脑膜瘤中DNA拓扑异构酶II-α和细胞周期蛋白A的免疫表达及其预后意义:263例分析
DNA topoisomerase II-alpha and cyclin A immunoexpression in meningiomas and its prognostic significance: an analysis of 263 cases.
作者信息
Korshunov Andrey, Shishkina Lyudmila, Golanov Andrey
机构信息
Department of Neuropathology, Burdenko Neurosurgical Institute, Moscow, Russia.
出版信息
Arch Pathol Lab Med. 2002 Sep;126(9):1079-86. doi: 10.5858/2002-126-1079-DTIACA.
CONTEXT
Routine pathologic examination cannot distinctively predict the clinical course of meningiomas because even histologically benign tumors may recur after gross total resection. Therefore, numerous efforts have been made to evaluate the meningioma growth fraction and its prognostic value. However, a universally applicable proliferative marker for meningioma outcome is not yet a reality.
OBJECTIVE
To investigate the prognostic utility of 3 proliferative markers, namely, Ki-67, DNA topoisomerase II-alpha (topoII), and cyclin A in a representative series of intracranial meningiomas.
DESIGN
Two hundred sixty-three adult patients with intracranial meningiomas (208 benign, 42 atypical, and 13 anaplastic) were studied retrospectively. Tumor specimens were immunohistochemically examined with antibodies to Ki-67 (MM-1), topoII, and cyclin A. A computerized color image analyzer was used to count immunostained nuclei.
RESULTS
The topoII and cyclin A scores exhibited a close correlation with Ki-67 immunostaining. Significant differences between the indices for all 3 markers were noted among the 3 grades of meningiomas. The scores for all 3 markers were significantly different between recurrent and nonrecurrent meningiomas, including benign tumors that were treated with gross total resection. Recurrence-free survival was significantly reduced for cases with a Ki-67 labeling index (LI) of 4.4% or greater, a topoII LI of 3.2% or greater, and a cyclin A LI of 3.1% or greater. Multivariate analysis revealed that the risk of recurrence for the entire meningioma cohort was significantly associated with tumor grade (hazard ratio = 2.7; P =.004), topoII LI of 3.2% or greater (hazard ratio = 5.5; P <.001), and a cyclin A LI of 3.1% or greater (hazard ratio = 2.4; P =.01).
CONCLUSIONS
There is a close correlation in the expression of these 3 proliferative markers in meningiomas, and all of the markers showed a significant association with tumor grade, recurrence rate, and recurrence-free survival. Consequently, in addition to Ki-67, immunoexpression of topoII and cyclin A is available for predicting meningioma recurrence. Moreover, the topoII and cyclin A staining scores were found to be more sensitive predictors for meningioma progression than Ki-67 and, therefore, either of these 2 markers may prove to be clinically informative and useful.
背景
常规病理检查无法明确预测脑膜瘤的临床病程,因为即使是组织学上的良性肿瘤在全切术后也可能复发。因此,人们已做出诸多努力来评估脑膜瘤的生长分数及其预后价值。然而,尚未有一个普遍适用的脑膜瘤预后增殖标志物。
目的
在一组具有代表性的颅内脑膜瘤中研究3种增殖标志物,即Ki-67、DNA拓扑异构酶II-α(topoII)和细胞周期蛋白A的预后效用。
设计
对263例成年颅内脑膜瘤患者(208例良性、42例非典型性和13例间变性)进行回顾性研究。用抗Ki-67(MM-1)、topoII和细胞周期蛋白A的抗体对肿瘤标本进行免疫组化检查。使用计算机化彩色图像分析仪对免疫染色的细胞核进行计数。
结果
topoII和细胞周期蛋白A评分与Ki-67免疫染色密切相关。在3级脑膜瘤中,所有3种标志物的指数存在显著差异。所有3种标志物的评分在复发和未复发的脑膜瘤之间存在显著差异,包括接受全切治疗的良性肿瘤。Ki-67标记指数(LI)≥4.4%、topoII LI≥3.2%和细胞周期蛋白A LI≥3.1%的病例无复发生存期显著缩短。多因素分析显示,整个脑膜瘤队列的复发风险与肿瘤分级(风险比=2.7;P=0.004)、topoII LI≥3.2%(风险比=5.5;P<0.001)和细胞周期蛋白A LI≥3.1%(风险比=2.4;P=0.01)显著相关。
结论
这3种增殖标志物在脑膜瘤中的表达密切相关,且所有标志物均与肿瘤分级、复发率和无复发生存期显著相关。因此,除Ki-67外,topoII和细胞周期蛋白A的免疫表达也可用于预测脑膜瘤复发。此外,发现topoII和细胞周期蛋白A染色评分比Ki-67对脑膜瘤进展的预测更敏感,因此这2种标志物中的任何一种可能都具有临床信息价值且有用。
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