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使用靶向七肽和共聚焦显微内镜在体内检测结肠发育异常

Detection of colonic dysplasia in vivo using a targeted heptapeptide and confocal microendoscopy.

作者信息

Hsiung Pei-Lin, Hardy Jonathan, Friedland Shai, Soetikno Roy, Du Christine B, Wu Amy P, Sahbaie Peyman, Crawford James M, Lowe Anson W, Contag Christopher H, Wang Thomas D

机构信息

Department of Pediatrics, Radiology and Microbiology & Immunology, Stanford University School of Medicine, 318 Campus Dr., Rm. E-150, Stanford, California 94305, USA.

出版信息

Nat Med. 2008 Apr;14(4):454-8. doi: 10.1038/nm1692. Epub 2008 Mar 16.

Abstract

A combination of targeted probes and new imaging technologies provides a powerful set of tools with the potential to improve the early detection of cancer. To develop a probe for detecting colon cancer, we screened phage display peptide libraries against fresh human colonic adenomas for high-affinity ligands with preferential binding to premalignant tissue. We identified a specific heptapeptide sequence, VRPMPLQ, which we synthesized, conjugated with fluorescein and tested in patients undergoing colonoscopy. We imaged topically administered peptide using a fluorescence confocal microendoscope delivered through the instrument channel of a standard colonoscope. In vivo images were acquired at 12 frames per second with 50-microm working distance and 2.5-microm (transverse) and 20-microm (axial) resolution. The fluorescein-conjugated peptide bound more strongly to dysplastic colonocytes than to adjacent normal cells with 81% sensitivity and 82% specificity. This methodology represents a promising diagnostic imaging approach for the early detection of colorectal cancer and potentially of other epithelial malignancies.

摘要

靶向探针与新型成像技术相结合,提供了一套强大的工具,具有改善癌症早期检测的潜力。为了开发一种检测结肠癌的探针,我们针对新鲜人类结肠腺瘤筛选噬菌体展示肽库,以寻找与癌前组织优先结合的高亲和力配体。我们鉴定出一个特定的七肽序列VRPMPLQ,将其合成、与荧光素偶联,并在接受结肠镜检查的患者中进行测试。我们使用通过标准结肠镜器械通道递送的荧光共聚焦微型内窥镜对局部施用的肽进行成像。以每秒12帧的速度采集体内图像,工作距离为50微米,横向分辨率为2.5微米,轴向分辨率为20微米。与相邻正常细胞相比,荧光素偶联肽与发育异常结肠细胞的结合更强,灵敏度为81%,特异性为82%。这种方法代表了一种有前景的诊断成像方法,可用于早期检测结直肠癌以及其他上皮性恶性肿瘤。

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