PMID- 15977639 OWN - NLM STAT- MEDLINE DCOM- 20050812 LR - 20240109 IS - 0022-3069 (Print) IS - 0022-3069 (Linking) VI - 64 IP - 6 DP - 2005 Jun TI - Population-based studies on incidence, survival rates, and genetic alterations in astrocytic and oligodendroglial gliomas. PG - 479-89 AB - Published data on prognostic and predictive factors in patients with gliomas are largely based on clinical trials and hospital-based studies. This review summarizes data on incidence rates, survival, and genetic alterations from population-based studies of astrocytic and oligodendrogliomas that were carried out in the Canton of Zurich, Switzerland (approximately 1.16 million inhabitants). A total of 987 cases were diagnosed between 1980 and 1994 and patients were followed up at least until 1999. While survival rates for pilocytic astrocytomas were excellent (96% at 10 years), the prognosis of diffusely infiltrating gliomas was poorer, with median survival times (MST) of 5.6 years for low-grade astrocytoma WHO grade II, 1.6 years for anaplastic astrocytoma grade III, and 0.4 years for glioblastoma. For oligodendrogliomas the MSTwas 11.6 years for grade II and 3.5 years for grade III. TP53 mutations were most frequent in gemistocytic astrocytomas (88%), followed by fibrillary astrocytomas (53%) and oligoastrocytomas (44%), but infrequent (13%) in oligodendrogliomas. LOH 1p/19q typically occurred in tumors without TP53 mutations and were most frequent in oligodendrogliomas (69%), followed by oligoastrocytomas (45%), but were rare in fibrillary astrocytomas (7%) and absent in gemistocytic astrocytomas. Glioblastomas were most frequent (3.55 cases per 100,000 persons per year) adjusted to the European Standard Population, amounting to 69% of total incident cases. Observed survival rates were 42.4% at 6 months, 17.7% at one year, and 3.3% at 2 years. For all age groups, survival was inversely correlated with age, ranging from an MST of 8.8 months (<50 years) to 1.6 months (>80 years). In glioblastomas, LOH 10q was the most frequent genetic alteration (69%), followed by EGFR amplification (34%), TP53 mutations (31%), p16INK4a deletion (31%), and PTEN mutations (24%). LOH 10q occurred in association with any of the other genetic alterations, and was the only alteration associated with shorter survival of glioblastoma patients. Primary (de novo) glioblastomas prevailed (95%), while secondary glioblastomas that progressed from low-grade or anaplastic gliomas were rare (5%). Secondary glioblastomas were characterized by frequent LOH 10q (63%) and TP53 mutations (65%). Of the TP53 mutations in secondary glioblastomas, 57% were in hot-spot codons 248 and 273, while in primary glioblastomas, mutations were more evenly distributed. G:C-->A:T mutations at CpG sites were more frequent in secondary than primary glioblastomas, suggesting that the acquisition of TP53 mutations in these glioblastoma subtypes may occur through different mechanisms. FAU - Ohgaki, Hiroko AU - Ohgaki H AD - Pathology Group, International Agency for Research on Cancer (HO), F-69372, Lyon, France. ohgaki@iarc.fr FAU - Kleihues, Paul AU - Kleihues P LA - eng PT - Journal Article PT - Review PL - England TA - J Neuropathol Exp Neurol JT - Journal of neuropathology and experimental neurology JID - 2985192R RN - 0 (Tumor Suppressor Protein p53) SB - IM MH - Age Distribution MH - *Astrocytoma/epidemiology/genetics/mortality/secondary MH - *Brain Neoplasms/epidemiology/genetics/mortality MH - Chromosomes, Human, Pair 10 MH - Disease Progression MH - Humans MH - Incidence MH - *Loss of Heterozygosity MH - Mutation MH - *Oligodendroglioma/epidemiology/genetics/mortality MH - Predictive Value of Tests MH - Recurrence MH - Sex Factors MH - Survival Rate MH - Switzerland/epidemiology MH - Tumor Suppressor Protein p53/*genetics/metabolism RF - 67 EDAT- 2005/06/28 09:00 MHDA- 2005/08/13 09:00 CRDT- 2005/06/28 09:00 PHST- 2005/06/28 09:00 [pubmed] PHST- 2005/08/13 09:00 [medline] PHST- 2005/06/28 09:00 [entrez] AID - 10.1093/jnen/64.6.479 [doi] PST - ppublish SO - J Neuropathol Exp Neurol. 2005 Jun;64(6):479-89. doi: 10.1093/jnen/64.6.479.