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使用针对 EpCAM 的定量近红外荧光分子成像进行肿瘤边缘检测,远红基因报告 iRFP 验证。

Tumor margin detection using quantitative NIRF molecular imaging targeting EpCAM validated by far red gene reporter iRFP.

机构信息

Center for Molecular Imaging, The Brown Foundation Institute of Molecular Medicine, The University of Texas Health Science Center, 1825 Pressler Street, Houston, TX, 77030, USA.

出版信息

Mol Imaging Biol. 2013 Oct;15(5):560-8. doi: 10.1007/s11307-013-0637-8.

Abstract

PURPOSE

Wide-field surgical excision reduces the chance of residual disease, but can also lead to disfigurement and devastating morbidities when resection is close to critical structures. We hypothesize that near-infrared fluorescence (NIRF) imaging can enable accurate detection of tumor margins for image-guided resection.

EXPERIMENTAL DESIGN

An orthotopic model of human prostate cancer (PCa) was used to assess primary tumor margins using a NIRF-labeled antibody against epithelial cell adhesion molecule (EpCAM). PCa cells stably expressing far red fluorescent gene reporter, iRFP, enabled colocalization with NIRF signals for direct assessment of tumor margins.

RESULTS

Using receiver operating characteristic analysis, far red fluorescence was validated against standard pathology of primary and metastatic lesions with >96 % accuracy. Primary tumor margins were more accurately detected by quantitative NIRF imaging using the EpCAM-targeting antibody as compared to a NIRF-labeled isotype control antibody.

CONCLUSIONS

NIRF molecular imaging may enable real-time and accurate assessment of tumor margins.

摘要

目的

广泛的手术切除可以降低残留疾病的机会,但当切除接近关键结构时,也可能导致毁容和严重的病态。我们假设近红外荧光(NIRF)成像可以实现对肿瘤边界的准确检测,从而进行图像引导切除。

实验设计

使用人前列腺癌(PCa)的原位模型,使用针对上皮细胞黏附分子(EpCAM)的 NIRF 标记抗体来评估原发性肿瘤边界。稳定表达远红荧光基因报告基因 iRFP 的 PCa 细胞可与 NIRF 信号共定位,从而直接评估肿瘤边界。

结果

使用受试者工作特征分析,远红荧光与原发性和转移性病变的标准病理学相比具有 >96%的准确率。与 NIRF 标记的同种型对照抗体相比,使用针对 EpCAM 的靶向抗体进行定量 NIRF 成像可以更准确地检测原发性肿瘤边界。

结论

NIRF 分子成像可能能够实时、准确地评估肿瘤边界。

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