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First Published Online January 31, 2009
The Oncologist, doi: 10.1634/theoncologist.2008-0248
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Neuro-Oncology

Oligodendrogliomas: Molecular Biology and Treatment

Jacolien E. C. Bromberg1, Martin J. van den Bent1

1Neuro-Oncology Unit, Daniel den Hoed Cancer Center/Erasmus University Medical Center, Rotterdam, The Netherlands

Key Words. Oligodendroglioma • Oligoastrocytoma • 1p • 19q • MGMT • Temozolomide

Correspondence: Correspondence: Martin J. van den Bent, M.D., Neuro-Oncology Unit, Daniel den Hoed Cancer Center/Erasmus University Medical Center, PO Box 5201, 3008AE Rotterdam, The Netherlands. Telephone: 31-10-4391415; Fax: 31-10-4391031; e-mail: m.vandenbent{at}erasmusmc.nl

Received November 14, 2008; accepted for publication January 12, 2009.

Disclosures: Jacolien E. C. Bromberg: None; Martin J. van den Bent: Consultant/advisory role: Schering Plough; Honoraria: Schering Plough. The content of this article has been reviewed by independent peer reviewers to ensure that it is balanced, objective, and free from commercial bias. No financial relationships relevant to the content of this article have been disclosed by independent peer reviewers.

Oligodendroglial tumors continue to receive much attention because of their relative sensitivity to chemotherapy. The histological diagnosis of oligodendroglial tumors is subject to considerable interobserver variation. The revised 2007 World Health Organization classification of brain tumors no longer accepts the diagnosis "mixed anaplastic oligoastrocytoma" if necrosis is present; these tumors should be considered glioblastomas (perhaps with oligodendroglial features). The 1p/19q codeletion that is associated with sensitivity to chemotherapy is mediated by an unbalanced translocation of 19p to 1q. Randomized studies have shown that patients with 1p/19q codeleted tumors also have a better outcome with radiotherapy. Histologically more atypical tumors are less likely to have this 1p/19q codeletion; here, other alterations usually associated with astrocytic tumors are often found. Some patients with tumors with classic histological features but no 1p/19q codeletion still have a very favorable prognosis. %Currently, the best approach for newly diagnosed anaplastic oligodendroglial tumors is unclear. Early adjuvant chemotherapy does not provide a better outcome than chemotherapy at the time of progression. The value of combined chemoirradiation with temozolomide has not been proven in these tumors, and could at least theoretically be associated with greater neurotoxicity. Tumors with 1p and 19q loss can also be managed with early chemotherapy, while deferring radiotherapy to the time of further progression. The presently available second-line chemotherapy results are modest, and better salvage treatments are necessary. The molecular explanation for the greater sensitivity of 1p/19q codeleted tumors is still unclear, and this could, in part, be explained by more frequent MGMT promoter gene methylation.







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