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在无框架神经导航针活检的术中新鲜组织切片上检测 IDH1 突变和 MGMT 启动子状态。对 17 例不符合开颅和肿瘤切除条件的脑胶质肿瘤患者进行分析。

Detection of IDH1 mutations and the status of MGMT promoter on intraoperative fresh tissue section from frameless neuronavigation needle biopsy. Analysis on 17 patients with brain glial tumor ineligible for craniotomy and tumor resection.

机构信息

Hub and Spoke Neurosurgery Unit-Emergency Department, University Hospital of Parma, Parma, Italy.

出版信息

Int J Immunopathol Pharmacol. 2011 Apr-Jun;24(2 Suppl):45-50. doi: 10.1177/03946320110240S209.

Abstract

It is well known that primary and secondary glioblastomas are histologically largely indistinguishable. Therefore, the detection of IDH1 mutations or the status of the MGMT promoter on a simple bioptic sample could be one of major diagnostic and prognostic importance for glial patients that complements clinical criteria for distinguishing secondary from primary glioblastomas and to predict a more favourable prognosis. Currently, biopsy is the method of choice to obtain tissue from intracranial lesions with uncertain neurodiagnostic findings or in deep locations, with a minimal invasive approach. The needle biopsy with frameless neuronavigation could provide a sampling with elevated diagnostic yield and high concentration of DNA, due to the "image-guided" computer assisted technique of needle insertion through the most neurodiagnostic representative tumor area. The freezing of fresh tumor tissue at biopsy could greatly improve the success of DNA extraction. The concentration of the DNA samples can also improved from a withdrawal in an area with high probability of neoplastic cells. The present study reports the results of 17 patients who had undergone frameless image-guided intracranial needle biopsy from April 2008 until July 2010 at Neurosurgery Unit of the "Arcispedale Santa Maria Nuova" of Reggio Emilia. For these patients the molecular determination of MGMT promoter was assessed with the Nested-Methylation Specific-Polymerase Chain Reaction and the screening of mutations in IDH1 e IDH2 genes was performer by polymerase chain reaction (PCR) and direct sequencing on fresh or cryopreserved needle bioptic tissue.

摘要

众所周知,原发性和继发性胶质母细胞瘤在组织学上大多无法区分。因此,在简单的活检样本中检测 IDH1 突变或 MGMT 启动子的状态可能是胶质母细胞瘤患者的主要诊断和预后指标之一,有助于补充用于区分继发性和原发性胶质母细胞瘤的临床标准,并预测更有利的预后。目前,活检是获得颅内病变组织的首选方法,这些病变组织的神经诊断结果不确定或位于深部,且具有微创性。无框架神经导航下的针吸活检可以通过“图像引导”的计算机辅助技术,通过最具神经诊断代表性的肿瘤区域插入针头,从而提高采样的诊断率和 DNA 浓度。在活检时对新鲜肿瘤组织进行冷冻处理,可以大大提高 DNA 提取的成功率。还可以从肿瘤细胞高概率存在的区域提高 DNA 样本的浓度。本研究报告了 2008 年 4 月至 2010 年 7 月在雷焦艾米利亚的“Arcispedale Santa Maria Nuova”神经外科进行的 17 例无框架图像引导颅内针吸活检患者的结果。对这些患者,使用巢式甲基化特异性聚合酶链反应(Nested-Methylation Specific-Polymerase Chain Reaction)评估 MGMT 启动子的分子测定,通过聚合酶链反应(PCR)和直接测序对新鲜或冷冻的针吸活检组织进行 IDH1 和 IDH2 基因突变的筛选。

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