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膀胱移行细胞癌中血管内皮生长因子及血管生成素-1和-2通路的改变与肿瘤进展相关。

Alteration of the vascular endothelial growth factor and angiopoietins-1 and -2 pathways in transitional cell carcinomas of the urinary bladder associated with tumor progression.

作者信息

Quentin Thomas, Schlott Thilo, Korabiowska Monika, Käthei Nadine, Zöller Gerhard, Glaser Frank, Kunze Ekkehard

机构信息

Department of Osteopathology and Hematopathology, Centre of Pathology, Georg-August-University, Göttingen, Germany.

出版信息

Anticancer Res. 2004 Sep-Oct;24(5A):2745-56.

Abstract

Neoangiogenesis is assumed to play an important role in the progression, metastasis and prognosis of a wide variety of tumors. To get insights into the molecular-genetic pathways and the biological role of angiogenesis in urothelial carcinogenesis, we analyzed comparatively the expression of the mRNA of the vascular endothelial growth factor (VEGF) and of the angiopoietins-1 and -2 (Ang-1 and Ang-2) in 71 transitional cell carcinomas (TCC) of the urinary bladder in relation to the tumor grades and stages, and referring to epidemiological risk factors. Using real-time quantitative reverse transcription-polymerase chain reaction, low-stage superficial TCC expressed VEGF and Ang-2 mRNA at a significantly higher level than high-stage muscle invasive carcinomas, and low-grade TCC at an insignificantly higher level than high-grade tumors. The activity of both angiogenic factors was found to be significantly correlated. Conversely, Ang-1 mRNA was expressed at a 3-fold significantly lower level in low-grade, low-stage compared to high-grade, high-stage TCC. A significantly 3- and 2-fold respectively, drop of the VEGF and Ang-2 mRNA expression in conjunction with a 2-fold significantly higher expression of Ang-1 mRNA in the group of grade 2 TCC when infiltrating the muscle layer may represent a crucial event during urothelial carcinogenesis, and possibly indicates an important step in promoting the conversion of bladder cancer from a low to a high malignancy in this subset of carcinomas. By immunhistochemistry, high-grade, high-stage carcinomas less frequently displayed areas with a strong reactivity for the VEGF protein ('hot spots") than low-grade, low-stage TCC, paralleling the expression of the mRNA. The expression patterns observed are compatible with a reduced vascular destabilization and decreased formation of new blood vessels in advanced TCC, suggesting a balance between vessel regression and vascular growth, with a less pronounced vascular remodeling during late phases of urothelial carcinogenesis. Analyzing the effect of life-style bladder cancer risk factors, habitual smoking and coffee consumption was not observed to substantially alter the expression of the angiogenic mediators, except for weakly elevated levels of VEGF and Ang-2 mRNA in TCC of strong smokers and a borderline significantly decreased VEGF mRNA expression associated with heavy coffee consumption. Certain hazardous occupational exposures (polycyclic hydrocarbons, paints and lacquer, stone dust) may play a role in modulating tumor angiogenesis. The current data indicate that the signaling molecular-genetic pathways underlying vascular remodeling are involved in the progression of urinary bladder cancer to a more malignant and aggressive behaviour.

摘要

新血管生成被认为在多种肿瘤的进展、转移和预后中起重要作用。为深入了解血管生成在尿路上皮癌发生中的分子遗传途径和生物学作用,我们比较分析了71例膀胱移行细胞癌(TCC)中血管内皮生长因子(VEGF)、血管生成素-1和-2(Ang-1和Ang-2)的mRNA表达与肿瘤分级和分期的关系,并参考了流行病学危险因素。使用实时定量逆转录聚合酶链反应,低分期浅表性TCC中VEGF和Ang-2 mRNA的表达水平显著高于高分期肌层浸润性癌,低级别TCC中VEGF和Ang-2 mRNA的表达水平略高于高级别肿瘤。发现这两种血管生成因子的活性显著相关。相反,与高级别、高分期TCC相比,低级别、低分期TCC中Ang-1 mRNA的表达水平显著低3倍。在2级TCC浸润肌层时,VEGF和Ang-2 mRNA表达分别显著下降3倍和2倍,同时Ang-! mRNA表达显著升高2倍,这可能是尿路上皮癌发生过程中的关键事件,可能表明在这一亚组癌症中促进膀胱癌从低恶性向高恶性转化的重要步骤。通过免疫组织化学,高级别、高分期癌中VEGF蛋白强反应性区域(“热点”)的出现频率低于低级别、低分期TCC,这与mRNA的表达情况一致。观察到的表达模式与晚期TCC中血管不稳定减少和新血管形成减少相符,提示在尿路上皮癌发生后期血管消退与血管生长之间存在平衡,血管重塑不太明显。分析生活方式膀胱癌危险因素的影响,除了重度吸烟者的TCC中VEGF和Ang-2 mRNA水平略有升高,以及大量饮用咖啡与VEGF mRNA表达显著降低相关外,习惯性吸烟和饮用咖啡未观察到对血管生成介质表达有实质性改变。某些有害职业暴露(多环烃、油漆和清漆、石粉)可能在调节肿瘤血管生成中起作用。目前的数据表明,血管重塑背后的信号分子遗传途径参与了膀胱癌向更恶性和侵袭性更强行为的进展。

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