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分子标志物评估表明,在间变性星形细胞瘤和胶质母细胞瘤中,通过立体定向活检和开颅手术获取的样本之间具有一致性。

Assessment of molecular markers demonstrates concordance between samples acquired via stereotactic biopsy and open craniotomy in both anaplastic astrocytomas and glioblastomas.

作者信息

Gessler Florian, Baumgarten Peter, Bernstock Joshua D, Harter Patrick, Lescher Stephanie, Senft Christian, Seifert Volker, Marquardt Gerhard, Weise Lutz

机构信息

Department of Neurosurgery, University Hospital Frankfurt, Goethe-University, Schleusenweg 2-16, 60528, Frankfurt, Germany.

Institute of Neurology (Edinger-Institute), University Hospital Frankfurt, Goethe-University, Heinrich-Hoffmann-Straße 7, 60528, Frankfurt, Germany.

出版信息

J Neurooncol. 2017 Jun;133(2):399-407. doi: 10.1007/s11060-017-2448-2. Epub 2017 May 15.

Abstract

The classification, treatment and prognosis of high-grade gliomas has been shown to correlate with the expression of molecular markers (e.g. MGMT promotor methylation and IDH1 mutations). Acquisition of tumor samples may be obtained via stereotactic biopsy or open craniotomy. Between the years 2009 and 2013, 22 patients initially diagnosed with HGGs via stereotactic biopsy, that ultimately underwent open craniotomy for resection of their tumor were prospectively included in an institutional glioma database. MGMT promotor analysis was performed using methylation-specific (MS)-PCR and IDH1R132H mutation analysis was performed using immunohistochemistry. Three patients (13.7%) exhibited IDH1R132H mutations in samples obtained via stereotactic biopsy. Tissue derived from stereotaxic biopsy was demonstrated to have MGMT promotor methylation in ten patients (45.5%), while a non-methylated MGMT promotor was demonstrated in ten patients (45.5%); inconclusive results were obtained for the remaining two patients (9%) within our cohort. The initial histologic grading, IDH1R132H mutation and MGMT promotor methylation results were confirmed using samples obtained during open craniotomy in all but one patient; here inconclusive MGMT promotor analysis was obtained in contrast to that which was obtained via stereotactic biopsy. Tumor samples acquired via stereotactic biopsy provide accurate information with regard to clinically relevant molecular markers that have been shown to impact patient care decisions. The profile of markers analyzed in our cohort was nearly concordant between those samples obtained via stereotactic biopsy or open craniotomy thereby suggesting that clinical decisions may be based on the molecular profile of the tumor samples obtained via stereotactic biopsy.

摘要

高级别胶质瘤的分类、治疗及预后已被证明与分子标志物的表达相关(如MGMT启动子甲基化和异柠檬酸脱氢酶1(IDH1)突变)。肿瘤样本可通过立体定向活检或开颅手术获取。在2009年至2013年期间,22例最初经立体定向活检诊断为高级别胶质瘤、最终接受开颅手术切除肿瘤的患者被前瞻性纳入一个机构性胶质瘤数据库。使用甲基化特异性(MS)-PCR进行MGMT启动子分析,使用免疫组织化学进行IDH1R132H突变分析。在通过立体定向活检获取的样本中,3例患者(13.7%)表现出IDH1R132H突变。立体定向活检获得的组织在10例患者(45.5%)中显示有MGMT启动子甲基化,而在10例患者(45.5%)中显示为非甲基化MGMT启动子;在我们的队列中,其余2例患者(9%)结果不确定。除1例患者外,所有患者在开颅手术期间获取的样本均证实了最初的组织学分级、IDH1R132H突变和MGMT启动子甲基化结果;与立体定向活检结果相反,此次MGMT启动子分析结果不确定。通过立体定向活检获取的肿瘤样本能提供有关临床相关分子标志物的准确信息,这些标志物已被证明会影响患者的治疗决策。我们队列中分析的标志物情况在通过立体定向活检或开颅手术获取的样本之间几乎一致,这表明临床决策可以基于通过立体定向活检获得的肿瘤样本的分子特征。

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