Cressey Ratchada, Wattananupong Onusa, Lertprasertsuke Nirush, Vinitketkumnuen Usanee
Department of Associated Medical Science, Chiang Mai University, Chiang Mai, Thailand.
BMC Cancer. 2005 Oct 4;5:128. doi: 10.1186/1471-2407-5-128.
Vascular endothelial growth factor (VEGF) is a potent mitogen for endothelial cells, and its expression has been correlated with increased tumour angiogenesis. Although numerous publications dealing with the measurement of circulating VEGF for diagnostic and therapeutic monitoring have been published, the relationship between the production of tissue VEGF and its concentration in blood is still unclear. The aims of this study were to determine: 1) The expression pattern of VEGF isoforms at the protein level in colorectal and lung adenocarcinoma in comparison to the pattern in corresponding adjacent normal tissues 2) The relationship between the expression pattern of VEGF and total level of circulating VEGF in the blood to clarify whether the results of measuring circulating VEGF can be used to predict VEGF expression in tumour tissues.
Ninety-four tissue samples were obtained from patients, 76 colorectal tumour tissues and 18 lung tumour tissues. VEGF protein expression pattern and total circulating VEGF were examined using western blot and capture ELISA, respectively.
Three major protein bands were predominately detected in tumour samples with an apparent molecular mass under reducing conditions of 18, 23 and 26 kDa. The 18 kDa VEGF protein was expressed equally in both normal and colorectal tumour tissues and predominately expressed in normal tissues of lung, whereas the 23 and 26 kDa protein was only detected at higher levels in tumour tissues. The 18, 23 and 26 kDa proteins are believed to represent the VEGF121, the VEGF165 and the VEGF189, respectively. There was a significant correlation of the expression of VEGF165 with a smaller tumour size maximum diameter < 5 cm (p < 0.05), and there was a significant correlation of VEGF189 with advanced clinical stage of colorectal tumours. The measurement of total circulating VEGF in serum revealed that cancer patients significantly (p < 0.001) possessed a higher level of circulating VEGF (1081 +/- 652 pg/ml in colorectal and 1,251 +/- 568 pg/ml in lung) than a healthy volunteer group (543 +/- 344 pg/ml). No correlation between the level of circulating VEGF and the pathologic features of tumours was observed.
Our findings indicate that the expression patterns of VEGF isoforms are altered during tumourigenesis as certain isoform overexpression in tumour tissues correlated with tumour progression indicating their important role in tumour development. However, measurement of VEGF in the circulation as a prognostic marker needs to be carefully evaluated as the cell-associated isoform (VEGF189), but not the soluble isoform (VEGF121 and VEGF165) appears to play important role in tumour progression.
血管内皮生长因子(VEGF)是一种强效的内皮细胞促有丝分裂原,其表达与肿瘤血管生成增加相关。尽管已经发表了许多关于测量循环VEGF用于诊断和治疗监测的文章,但组织VEGF的产生与其血液浓度之间的关系仍不清楚。本研究的目的是确定:1)与相应相邻正常组织中的模式相比,结直肠癌和肺腺癌中VEGF异构体在蛋白质水平的表达模式;2)VEGF的表达模式与血液中循环VEGF总水平之间的关系,以阐明测量循环VEGF的结果是否可用于预测肿瘤组织中的VEGF表达。
从患者处获得94个组织样本,76个结直肠肿瘤组织和18个肺肿瘤组织。分别使用蛋白质印迹法和捕获ELISA检测VEGF蛋白表达模式和循环VEGF总量。
在肿瘤样本中主要检测到三条主要蛋白带,在还原条件下的表观分子量为18、23和26 kDa。18 kDa的VEGF蛋白在正常和结直肠肿瘤组织中表达相同,在肺正常组织中主要表达,而23和26 kDa蛋白仅在肿瘤组织中高水平检测到。据信18、23和26 kDa蛋白分别代表VEGF121、VEGF165和VEGF189。VEGF165的表达与较小的肿瘤大小(最大直径<5 cm)有显著相关性(p<0.05),VEGF189与结直肠肿瘤的晚期临床分期有显著相关性。血清中循环VEGF总量的测量显示,癌症患者(结直肠癌患者为1081±652 pg/ml,肺癌患者为1251±568 pg/ml)的循环VEGF水平显著高于健康志愿者组(543±344 pg/ml)(p<0.001)。未观察到循环VEGF水平与肿瘤病理特征之间的相关性。
我们的研究结果表明,VEGF异构体的表达模式在肿瘤发生过程中发生改变,因为肿瘤组织中某些异构体的过表达与肿瘤进展相关,表明它们在肿瘤发展中起重要作用。然而,作为预后标志物测量循环中的VEGF需要仔细评估,因为细胞相关异构体(VEGF189)而非可溶性异构体(VEGF121和VEGF165)似乎在肿瘤进展中起重要作用。
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