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作 者:崔晓敏[1] 林宁[1] 刘彦伟[2] 李瑞[1] 尤永平[1] 颜伟[1]
机构地区:[1]南京医科大学第一附属医院神经外科,210029 [2]北京市神经外科研究所,100050
出 处:《中国微侵袭神经外科杂志》2016年第1期4-6,共3页Chinese Journal of Minimally Invasive Neurosurgery
基 金:国家自然科学基金青年基金(编号:81402056)
摘 要:目的基于分子病理标志物IDH1/2和p53突变状态对初诊恶性脑胶质瘤(WHOⅡ~Ⅳ级)进行分型。方法选择541例初诊胶质瘤样本,通过焦磷酸测序检测IDH1/2突变状态,免疫组化检测突变型P53蛋白表达水平来获得p53突变状态,进一步联合分析IDH1/2突变和p53突变在初诊脑胶质瘤分型中的临床价值。结果联合IDH1/2和p53突变状态可以将脑胶质瘤分成4种分子亚型。其中IDH1/2突变型/p53野生型(Group1)预后最好,IDH1/2突变型/p53突变型(Group2)预后次之,IDH1/2野生型/p53野生型(Group3)再次之,IDH1/2野生型/p53突变型(Group4)预后最差。结论基于IDH1/2和p53突变状态提出初诊脑胶质瘤的预后分型,其具有更加简便的临床应用性和潜在的治疗指导价值。Objective To classify subtypes of the newly diagnosed gliomas (WHO grade Ⅱ to Ⅳ) based on IDH1/2 and p53 mutation status. Methods A total of 541 newly diagnosed glioma samples were selected. IDH1/2 mutation status was assessed by pyrosequencing and p53 mutation status was obtained via immunohistochemical staining examination of mutant P53 protein. The clinical value of IDH1/2 and p53 mutation status in the subtype of gliomas was analyzed conjointly. Results Conjoint analysis of IDH1/2 andp53 mutation status defined 4 subtypes of gliomas. IDH1/2 mutation/p53 wild-type (Groupl) had the best prognosis, 1DH1/2 mutation/p53 mutation (Group2) took second place, IDH1/2 wild-type/p53 wild-type (Group3) was the third, and IDH1/2 wild-type/p53 mutation (Group4) showed the worst prognosis. Conclusion Based on IDH1/2 and p53 mutation status in newly diagnosed glioma, the novel subtype has more convenient clinical application and potential guidance value for treatment.
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