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Evaluation of New Morphometric Parameters of Neoangiogenesis in Human Colorectal Cancer Using Confocal Laser Endomicroscopy (CLE) and Targeted Panendothelial Markers

机译:使用共聚焦激光内窥镜检查(CLE)和靶向血管内皮标记物评估人大肠癌新血管生成的新形态计量学参数

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摘要

The tumor microcirculation is characterized by an abnormal vascular network with dilated, tortuous and saccular vessels. Therefore, imaging the tumor vasculature and determining its morphometric characteristics represent a critical goal for optimizing the cancer treatment that targets the blood vessels (i.e. antiangiogenesis therapy). The aim of this study was to evaluate new vascular morphometric parameters in colorectal cancer, difficult to achieve through conventional immunohistochemistry, by using the confocal laser endomicroscopy method. Fresh biopsies from tumor and normal tissue were collected during colonoscopy from five patients with T3 colorectal carcinoma without metastasis and were marked with fluorescently labeled anti-CD31 antibodies. A series of optical slices spanning 250 µm inside the tissue were immediately collected for each sample using a confocal laser endomicroscope. All measurements were expressed as the mean ± standard error. The mean diameter of tumor vessels was significantly larger than the normal vessels (9.46±0.4 µm vs. 7.60±0.3 µm, p = 0.0166). The vessel density was also significantly higher in the cancer vs. normal tissue samples (5541.05±262.81 vs. 3755.79±194.96 vessels/mm3, p = 0.0006). These results were confirmed by immunohistochemistry. In addition, the tortuosity index and vessel lengths were not significantly different (1.05±0.016 and 28.30±3.27 µm in normal tissue, vs. 1.07±0.008 and 26.49±3.18 µm in tumor tissue respectively, p = 0.5357 and p = 0.7033). The daughter/mother ratio (ratio of the sum of the squares of daughter vessel radii over the square of the mother vessel radius) was 1.15±0.09 in normal tissue, and 1.21±0.08 in tumor tissue (p = 0.6531). The confocal laser endomicroscopy is feasible for measuring more vascular parameters from fresh tumor biopsies than conventional immunohistochemistry alone. Provided new contrast agents will be clinically available, future in vivo use of CLE could lead to identification of novel biomarkers based on the morphometric characteristics of tumor vasculature.
机译:肿瘤微循环的特征是具有扩张的,曲折的和囊状血管的异常血管网络。因此,对肿瘤脉管系统进行成像并确定其形态特征代表了优化针对血管的癌症治疗(即抗血管生成治疗)的关键目标。这项研究的目的是通过使用共聚焦激光内窥镜检查方法来评估大肠癌中新的血管形态参数,这是常规免疫组织化学难以达到的。在结肠镜检查期间从五名无转移的T3大肠癌患者的结肠镜检查中收集了来自肿瘤和正常组织的新鲜活检样本,并用荧光标记的抗CD31抗体进行了标记。使用共聚焦激光内窥镜立即为每个样品收集一系列组织内部250 µm的光学切片。所有测量值均表示为平均值±标准误差。肿瘤血管的平均直径明显大于正常血管(9.46±0.4 µm对7.60±0.3 µm,p = 0.0166)。与正常组织样品相比,癌症中的血管密度也显着更高(5541.05±262.81 vs. 3755.79±194.96血管/ mm 3 ,p = 0.0006)。免疫组织化学证实了这些结果。另外,曲折指数和血管长度没有显着差异(正常组织为1.05±0.016和28.30±3.27 µm,而肿瘤组织分别为1.07±0.008和26.49±3.18 µm,p = 0.5357和p = 0.7033)。正常组织中的子母比(子管半径的平方和与子管半径的平方之比)在肿瘤组织中为1.15±0.09,在肿瘤组织中为1.21±0.08(p = 0.6531)。共聚焦激光内窥镜检查比单独的常规免疫组织化学方法可用于测量新鲜肿瘤活检中的更多血管参数。如果有新的造影剂在临床上可用,将来在体内使用CLE可能会导致基于肿瘤脉管系统形态特征的新型生物标志物的鉴定。

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