[Correlation between the expression of VEGF-C mRNA, VEGFR-3, CD31 and tumor metastases in Chinese with prostate cancer].

Shi yan sheng wu xue bao Pub Date : 2005-06-01
Guo Fang Ding, Ji Cheng Li, Yin Feng Xu, Yu Sun, Li Tao
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Abstract

The expressions of VEGF-C mRNA, VEGFR-3 and CD31 were studied in order to investigate the correlation between them and neoangiogenesis, hyperplasia of micro-lymphatics and tumor metastases. 34 cases of prostate cancer tissue and 12 cases of adjacent nontumorous tissue specimens were tested. They were marked by VEGFR-3 and CD31 with immunohistochemistic staining and analyzed with image, the micro-lymphatics count (MLC) and microvessel density (MVD) were counted using Weidner's highest vessel density count method; the expression of VEGF-C mRNA was inspected in situ hybridization. The expression of VEGF-C mRNA was 44.12% positive in 34 cases of prostate cancer, the MLC (8.26 +/- 2.73)mm2 and MVD (74.82 +/- 11.76)mm2 in prostate cancer were significantly higher than those in adjacent nontumorous tissue (MLC, 4.82 +/- 3.48/mm2; MVD, 32.86 +/- 5.41/mm2). In addition, there was a correlation between the expression of VEGF-C mRNA and micro-lymphatics metastases and there was a positive correlation between the expression of VEGFR-3 and CD31. The expressions of VEGF-C mRNA , MLC, MVD in stage III and IV and those who have lymph metastasis were higher than those in stage I and II and those who have no lymph metastasis; the expressions of VEGFR-3 and CD31 in VEGF-C mRNA positive groups were significantly higher than those in negative groups. The difference of histopathologic grading in prostate cancer had no statistical significance. VEGF-C could accelerate the hyperplasia of micro-lymphatics and neoangiogenesis induced by tumor and play an important role in tumor lymph metastases. There was a close correlation between the expressions of VEGFR-3, CD31 and tumor metastases. The increase of MLC and MVD on prostate cancer indicated the hyperplasia of new micro-lymphatics and neoangiogenesis in the tumor tissue, which could also be a signal to determine the tumor metastases in clinic.

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[中国前列腺癌患者VEGF-C mRNA、VEGFR-3、CD31表达与肿瘤转移的关系]。
研究VEGF-C mRNA、VEGFR-3和CD31的表达与新生血管生成、微淋巴管增生和肿瘤转移的关系。34例前列腺癌组织及12例癌旁非肿瘤组织标本。采用免疫组织化学方法对其进行VEGFR-3和CD31标记,并进行图像分析,采用Weidner最高血管密度计数法计算微淋巴管计数(MLC)和微血管密度(MVD);原位杂交法检测VEGF-C mRNA的表达。34例前列腺癌组织中VEGF-C mRNA的阳性表达率为44.12%,前列腺癌组织的MLC (8.26 +/- 2.73)mm2和MVD (74.82 +/- 11.76)mm2显著高于癌旁非肿瘤组织(MLC, 4.82 +/- 3.48/mm2;MVD为32.86±5.41/mm2)。此外,VEGF-C mRNA的表达与微淋巴转移呈相关,VEGFR-3的表达与CD31呈正相关。VEGF-C mRNA、MLC、MVD在ⅲ期、ⅳ期及有淋巴结转移组的表达高于ⅰ期、ⅱ期及无淋巴结转移组;VEGF-C mRNA阳性组中VEGFR-3、CD31的表达明显高于阴性组。前列腺癌组织病理学分级差异无统计学意义。VEGF-C能加速肿瘤诱导的微淋巴管增生和新生血管生成,在肿瘤淋巴转移中起重要作用。VEGFR-3、CD31的表达与肿瘤转移密切相关。前列腺癌的MLC和MVD升高,提示肿瘤组织中新生微淋巴管增生和新生血管生成,也可作为临床判断肿瘤转移的信号。
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