sick Children, Toronto, Ontario, Canada
² Division of Neurosurgery, University Health Network, Toronto, Ontario, Canada
³ Division of Neuropathology, University Health Network, Toronto, Ontario, Canada
⁴ Arthur and Sonia Labatt Brain Tumour Research Centre, Hospital for Sick Children and Division of Neurosurgery, University Health Network, Toronto, Ontario, Canada

^* To whom correspondence should be addressed. E-mail: Abhijit.Guha{at}uhn.on.ca.

Abstract

Gangliogliomas are generally benign tumors, composed of transformedneuronal and glial elements, with rare malignant progressionof the glial component. The current study of a rare case ofa woman harboring a ganglioglioma with areas of malignant transformationaddresses two fundamental questions: (1) Are the gangliogliomaand its malignant component clonal in origin? (2) What are thegenetic alterations associated with the initiation and subsequentmalignant progression of ganglioglioma? By using the human androgenreceptor gene (HUMARA) assay, we found the ganglioglioma andthe malignant component to be clonal in origin, suggestive ofinitial transformation of a single neuroglial precursor cellwith subsequent malignant progression. Conventional and arraycomparative genomic hybridization (approximately 2.5-Mb resolution)analyses found chromosomal losses to be predominant in the benignareas of the ganglioglioma, with gains more prevalent in themalignant component. Regions of chromosomal loss, postulatedto harbor genes involved in the initiation of ganglioglioma,included 1p35-36, 2p16-15, 3q13.1-13.3, 3q24-25.3, 6p21.3-21.2,6q24-25.2, 9p12, Xp11.3-11.22, and Xq22.1-22.3. Direct analysisdemonstrated loss of p19 expression and p53 mutation in themalignant areas, highly suggestive of these alterations beinginvolved in the malignant progression of the ganglioglioma.Additional chromosomal alterations specific to the malignancyinvolved gains on 1p35-34.2, 2q24.1-32.3, 3q13.1-13.3, 6q13-16.2,7q11.2-31.3, 8q21.1-23, 11q12-31, and 12q13.2-21.3. This molecular-pathologicalstudy has provided insight into the pathogenesis of gangliogliomasand associated rare malignant progression. Deciphering the specificgenes residing in these chromosomal regions may further ourunderstanding of not only these rare tumors but also the morecommon gliomas.

Key Words: array CGH (aCGH), comparative genomic hybridization (CGH), ganglioglioma, human androgen receptor gene (HUMARA), malignant ganglioglioma

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