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胰腺癌靶向性的改善:一种新型双特异性抗体的实验研究,免疫闪烁显像的预靶向增强系统

Improved targeting of pancreatic cancer: experimental studies of a new bispecific antibody, pretargeting enhancement system for immunoscintigraphy.

作者信息

Cardillo Thomas M, Karacay Habibe, Goldenberg David M, Yeldell Dion, Chang Chien-Hsing, Modrak David E, Sharkey Robert M, Gold David V

机构信息

Garden State Cancer Center, Belleville, New Jersey 07109, USA.

出版信息

Clin Cancer Res. 2004 May 15;10(10):3552-61. doi: 10.1158/1078-0432.CCR-03-0340.

Abstract

PURPOSE

The early detection and diagnosis of pancreatic cancer remains a major clinical challenge in which imaging procedures have a central role. The purpose of this study was to evaluate a pretargeting method with a bispecific PAM4 (bsPAM4; anti-MUC1) antibody for radioimmunoscintigraphy of experimental human pancreatic cancer.

EXPERIMENTAL DESIGN

A bispecific F(ab')(2) antibody was generated from chimeric PAM4 Fab' and murine 734 (anti-indium-diethylenetriaminepentaacetic acid) Fab' fragments and then used in conjunction with 2 peptide haptens ((111)In-IMP-156 and (99m)Tc-IMP-192). Biodistribution studies and radioimmunoscintigraphic imaging properties of the radiolabeled bsPAM4, and pretargeted, radiolabeled peptides were examined in the CaPan1 human pancreatic tumor grown as s.c. xenografts in athymic nude mice. Tumor uptake and tumor:nontumor ratios were compared with a nontargeting irrelevant anti-CD20, bispecific rituximab, radiolabeled peptides alone, and with directly labeled PAM4.

RESULTS

Biodistribution results indicated significantly greater tumor uptake of radiolabeled peptides at 3 h after injection when pretargeting was performed with bsPAM4 as compared with the bispecific rituximab [20.2 +/- 5.5 percentage of injected dose per gram of tissue (%ID/g) versus 0.9 +/- 0.1%ID/g, respectively, for (111)In-IMP-156, and 16.8 +/- 4.8%ID/g versus 1.1 +/- 0.2%ID/g, respectively, for (99m)Tc-IMP-192]. Similar results were obtained at the 24-h time point. Tumor:nontumor ratios were >30 for all of the tissues except the kidneys, where a ratio of 7.8 +/- 2.8 was observed. By immunoscintigraphy, tumors could be visualized as early as 30 min after injection of the radiolabeled peptide.

CONCLUSIONS

These studies demonstrate the feasibility of using the pretargeted, bispecific antibody technology for nuclear imaging of pancreatic cancer. The advantage of pretargeted bsPAM4 antibody as an imaging platform is the high specificity for pancreatic cancer as compared with the physicochemical parameters identified by current imaging technologies.

摘要

目的

胰腺癌的早期检测和诊断仍然是一项重大临床挑战,其中成像程序起着核心作用。本研究的目的是评估一种使用双特异性PAM4(bsPAM4;抗MUC1)抗体的预靶向方法用于实验性人类胰腺癌的放射免疫闪烁成像。

实验设计

从嵌合PAM4 Fab'片段和鼠源734(抗铟-二乙烯三胺五乙酸)Fab'片段生成双特异性F(ab')(2)抗体,然后与2种肽半抗原((111)In-IMP-156和(99m)Tc-IMP-192)联合使用。在无胸腺裸鼠皮下生长的CaPan1人胰腺肿瘤中检查放射性标记的bsPAM4以及预靶向的放射性标记肽的生物分布研究和放射免疫闪烁成像特性。将肿瘤摄取和肿瘤与非肿瘤比值与非靶向无关抗CD20、双特异性利妥昔单抗、单独的放射性标记肽以及直接标记的PAM4进行比较。

结果

生物分布结果表明,与双特异性利妥昔单抗相比,当用bsPAM4进行预靶向时,注射后3小时放射性标记肽在肿瘤中的摄取显著更高(对于(111)In-IMP-156,分别为每克组织20.2±5.5%注射剂量(%ID/g)对0.9±0.1%ID/g,对于(99m)Tc-IMP-192,分别为16.8±4.8%ID/g对1.1±0.2%ID/g)。在24小时时间点获得了类似结果。除肾脏外,所有组织的肿瘤与非肿瘤比值均>30,在肾脏中观察到的比值为7.8±2.8。通过免疫闪烁成像,在注射放射性标记肽后30分钟即可观察到肿瘤。

结论

这些研究证明了使用预靶向双特异性抗体技术进行胰腺癌核成像的可行性。与当前成像技术确定的物理化学参数相比,预靶向bsPAM4抗体作为成像平台的优势在于对胰腺癌具有高特异性。

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