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首页> 外文期刊>Gynecologic Oncology: An International Journal >Improved detection of ovarian cancer metastases by intraoperative quantitative fluorescence protease imaging in a pre-clinical model.
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Improved detection of ovarian cancer metastases by intraoperative quantitative fluorescence protease imaging in a pre-clinical model.

机译:在临床前模型中通过术中定量荧光蛋白酶成像改进对卵巢癌转移的检测。

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OBJECTIVES: Cytoreductive surgery is a cornerstone of therapy in metastatic ovarian cancer. While conventional white light (WL) inspection detects many obvious tumor foci, careful histologic comparison has shown considerable miss rates for smaller foci. The goal of this study was to compare tumor detection using WL versus near infrared (NIR) imaging with a protease activatable probe, as well as to evaluate the ability to quantify NIR fluorescence using a novel quantitative optical imaging system. METHODS: A murine model for peritoneal carcinomatosis was generated and metastatic foci were imaged using WL and NIR imaging following the i.v. administration of the protease activatable probe ProSense750. The presence of tumor was confirmed by histology. Additionally, the ability to account for variations in fluorescence signal intensity due to changes in distance between the catheter and target lesion during laparoscopic procedures was evaluated. RESULTS: NIR imaging with a ProSense750 significantly improvedupon the target-to-background ratios (TBRs) of tumor foci in comparison to WL imaging (minimum improvement was approximately 3.5 fold). Based on 52 histologically validated samples, the sensitivity for WL imaging was 69%, while the sensitivity for NIR imaging was 100%. The effects of intraoperative distance changes upon fluorescence intensity were corrected in realtime, resulting in a decrease from 89% to 5% in signal variance during fluorescence laparoscopy. CONCLUSIONS: With its molecular specificity, low background autofluorescence, high TBRs, and quantitative signal, optical imaging with NIR protease activatable probes greatly improves upon the intraoperative detection of ovarian cancer metastases.
机译:目的:细胞减灭术是转移性卵巢癌治疗的基石。传统的白光(WL)检查可以检测到许多明显的肿瘤灶,但仔细的组织学比较显示,较小灶灶的漏诊率相当高。这项研究的目的是比较使用WL的肿瘤检测与使用可蛋白酶激活的探针的近红外(NIR)成像的比较,以及评估使用新型定量光学成像系统对NIR荧光进行定量的能力。方法:建立腹膜癌的小鼠模型,并在静脉内注射后使用WL和NIR成像对转移灶进行成像。蛋白酶激活探针ProSense750的使用。通过组织学证实肿瘤的存在。另外,评估了在腹腔镜手术期间由于导管和目标病变之间的距离变化导致的荧光信号强度变化的能力。结果:与WL成像相比,使用ProSense750进行NIR成像显着改善了肿瘤灶的目标背景比(TBR)(最小改善约为3.5倍)。根据52个经过组织学验证的样本,WL成像的灵敏度为69%,而NIR成像的灵敏度为100%。实时纠正术中距离变化对荧光强度的影响,从而在荧光腹腔镜检查期间将信号差异从89%降低到5%。结论:由于其分子特异性,低背景自发荧光,高TBR和定量信号,NIR蛋白酶可活化探针的光学成像可在术中检测卵巢癌转移时大大改善。

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