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胶质肿瘤的计算机断层扫描与组织学边界:肿瘤类型及体积切除的选择

Computed tomography and histologic limits in glial neoplasms: tumor types and selection for volumetric resection.

作者信息

Kelly P J

机构信息

Department of Neurosurgery, Mayo Clinic, Rochester, MN 55905.

出版信息

Surg Neurol. 1993 Jun;39(6):458-65. doi: 10.1016/0090-3019(93)90031-u.

Abstract

Selective and accurate resection of any computed tomography (CT) or magnetic resonance imaging (MRI) defined intracranial volume is possible by employing imaging-based computer-assisted volumetric stereotactic methods. Although the target volume can be any intracranial lesion, volumetric resection techniques were most frequently applied to the most commonly referred intraaxial lesions: glial neoplasms located in eloquent brain regions. Requirements for understanding of glial neoplasms as target volumes prompted investigations of the three-dimensional spatial configuration of these lesions, their histologic margins, and the accuracy with which these margins could be detected on CT and MRI. Stereotactic serial biopsy studies have shown that glial neoplasms frequently comprise two elements: tumor tissue and isolated tumor cells which infiltrate brain parenchyma. The tumor tissue component of high grade gliomas is most accurately defined by the volume which exhibits contrast enhancement. However, tumor tissue in low grade (nonpilocytic) gliomas is usually indistinguishable from infiltrated parenchyma on CT and MRI; both are hypodense on CT and do not usually exhibit contrast enhancement. Stereotactic serial biopsy is the only reliable method by which CT hypodense tumor tissue can be differentiated from infiltrated parenchyma in low grade (nonpilocytic) astrocytomas, oligodendrogliomas, and mixed gliomas. Stereotactic volumetric resection of infiltrated parenchyma defined by CT/MRI is advisable only in nonessential brain regions. In eloquent brain areas, stereotactic resection is appropriate for the glial tumor tissue component of high grade glial neoplasms, pilocytic astrocytomas, and low grade CT hypodense gliomas in which a stereotactic serial biopsy procedure has confirmed tumor tissue only.

摘要

通过采用基于成像的计算机辅助容积立体定向方法,可以对任何计算机断层扫描(CT)或磁共振成像(MRI)定义的颅内体积进行选择性和精确切除。尽管目标体积可以是任何颅内病变,但容积切除技术最常应用于最常见的轴内病变:位于明确脑区的胶质肿瘤。将胶质肿瘤作为目标体积进行理解的需求促使人们对这些病变的三维空间构型、组织学边界以及在CT和MRI上检测这些边界的准确性进行研究。立体定向系列活检研究表明,胶质肿瘤通常包含两个成分:肿瘤组织和浸润脑实质的孤立肿瘤细胞。高级别胶质瘤的肿瘤组织成分最准确地由显示对比增强的体积来定义。然而,低级别(非毛细胞型)胶质瘤中的肿瘤组织在CT和MRI上通常与浸润的实质难以区分;两者在CT上均为低密度,通常不显示对比增强。立体定向系列活检是区分低级别(非毛细胞型)星形细胞瘤、少突胶质细胞瘤和混合性胶质瘤中CT低密度肿瘤组织与浸润实质的唯一可靠方法。仅在非重要脑区建议对由CT/MRI定义的浸润实质进行立体定向容积切除。在明确的脑区,立体定向切除适用于高级别胶质肿瘤的胶质肿瘤组织成分、毛细胞型星形细胞瘤以及低级别CT低密度胶质瘤,其中立体定向系列活检程序仅证实了肿瘤组织。

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