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使用放射性标记的 DARPin Ec1 成像卵巢癌中 EpCAM 表达的可行性。

Feasibility of Imaging EpCAM Expression in Ovarian Cancer Using Radiolabeled DARPin Ec1.

机构信息

Department of Immunology, Genetics and Pathology, Uppsala University, 751 85 Uppsala, Sweden.

Research Centrum for Oncotheranostics, Research School of Chemistry and Applied Biomedical Sciences, Tomsk Polytechnic University, 634050 Tomsk, Russia.

出版信息

Int J Mol Sci. 2020 May 7;21(9):3310. doi: 10.3390/ijms21093310.

Abstract

Epithelial cell adhesion molecule (EpCAM) is overexpressed in 55%-75% of ovarian carcinomas (OC). EpCAM might be used as a target for a treatment of disseminated OC. Designed ankyrin repeats protein (DARPin) Ec1 is a small (18 kDa) protein, which binds to EpCAM with subnanomolar affinity. We tested a hypothesis that Ec1 labeled with a non-residualizing label might serve as a companion imaging diagnostic for stratification of patients for EpCAM-targeting therapy. Ec1 was labeled with I using N-succinimidyl--iodobenzoate. Binding affinity, specificity, and cellular processing of [I]I-PIB-Ec1 were evaluated using SKOV-3 and OVCAR-3 ovarian carcinoma cell lines. Biodistribution and tumor-targeting properties of [I]I-PIB-Ec1 were studied in Balb/c nu/nu mice bearing SKOV-3 and OVCAR-3 xenografts. EpCAM-negative Ramos lymphoma xenografts served as specificity control. Binding of [I]I-PIB-Ec1 to ovarian carcinoma cell lines was highly specific and had affinity in picomolar range. Slow internalization of [I]I-PIB-Ec1 by OC cells confirmed utility of non-residualizing label for in vivo imaging. [I]I-PIB-Ec1 provided 6 h after injection tumor-to-blood ratios of 30 ± 11 and 48 ± 12 for OVCAR-3 and SKOV-3 xenografts, respectively, and high contrast to other organs. Tumor targeting was highly specific. Saturation of tumor uptake at a high dose of Ec1 in SKOV-3 model provided a rationale for dose selection in further studies using therapeutic conjugates of Ec1 for targeted therapy. In conclusion, [I]I-PIB-Ec1 is a promising agent for visualizing EpCAM expression in OC.

摘要

上皮细胞黏附分子 (EpCAM) 在 55%-75%的卵巢癌 (OC) 中过表达。EpCAM 可能被用作治疗播散性 OC 的靶点。设计的锚蛋白重复蛋白 (DARPin) Ec1 是一种小的 (18 kDa) 蛋白,与 EpCAM 以亚纳摩尔亲和力结合。我们测试了一个假设,即用非残留标记物标记的 Ec1 可能作为一种伴随的成像诊断方法,用于分层接受 EpCAM 靶向治疗的患者。Ec1 用 N-琥珀酰亚胺基--碘代苯甲酸标记。使用 SKOV-3 和 OVCAR-3 卵巢癌细胞系评估 [I]I-PIB-Ec1 的结合亲和力、特异性和细胞处理。在携带 SKOV-3 和 OVCAR-3 异种移植物的 Balb/c nu/nu 小鼠中研究了 [I]I-PIB-Ec1 的生物分布和肿瘤靶向特性。EpCAM 阴性 Ramos 淋巴瘤异种移植物作为特异性对照。[I]I-PIB-Ec1 与卵巢癌细胞系的结合具有高度特异性,亲和力处于皮摩尔范围。OC 细胞中 [I]I-PIB-Ec1 的缓慢内化证实了非残留标记物在体内成像中的应用。注射后 6 小时,[I]I-PIB-Ec1 对 OVCAR-3 和 SKOV-3 异种移植物的肿瘤与血液比值分别为 30±11 和 48±12,与其他器官形成高对比。肿瘤靶向具有高度特异性。在 SKOV-3 模型中,高剂量 Ec1 对肿瘤摄取的饱和为进一步研究 Ec1 的治疗性缀合物用于靶向治疗提供了剂量选择的依据。总之,[I]I-PIB-Ec1 是一种很有前途的用于可视化 OC 中 EpCAM 表达的试剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f287/7246691/5f02935890d9/ijms-21-03310-g001.jpg

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