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脑肿瘤放疗和/或动脉内化疗后的脑坏死:PET与神经病理学研究

Cerebral necrosis after radiotherapy and/or intraarterial chemotherapy for brain tumors: PET and neuropathologic studies.

作者信息

Di Chiro G, Oldfield E, Wright D C, De Michele D, Katz D A, Patronas N J, Doppman J L, Larson S M, Ito M, Kufta C V

机构信息

Neuroimaging Section, National Institute of Neurological and Communicative Disorders and Stroke, Bethesda, MD 20892.

出版信息

AJR Am J Roentgenol. 1988 Jan;150(1):189-97. doi: 10.2214/ajr.150.1.189.

Abstract

Cerebral necrosis after radiotherapy for brain tumors is being recognized as a problem more common than previously estimated. Distinction between this iatrogenic complication and tumor recurrence cannot be made by either CT or MR imaging. By using positron emission tomography (PET) with 18F-deoxyglucose (FDG) we were able to reach a diagnosis of radiation necrosis, later verified, in 10 of 95 patients referred for the purpose of differentiating tumor recurrence from necrosis. The critical PET-FDG feature was focal hypometabolism in the area of necrosis, which contrasted with the hypermetabolism associated with the residual/recurrent tumor. In addition, four cases of cerebral necrosis after supraophthalmic, intraarterial chemotherapy (BCNU) were studied with the PET-FDG method. The area of chemotherapy damage was also characterized by marked hypometabolism. Histology revealed both similarities and differences between radio- and chemonecrosis.

摘要

脑肿瘤放疗后发生的脑坏死,正被视为一个比先前估计更为常见的问题。通过CT或磁共振成像(MR)无法区分这种医源性并发症与肿瘤复发。通过使用18F-脱氧葡萄糖(FDG)正电子发射断层扫描(PET),我们得以在95例因区分肿瘤复发与坏死而转诊的患者中,对10例做出了放射性坏死的诊断,该诊断随后得到证实。PET-FDG的关键特征是坏死区域出现局灶性代谢减低,这与残留/复发性肿瘤相关的代谢增高形成对比。此外,还采用PET-FDG方法对4例经眼动脉内化疗(卡氮芥)后发生脑坏死的病例进行了研究。化疗损伤区域也表现为明显的代谢减低。组织学显示放射性坏死与化学性坏死既有相似之处,也有不同之处。

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