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缺氧诱导蛋白2在肾细胞癌中的表达:分子靶向治疗的一个有前景的候选靶点

Expression of hypoxia-inducible protein 2 in renal cell carcinoma: A promising candidate for molecular targeting therapy.

作者信息

Seo Takashi, Konda Ryuichiro, Sugimura Jun, Iwasaki Kazuhiro, Nakamura Yusuke, Fujioka Tomoaki

机构信息

Department of Urology, Iwate Medical University School of Medicine, Morioka.

出版信息

Oncol Lett. 2010 Jul;1(4):697-701. doi: 10.3892/ol_00000122. Epub 2010 Jul 1.

Abstract

This study investigated the expression of hypoxia-inducible protein 2 (HIG2), a novel renal cell carcinoma (RCC)-associated molecule and an essential growth factor for RCC, in kidneys to elucidate its clinical significance in RCC. An immunohistochemical study of HIG2 was conducted in 93 surgical samples of RCC tissues and 10 samples of normal kidney tissues obtained after nephrectomies for localized RCC. HIG2 expression was also correlated with clinicopathological characteristics and survival. Only faint or weak immunostaining for HIG2 was observed in normal kidney samples. HIG2 expression was found in 86% of RCC tissues (80/93). When analyzed by histological type, positive staining for HIG2 was detected in all papillary (7/7), chromophobe (1/1) and cyst-associated (3/3) RCC. In contrast, the HIG2 expression was observed in 85% of clear cell (68/80) and 50% of spindle cell (1/2) RCC. Labeling indices were 74.1, 45.4, 39, 24.8 and 12.1% in papillary, spindle, clear cell, cyst-associated and chromophobe RCC, respectively. A significant increase in HIG2 expression was noted in RCC tissues obtained from patients with high stage RCC, lymph node metastasis and high nuclear grade (p<0.001, p<0.02 and p<0.006, respectively). RCC patients with a negative HIG2 staining had prolonged 5-year cancer-specific survival. In conclusion, HIG2 expression was extensively observed in RCC tissues and was higher in advanced RCC, suggesting that HIG2 is a candidate for the development of molecular targeting therapy.

摘要

本研究调查了缺氧诱导蛋白2(HIG2)在肾脏中的表达情况,HIG2是一种新型的与肾细胞癌(RCC)相关的分子,也是RCC的一种重要生长因子,以阐明其在RCC中的临床意义。对93例RCC组织手术样本和10例因局限性RCC行肾切除术后获得的正常肾组织样本进行了HIG2的免疫组织化学研究。HIG2表达还与临床病理特征及生存率相关。在正常肾样本中仅观察到微弱的HIG2免疫染色。在86%的RCC组织(80/93)中发现了HIG2表达。按组织学类型分析时,在所有乳头状(7/7)、嫌色细胞(1/1)和囊肿相关性(3/3)RCC中均检测到HIG2阳性染色。相比之下,在85%的透明细胞(68/80)和50%的梭形细胞(1/2)RCC中观察到HIG2表达。乳头状、梭形、透明细胞、囊肿相关性和嫌色细胞RCC的标记指数分别为74.1%、45.4%、39%、24.8%和12.1%。在高分期RCC、有淋巴结转移和高核分级的患者的RCC组织中,HIG2表达显著增加(分别为p<0.001、p<0.02和p<0.006)。HIG2染色阴性的RCC患者5年癌症特异性生存率延长。总之,HIG2表达在RCC组织中广泛存在,且在晚期RCC中更高,提示HIG2是分子靶向治疗开发的一个候选靶点。

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