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术中隐匿性神经母细胞瘤的检测与切除:一种利用生长抑素受体表达的技术

Intraoperative detection and resection of occult neuroblastoma: a technique exploiting somatostatin receptor expression.

作者信息

Martinez D A, O'Dorisio M S, O'Dorisio T M, Qualman S J, Caniano D A, Teich S, Besner G E, King D R

机构信息

Department of Pediatrics, Ohio State University College of Medicine, Columbus 43205-2696, USA.

出版信息

J Pediatr Surg. 1995 Nov;30(11):1580-9. doi: 10.1016/0022-3468(95)90161-2.

Abstract

Tumor cell expression of specific high-affinity somatostatin receptors has been associated with a favorable prognosis in children with neuroblastoma. The purpose of this study was (1) to document intraoperatively the in vivo binding of the somatostatin analogue 125I-tyr3-octreotide to high-affinity somatostatin receptors expressed on human neuroblastoma, using a hand-held gamma detector; (2) to determine whether gamma-probe detection of radioligand binding to tumor receptors could identify occult malignancy; and (3) to determine the safety and biodistribution of 125I-tyr3-octreotide in children. Six children with stage III or IV neuroblastoma received an intravenous injection of 125I-tyr3-octreotide and underwent operative exploration using gamma-probe detection of radioligand binding to tumor somatostatin receptors. Tissue that demonstrated in vivo binding of 125I-tyr3-octreotide, or that was suspicious for tumor, was extirpated and analyzed by histopathology, immunohistochemistry, and microautoradiography. The biodistribution of 125I-tyr3-octreotide was recorded intraoperatively over time. Tumor tissue from each child also was assayed in vitro for somatostatin receptor expression by competitive binding studies using 125I-tyr3-octreotide. In vivo binding of 125I-tyr3-octreotide to malignant tissue was documented in the five children with a known tumor burden. Seventeen sites of radioreceptor binding were amenable to resection. Histopathological analysis confirmed neuroblastoma in 15 of these specimens. Four of the 15 proven tumor foci were occult malignancies. Every site of histologically proven neuroblastoma demonstrated in vivo binding of 125I-tyr3-octreotide. Five of seven sites histologically negative for neuroblastoma also were negative for in vivo radioreceptor binding. Microautoradiography confirmed in vivo binding of 125I-tyr3-octreotide to tumor cells. Uptake of 125I-tyr3-octreotide in abdominal organs occurred within 15 minutes of injection, was highest in the liver and gallbladder, and decreased over 24 hours. The conclusions were as follows. (1) 125I-tyr3-octreotide binds, in vivo, to somatostatin receptors on neuroblastoma, with 100% sensitivity and 71% specificity. (2) Occult neuroblastoma is found through gamma-probe detection of radioligand binding to receptors. (2) The biodistribution of 125I-tyr3-octreotide reflects the hepatobiliary clearance of this radionuclide. (4) Radioreceptor-guided surgery may safely provide more complete operative staging and cytoreduction of neuroblastoma.

摘要

肿瘤细胞表达特定的高亲和力生长抑素受体与神经母细胞瘤患儿的良好预后相关。本研究的目的是:(1)使用手持式γ探测器在术中记录生长抑素类似物125I-酪氨酰3-奥曲肽与人神经母细胞瘤上表达的高亲和力生长抑素受体的体内结合情况;(2)确定γ探针检测放射性配体与肿瘤受体的结合是否能识别隐匿性恶性肿瘤;(3)确定125I-酪氨酰3-奥曲肽在儿童中的安全性和生物分布。6例Ⅲ期或Ⅳ期神经母细胞瘤患儿静脉注射125I-酪氨酰3-奥曲肽,并使用γ探针检测放射性配体与肿瘤生长抑素受体的结合情况进行手术探查。显示有125I-酪氨酰3-奥曲肽体内结合或怀疑为肿瘤的组织被切除,并通过组织病理学、免疫组织化学和微放射自显影进行分析。术中记录125I-酪氨酰3-奥曲肽随时间的生物分布情况。还通过使用125I-酪氨酰3-奥曲肽的竞争性结合研究,对每个患儿的肿瘤组织进行体外生长抑素受体表达检测。在5例已知肿瘤负荷的患儿中记录到125I-酪氨酰3-奥曲肽与恶性组织的体内结合情况。17个放射性受体结合部位适合切除。组织病理学分析在其中15个标本中证实为神经母细胞瘤。15个经证实的肿瘤病灶中有4个为隐匿性恶性肿瘤。组织学证实为神经母细胞瘤的每个部位均显示有125I-酪氨酰3-奥曲肽的体内结合。7个组织学检查神经母细胞瘤阴性的部位中有5个在体内放射性受体结合检查中也为阴性。微放射自显影证实125I-酪氨酰3-奥曲肽与肿瘤细胞的体内结合。125I-酪氨酰3-奥曲肽在注射后15分钟内在腹部器官中摄取,在肝脏和胆囊中最高,并在24小时内下降。结论如下:(1)125I-酪氨酰3-奥曲肽在体内与神经母细胞瘤上的生长抑素受体结合,敏感性为100%,特异性为71%。(2)通过γ探针检测放射性配体与受体的结合发现隐匿性神经母细胞瘤。(三)125I-酪氨酰3-奥曲肽的生物分布反映了该放射性核素的肝胆清除情况。(4)放射性受体引导的手术可安全地提供更完整的手术分期和神经母细胞瘤的细胞减灭。

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