Glioma-associated Antigen Expression in Oligodendroglial Neoplasms: Tenascin and Epidermal Growth Factor Receptor

Journal of Histochemistry and Cytochemistry

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ARTICLE

Glioma-associated Antigen Expression in Oligodendroglial Neoplasms: Tenascin and Epidermal Growth Factor Receptor

Roger E. McLendon^a, Carol J. Wikstrand^a, Mark R. Matthews^a, Raid Al-Baradei^a, Sandra H. Bigner^a, and Darell D. Bigner^a
^a Department of Pathology, Duke University Medical Center, Durham, North Carolina

Correspondence to: Roger E. McLendon, DUMC 3712, Durham, NC 27710. E-mail: roger.mclendon@duke.edu

Epidermal growth factor receptor (EGFR), its variant, EGFRvIII,and tenascin are glioma-associated antigens that are hyperexpressedby neoplastic glial cells relative to normal brain, making themattractive antigenic targets for immunotherapy. Preliminarysurveys indicate that oligodendroglial tumors also produce theseproteins, although the exact patterns and degrees of reactivityare not known. In this study we examined the immunoreactivityof tenascin among 50 oligodendroglial tumors, including 25 well-differentiatedoligodendrogliomas (WDOs) and 12 glioblastomas (GBMs) exhibitinghigh proportions of oligodendroglia-like cells. We used well-characterizedimmunoreagents with defined specificities against the targetantigens on formalin-fixed, paraffin-embedded archival tissue.The tumors were graded according to WHO guidelines. Immunoreactivitywas reported on a 1–3 scale according to staining intensitymultiplied by a 1–3 distribution scale distribution withintumor as focal (1), multifocal (2), and diffuse (3) for boththe parenchymal and the perivascular components. Although thereis considerable overlap in antigen production among the gradesof tumor, this study establishes the production of tenascinand wild-type EGFR (but not EGFR vIII) in oligodendroglial neoplasmsand supports the concept that antigen production increases withtumor grade.

(J Histochem Cytochem 48:1103–1110, 2000)

Key Words: epidermal growth factor, receptor, glioblastoma, immunotherapy,oligodendroglioma, tumor grade

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