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Fluorescence-based SMC and OCT endoscope to study aberrant crypt foci in the mouse colon

机译:基于荧光的SMC和OCT内窥镜研究小鼠结肠隐窝病灶

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The accepted model of colorectal cancer assumes the paradigm that aberrant crypt foci (ACF) are the earliest events in tumorigenesis and develop into adenoma, which further develop into adenocarcinoma. Under this assumption, basic research and drug studies have been performed using ACF as substitute markers for fully developed carcinoma. While studies have shown a correlation between the number of ACF present and the presence of adenoma/adenocarcinoma, a causal relationship has yet to be determined. The mouse has shown to be an excellent model for colorectal cancer; however, the outcomes of such experiments require sacrifice and histologic examination of ex vivo tissue. To better utilize the mouse model to study ACF and adenoma development, an endoscope was constructed for non-destructive in vivo surface visualization, molecular imaging and cross-sectional imaging of the colon. Our system combines surface magnifying chromoendoscopy (SMC) and optical coherence tomography (OCT) to image colon microstructure. Sixteen mice, treated with the carcinogen azoxymethane, were imaged at 2 week intervals, to visualize carcinogenesis events. With this dual-modality system we are able to visualize crypt structure alteration over time as well as adenoma development over time.
机译:公认的大肠癌模型假设范式是:隐窝灶(ACF)是肿瘤发生中最早的事件,并发展为腺瘤,然后进一步发展为腺癌。在此假设下,已经使用ACF作为完全发展的癌症的替代标记物进行了基础研究和药物研究。尽管研究表明存在的ACF数量与腺瘤/腺癌的存在之间存在相关性,但尚未确定因果关系。小鼠已被证明是结直肠癌的优秀模型。然而,这些实验的结果需要牺牲和离体组织的组织学检查。为了更好地利用小鼠模型来研究ACF和腺瘤的发展,构建了一种内窥镜,用于结肠的体内无损表面可视化,分子成像和横断面成像。我们的系统结合了表面放大色谱内镜(SMC)和光学相干断层扫描(OCT)来成像结肠微结构。每隔2周对用致癌物甲氧甲烷处理的16只小鼠进行成像,以观察致癌事件。通过这种双模态系统,我们能够直观地看到隐窝结构随时间变化以及腺瘤随时间变化的情况。

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