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首页> 外文期刊>Radiology >Changes of intratumoral microvessels and blood perfusion during establishment of hepatic metastases in mice.
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Changes of intratumoral microvessels and blood perfusion during establishment of hepatic metastases in mice.

机译:小鼠肝转移建立过程中肿瘤内微血管的变化和血液灌流。

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PURPOSE: To prospectively evaluate the stepwise changes that occur in intratumoral microvessels and microcirculation during the establishment of murine colonic hepatic metastases by using in vivo fluorescent microscopy and to compare the changes with tumor angiogenesis evaluated with an immunohistochemical study. MATERIALS AND METHODS: This study was approved by the institutional animal care and use committee. Twenty-five mice with hepatic metastases created with injection of murine colonic adenocarcinoma (colon 26) tumor cells into the spleen were examined with in vivo microscopy and immunohistochemical study for CD34, intracellular adhesion molecule (ICAM-1), and alpha smooth muscle actin (alpha-SMA). The tumor size, microcirculation in tumors, intratumoral microvessel density (MVD), afferent MVD, and CD34-positive MVD were evaluated. The data among the tumors that showed different hemodynamic or immunohistochemical patterns were compared with the Kruskal-Wallis test and the Student t test. RESULTS: Four stepwise patterns were observed according to the changes in morphology, hemodynamics, and immunohistochemical characteristics of intratumoral microvessels during the establishment of hepatic metastases, as follows: metastases without definite intratumoral blood perfusion or any intratumoral microvessels (mean diameter, approximately 180 microm), metastases with portal perfusion and intratumoral ICAM-1-positive residual hepatic sinusoids (mean diameter, approximately 290 microm), metastases with mixed portal and arterial perfusion and increased CD34-positive microvessels and alpha-SMA-positive arterioles (mean diameter, approximately 520 microm), and metastases with exclusively arterial perfusion and increased CD34-positive microvessels and alpha-SMA-positive arterioles (mean diameter, >2000 microm). The differences among the mean sizes of the tumors that showed these four patterns were statistically significant (P < .01). CONCLUSION: Stepwise changes of intratumoral microcirculation were revealed from direct diffusion, to portal perfusion, to mixed portal and arterial perfusion, and finally to arterial perfusion in accordance with stepwise tumor neovascularization during the growth of murine colonic hepatic metastases.
机译:目的:通过使用体内荧光显微镜前瞻性评估在鼠结肠肝转移建立过程中肿瘤内微血管和微循环中发生的逐步变化,并将其与免疫组织化学研究评估的肿瘤血管生成进行比较。材料与方法:本研究得到机构动物护理和使用委员会的批准。通过体内显微镜检查和CD34,细胞内黏附分子(ICAM-1)和α平滑肌肌动蛋白(CD34)的免疫组化研究,检查了通过将鼠类结肠腺癌(结肠26)肿瘤细胞注入脾脏而形成的25只具有肝转移的小鼠。 alpha-SMA)。评估肿瘤大小,肿瘤中的微循环,肿瘤内微血管密度(MVD),传入MVD和CD34阳性MVD。将显示出不同血液动力学或免疫组织化学模式的肿瘤数据与Kruskal-Wallis检验和St​​udent t检验进行了比较。结果:根据肝转移建立过程中肿瘤内微血管的形态,血液动力学和免疫组织化学特征的变化,观察到四个逐步变化的模式,如下所示:无明确的肿瘤内血流灌注或任何肿瘤内微血管(平均直径约180微米)的转移。 ,具有门脉灌注和瘤内ICAM-1阳性残留肝窦的转移瘤(平均直径,约290微米),具有门脉和动脉灌注混合的转移瘤以及CD34阳性微血管和α-SMA阳性小动脉增多(平均直径,约520)微米),并且仅通过动脉灌注和增加的CD34阳性微血管和α-SMA阳性小动脉(平均直径,> 2000微米)转移。显示这四种模式的肿瘤平均大小之间的差异具有统计学意义(P <0.01)。结论:在鼠结肠肝转移瘤生长过程中,根据肿瘤逐步新生血管的变化,发现了肿瘤内微循环的逐步改变,从直接扩散,门静脉灌注,门静脉和动脉混合灌注,最后到动脉灌注。

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