DNA repair and genome stability, and p53 mutants often lead to cancer development and poor outcome. TP53 mutations are one of the most crucial factors in the development of malignant gliomas. Considering the IDH mutations correlated with mutant P53 protein, the inherent mechanism of a better prognosis for RP5264 patients with IDH mutations requires further investigation. Co-deletion of chromosome 1p/19q, which is commonly observed in oligodendroglial tumours, is associated with a good prognosis and increased responsiveness to chemotherapy. These MGCD-265 hydrochloride chemical information genetic changes often occur in a staged order during malignant transformation. Watanabe et al. dissected multiple biopsies from the same glioma patients and found that there was no case in which IDH mutations had occurred after the acquisition of either a TP53 mutation or 1p/19q codeletion, suggesting that IDH mutations were early events occurring during human gliomagenesis and may affect a common glial precursor cell population. Our meta-analysis have found that IDH mutations carry a very strong prognostic significance for PFS and OS. Subgroup analyses according to tumour grade also revealed that the presence of IDH mutations was associated with a better outcome. For patients with IDH mutations, longer OS was observed in patients with grades III and IV gliomas. The PFS in patients with mutated IDH and grades III or IV gliomas had a better prognosis, but this observation had no statistical significance in grade IV gliomas. In our meta-analysis all the survival data were available in the form of a multivariate analysis. Therefore, IDH mutations seem to be an independent favorable prognostic marker in glioma patients. The reasons for an improved outcome could potentially be related to the biological results of mutant IDH. First, mutant IDH1R132H overexpression in stably transfected glioma cell lines in vitro resulted in a marked decrease in proliferation rates, decreased Akt phosphorylation, altered morphology, and a more contactdependent cell migration. The reduced proliferation is a consequence of the D-2-HG produced by IDH1R132H. Mice injected with IDH1R132H�CGFP-expressing cells have prolonged survival compared to mice injected with cells expressing either IDH1wt�C GFP or GFP. Second, the IDH1 codon 132 mutations consume rather than produce NADPH. NADPH plays an important role in detoxification processes and scavenging oxygen radicals; the low NADPH levels may be less resistant to irradiation and chemotherapy, thus expl
