Detection of colon cancer metastases with fluorescence laparoscopy in orthotopic nude mouse models.

Rhiana S Menen, Sharmeela Kaushal, Cynthia S Snyder, Mark A Talamini, Robert M Hoffman, Michael Bouvet
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引用次数: 7

Abstract

Objective: To improve detection of colon cancer metastases using fluorescence laparoscopy (FL).

Design: An orthotopic mouse model of human colon cancer was established by intracecal injection of HCT-116 human colon cancer cells expressing green fluorescent protein into 12 mice. One group modeled early disease and the second modeled late metastatic disease. For the early-disease model, 2 weeks after implantation, 6 mice underwent 2 modalities of laparoscopy: bright field laparoscopy (BL) and FL. The number of metastases identified within each of the 4 abdominal quadrants was recorded with both laparoscopy modalities. This process was repeated in the late-metastatic disease group 4 weeks after implantation. All animals were then humanely sacrificed and imaged using open fluorescence laparoscopy (OL) as a positive control to identify metastases.

Setting: Basic science laboratory.

Participants: Twelve female, 6-week-old nude mice.

Interventions: Detection of tumor foci by FL compared with BL.

Main outcome measures: Number of tumors identified in each quadrant. RESULTS Fluorescence laparoscopy enabled superior visualization of colon cancer metastases compared with BL in the early (P = .03) and late (P = .002) models of colon cancer. Compared with OL, BL was significantly inferior in the early (P = .04) and late (P < .001) groups. Fluorescence laparoscopy was not significantly different from OL in the early (P = .85) or late (P = .46) group. Thus, FL allowed identification of micrometastases that could not be distinguished from surrounding tissue using BL.

Conclusions: The use of FL enables identification of metastases that could not be visualized using standard laparoscopy. This report illustrates the important clinical potential for FL in the surgical treatment of cancer.

荧光腹腔镜在原位裸鼠模型中检测结肠癌转移。
目的:提高荧光腹腔镜(FL)对结肠癌转移的检测水平。设计:将表达绿色荧光蛋白的HCT-116人结肠癌细胞注入12只小鼠,建立人结肠癌原位小鼠模型。一组模拟早期疾病,另一组模拟晚期转移性疾病。对于早期疾病模型,在植入后2周,6只小鼠进行了两种腹腔镜检查:亮场腹腔镜检查(BL)和FL。两种腹腔镜检查方式记录了4个腹部象限内每一个象限内发现的转移瘤数量。这一过程在移植后4周的晚期转移性疾病组重复。然后将所有动物人道处死,并使用开放荧光腹腔镜(OL)作为阳性对照进行成像以确定转移。单位:基础科学实验室。参与者:12只6周大的雌性裸鼠。干预措施:比较FL和bl检测肿瘤病灶。主要结局指标:每个象限中发现的肿瘤数量。结果在结肠癌早期(P = 0.03)和晚期(P = 0.002)模型中,与BL相比,荧光腹腔镜能更好地显示结肠癌转移灶。早期组(P = 0.04)和晚期组(P < 0.001)的BL明显低于对照组(P < 0.01)。荧光腹腔镜在早期组(P = 0.85)和晚期组(P = 0.46)与OL组无显著差异。因此,FL可以识别无法与bl区分的微转移灶。结论:使用FL可以识别标准腹腔镜无法观察到的转移灶。本报告说明了FL在肿瘤手术治疗中的重要临床潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Archives of Surgery
Archives of Surgery 医学-外科
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4-8 weeks
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