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首页> 外文期刊>Oncology reports >Expression analysis of VEGF-A and VEGF-B: relationship with clinicopathological parameters in bladder cancer.
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Expression analysis of VEGF-A and VEGF-B: relationship with clinicopathological parameters in bladder cancer.

机译:VEGF-A和VEGF-B的表达分析:与膀胱癌临床病理参数的关系。

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The present investigation was conducted first to determine whether correlation exists between VEGF-A and -B mRNA levels and clinicopathological parameters and to assess their prognostic value in bladder cancer, then to clarify the expression level and biological significance of VEGF-A isoforms. Total RNA was isolated from 37 specimens of bladder cancer. Northern blot analysis revealed that VEGF-B mRNA was not expressed either in normal urothelium or in bladder cancer and detected three VEGF-A transcripts of 5.2, 4.5 and 1.7 kb in length, respectively. The VEGF-A transcript levels were greater in cancer tissues than in normal urothelium. They were significantly higher in pT2-T4 than in pTa and pT1 urothelial tumors and thus, were correlated to the pathologic stage. Contrary to the 4.5 kb transcript, elevated expression of the 5.2 and 1.7 kb transcripts was correlated with the histologic grade and the presence of carcinoma in situ. Patients with higher VEGF-A mRNA levels had a significantly shorter survival without progression compared to those with lower levels. Three VEGF-A splice variants were detected by southern blotting namely, VEGF121, 165 and 189. The expression intensity of each isoform was evaluated by quantitative real-time RT-PCR in 20 new fresh frozen recent tumors. VEGF121 and VEGF165 were expressed at the similar level. On the contrary, they were significantly more expressed than VEGF189 (p<0.05). The three isoforms were higher expressed in pT2 bladder cancers than in pTa tumors (p<0.05). There was only a significant correlation between the increased expression level of VEGF121 and 165 and the histological grade of the lesion (p<0.05). To conclude, VEGF-A mRNA level is a potential prognostic indicator of progression in bladder cancer as well as the expression level of the different VEGF-A splice variants.
机译:本研究首先确定VEGF-A和-B mRNA水平与临床病理参数之间是否存在相关性,并评估其在膀胱癌中的预后价值,然后阐明VEGF-A同工型的表达水平和生物学意义。从37个膀胱癌标本中分离出总RNA。 Northern印迹分析显示,VEGF-B mRNA在正常尿路上皮或膀胱癌中均未表达,并且检测到三个分别为5.2、4.5和1.7 kb的VEGF-A转录物。癌组织中的VEGF-A转录水平高于正常尿路上皮。它们在pT2-T4中明显高于pTa和pT1尿路上皮肿瘤,因此与病理分期相关。与4.5 kb的转录本相反,5.2和1.7 kb的转录本的升高表达与组织学分级和原位癌相关。 VEGF-A mRNA水平较高的患者与较低水平的患者相比,无进展的生存期明显缩短。通过Southern印迹检测到三种VEGF-A剪接变体,即VEGF121、165和189。通过定量实时RT-PCR评估每种同工型在20种新近冷冻的新近肿瘤中的表达强度。 VEGF121和VEGF165以相似的水平表达。相反,它们的表达明显高于VEGF189(p <0.05)。在pT2膀胱癌中,这三种同工型的表达高于pTa肿瘤(p <0.05)。 VEGF121和165的表达水平升高与病变的组织学分级之间仅存在显着相关性(p <0.05)。总之,VEGF-A mRNA水平是膀胱癌进展以及不同VEGF-A剪接变体表达水平的潜在预后指标。

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