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首页> 外文期刊>Microvascular Research: An International Journal >Tumor-line specific causes of intertumor heterogeneity in blood supply in human melanoma xenografts
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Tumor-line specific causes of intertumor heterogeneity in blood supply in human melanoma xenografts

机译:人类黑素瘤异种移植物供血中肿瘤间异质性的肿瘤线特异性原因

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The efficacy of most cancer treatments is strongly influenced by the tumor blood supply. The results of experimental studies using xenografted tumors to evaluate novel cancer treatments may therefore vary considerably depending on the blood supply of the specific tumor model being used. Mechanisms underlying intertumor heterogeneity in the blood supply of xenografted tumors derived from same tumor line are poorly understood, and were investigated here by using intravital microscopy to assess tumor blood supply and vascular morphology in human melanomas growing in dorsal window chambers in BALB/c nu/. nu mice. Two melanoma lines, A-07 and R-18, were included in the study. These lines differed substantially in angiogenic profiles. Thus, when the expression of 84 angiogenesis-related genes was investigated with a quantitative PCR array, 25% of these genes showed more than a 10-fold difference in expression. Furthermore, A-07 tumors showed higher vascular density, higher vessel tortuosity, higher vessel diameters, shorter vessel segments, and more chaotic vascular architecture than R-18 tumors. Both lines showed large intertumor heterogeneity in blood supply. In the A-07 line, tumors with low microvascular density, long vessel segment, and high vessel tortuosity showed poor blood supply, whereas in the R-18 line, poor tumor blood supply was associated with low tumor arteriolar diameters. Thus, tumor-line specific causes of intertumor heterogeneity in blood supply were identified in human melanoma xenografts, and these tumor-line specific mechanisms were possibly a result of tumor-line specific angiogenic profiles.
机译:大多数癌症治疗的功效在很大程度上受到肿瘤血液供应的影响。因此,使用异种移植肿瘤评估新型癌症治疗方法的实验研究结果可能会有所不同,具体取决于所用特定肿瘤模型的血液供应。源自同一肿瘤系的异种移植肿瘤的血液供应中潜在的肿瘤间异质性机制了解甚少,并且在这里通过活体显微镜研究了BALB / c nu / 。 nu小鼠。该研究包括两条黑色素瘤细胞系A-07和R-18。这些系在血管生成方面有很大的不同。因此,当用定量PCR阵列研究84个血管生成相关基因的表达时,这些基因中有25%的表达差异超过10倍。此外,与R-18肿瘤相比,A-07肿瘤显示出更高的血管密度,更高的血管曲折度,更高的血管直径,更短的血管节段和更混乱的血管结构。两条线均显示出较大的肿瘤间供血异质性。在A-07品系中,微血管密度低,血管段长且血管曲折性高的肿瘤显示出血液供应不足,而在R-18品系中,肿瘤的血液供应不足与肿瘤小动脉直径低有关。因此,在人类黑素瘤异种移植物中确定了血液供应中肿瘤间异质性的肿瘤细胞系特异性原因,并且这些肿瘤细胞系特异性机制可能是肿瘤细胞系特异性血管生成特征的结果。

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