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使用铟 - 111 - DTPA - D - 苯丙氨酸 - 1 - 奥曲肽进行中肠类癌综合征的全身放射性核素治疗。

Systemic radionuclide therapy using indium-111-DTPA-D-Phe1-octreotide in midgut carcinoid syndrome.

作者信息

Fjälling M, Andersson P, Forssell-Aronsson E, Grétarsdóttir J, Johansson V, Tisell L E, Wängberg B, Nilsson O, Berg G, Michanek A, Lindstedt G, Ahlman H

机构信息

Department of Nuclear Medicine, Sahlgrenska University Hospital, Göteborg, Sweden.

出版信息

J Nucl Med. 1996 Sep;37(9):1519-21.

PMID:8790206
Abstract

A 55-yr-old woman with a midgut carcinoid syndrome due to metastatic spread of an ileal tumor to the liver, paraortic and mediastinal lymph nodes and to the skeleton was given systemic radionuclide therapy with 111In-DTPA-D-Phe1-octreotide. Before therapy, dosimetric calculations were performed on whole-body scintigraphs and 111In retention was shown to be long-lasting. Excretion was mainly seen during the first 24 hr after injection; thereafter whole-body retention remained stationary at 30%. Indium-111 activity in tumor biopsies and blood was measured using a gamma counter. Very high tumor-to-blood ratios were obtained: 150 for the primary tumor and 400-650 for liver metastases, which further justified radiation therapy. Indium-111-DTPA-D-Phe1-octreotide treatment was given on three separate occasions (3.0, 3.5 and 3.1 GBq) 8 and 4 wk apart. After each therapy, the patient experienced facial flush and pain over the skeletal lesions followed by symptomatic relief, even though no objective tumor regression was found radiologically after 5 mo. After initiation of octreotide treatment, there was a 14% reduction of the main tumor marker, urinary 5-HIAA. After three subsequent radionuclide therapies, there was a further 31% reduction of 5-HIAA levels. No adverse reactions, other than a slight decrease in leukocyte counts, were seen. The mean absorbed radiation dose after the three treatments was estimated to be about 10-12 Gy in liver metastases and 3-6 Gy in other tumors, depending on the size and location of the metastases. Assuming internalization of 111In into tumor cells and a radiobiological effect from short range Auger and conversion electrons, there might be a therapeutic effect on the tumor.

摘要

一名55岁女性,因回肠肿瘤转移至肝脏、腹主动脉旁和纵隔淋巴结以及骨骼而患有中肠类癌综合征,接受了用111In-DTPA-D-Phe1-奥曲肽进行的全身放射性核素治疗。治疗前,对全身闪烁扫描图进行了剂量计算,结果显示111In滞留时间持久。排泄主要发生在注射后的头24小时内;此后全身滞留率保持在30%不变。使用γ计数器测量肿瘤活检组织和血液中的铟-111活性。获得了非常高的肿瘤与血液比值:原发肿瘤为150,肝转移瘤为400 - 650,这进一步证明了放射治疗的合理性。111In-DTPA-D-Phe1-奥曲肽分三次(分别为3.0、3.5和3.1 GBq)给药,间隔8周和4周。每次治疗后,患者出现面部潮红和骨骼病变部位疼痛,随后症状缓解,尽管5个月后影像学检查未发现客观的肿瘤消退。开始奥曲肽治疗后,主要肿瘤标志物尿5-羟吲哚乙酸(5-HIAA)降低了14%。在随后的三次放射性核素治疗后,5-HIAA水平又进一步降低了31%。除白细胞计数略有下降外,未观察到其他不良反应。根据转移灶的大小和位置,三次治疗后肝脏转移灶的平均吸收辐射剂量估计约为10 - 12 Gy,其他肿瘤为三3 - 6 Gy。假设111In内化进入肿瘤细胞并产生来自短程俄歇电子和转换电子的放射生物学效应,可能对肿瘤有治疗作用。

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