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DNA拓扑异构酶IIα可预测儿童恶性非脑干胶质瘤的无进展生存期和总生存期。

DNA topoisomerase IIalpha predicts progression-free and overall survival in pediatric malignant non-brainstem gliomas.

作者信息

Bredel Markus, Pollack Ian F, Hamilton Ronald L, Birner Peter, Hainfellner Johannes A, Zentner Josef

机构信息

Department of General Neurosurgery, Neurocenter, University of Freiburg, Freiburg, Germany.

出版信息

Int J Cancer. 2002 Jun 20;99(6):817-20. doi: 10.1002/ijc.10421.

Abstract

Malignant non-brainstem glioma (MNBG) is a rare pediatric brain tumor. The prognosis for children harboring this lesion remains largely unpredictable. Assessment of histologic features alone only provides a marginal insight into the biologic behavior of these lesions. Hence, the identification of novel molecular markers capable of characterizing these lesions more accurately with respect to their biologic aggressiveness is definitely needed. Our current study examined the expression of nuclear DNA topoisomerase IIalpha (TIIalpha), a novel marker of cell cycle turnover and a determinant of tumor cell resistance to chemotherapy, in a series of 17 archival pediatric MNBGs. TIIalpha expression was found to extend over a wide range in the study cohort (3.9-69.1%). A cutoff labeling index of 12% was found to define 2 prognostic subgroups (TIIalpha <12 vs. >or=12) with profoundly different 5-year progression-free survival (60% vs. 8%; p = 0.0108, log-rank test) and overall survival (100% vs. 8%; p = 0.0038) rates. TIIalpha expression was significantly linked to MIB-1 antibody labeling of the Ki-67 nuclear antigen (R = 0.919, p < 0.001). A high TIIalpha labeling index remained associated with short progression-free survival (p = 0.022) and overall survival (p = 0.022) in multivariate analysis (Cox regression). In conclusion, considering that TIIalpha expression was not related to histopathologic grade, biological characteristics as assessed by TIIalpha labeling may complement the information obtained by tumor morphology as a means of improving the accuracy of patient prognosis prediction.

摘要

恶性非脑干胶质瘤(MNBG)是一种罕见的儿童脑肿瘤。患有这种病变的儿童的预后在很大程度上仍然无法预测。仅评估组织学特征只能对这些病变的生物学行为提供有限的见解。因此,绝对需要鉴定能够更准确地根据其生物学侵袭性来表征这些病变的新型分子标志物。我们目前的研究检测了核DNA拓扑异构酶IIα(TIIα)的表达,TIIα是细胞周期转换的一种新型标志物,也是肿瘤细胞对化疗耐药性的一个决定因素,研究对象为17例存档的儿童MNBG。在研究队列中发现TIIα表达范围很广(3.9%-69.1%)。发现12%的截断标记指数可定义两个预后亚组(TIIα<12与≥12),其5年无进展生存率(60%对8%;p = 0.0108,对数秩检验)和总生存率(100%对8%;p = 0.0038)有显著差异。TIIα表达与Ki-67核抗原的MIB-1抗体标记显著相关(R = 0.919,p < 0.001)。在多变量分析(Cox回归)中,高TIIα标记指数仍与短的无进展生存期(p = 0.022)和总生存期(p = 0.022)相关。总之,考虑到TIIα表达与组织病理学分级无关,通过TIIα标记评估的生物学特征可能补充通过肿瘤形态学获得的信息,作为提高患者预后预测准确性的一种手段。

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