Molecular Pathogenesis of Malignant Gliomas.

Authors

Ahmed B. K. Rasheed PhDFollow
Rodney Wiltshire Ph.D, Lehigh Valley Health NetworkFollow
Sandra H. Bigner MDFollow
Darell D. Bigner MDFollow

Publication/Presentation Date

5-1999

Abstract

De novo glioblastomas develop in older patients without prior clinical history of less malignant tumors. Progressive glioblastomas are common among younger patients and arise through progression from lower-grade astrocytomas. CDKN2A deletions, PTEN alterations, and EGFR amplification are more prevalent among de novo glioblastomas, whereas p53 mutations are more common among progressive glioblastomas. Loss of heterozygosity (LOH) for chromosome 10 is seen uniformly among both de novo and progressive high-grade astrocytomas. The inactivation of the PTEN gene is found in approximately 30% to 40% of astrocytomas with chromosome 10 loss, and LOH pattern in the remaining astrocytomas strongly supports the presence of another yet unidentified tumor suppressor gene telomeric to PTEN. More than 80% of oligodendrogliomas exhibit LOH for 1 p and 19q alleles. Oligoastrocytomas with 1p/19q LOH are related to oligodendrogliomas, and those with p53 mutations are related to astrocytomas.

Volume

11

Issue

3

First Page

162

Last Page

167

ISSN

1040-8746

Published In/Presented At

Rasheed, B. K., Wiltshire, R. N., Bigner, S. H., and Bigner, D. D. (1999). Molecular pathogenesis of malignant gliomas. Current Opinion In Oncology, 11(3), 162-167.

Disciplines

Medical Pathology | Pathology

PubMedID

10328589

Department(s)

Department of Pathology and Laboratory Medicine, Pathology Laboratory Medicine Faculty

Document Type

Article