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从人肾皮质和肾细胞癌的原代细胞培养中证实了 Annexin A3 的两种剪接异构体的差异表达。

Primary cell cultures from human renal cortex and renal-cell carcinoma evidence a differential expression of two spliced isoforms of Annexin A3.

机构信息

Department of Experimental Medicine, University of Milano-Bicocca, 20052 Monza, Italy.

出版信息

Am J Pathol. 2010 Apr;176(4):1660-70. doi: 10.2353/ajpath.2010.090402. Epub 2010 Feb 18.

Abstract

Primary cell cultures from renal cell carcinoma (RCC) and normal renal cortex tissue of 60 patients have been established, with high efficiency (more than 70%) and reproducibility, and extensively characterized. These cultures composed of more than 90% of normal or tumor tubular cells have been instrumental for molecular characterization of Annexin A3 (AnxA3), never extensively studied before in RCC cells although AnxA3 has a prognostic relevance in some cancer and it has been suggested to be involved in the hypoxia-inducible factor-1 pathway. Western blot analysis of 20 matched cortex/RCC culture lysates showed two AnxA3 protein bands of 36 and 33 kDa, and two-dimensional Western blot evidenced several specific protein spots. In RCC cultures the 36-kDa isoform was significantly down-regulated and the 33-kDa isoform up-regulated. Furthermore, the inversion of the quantitative expression pattern of two AnxA3 isoforms in tumor cultures correlate with hypoxia-inducible factor-1alpha expression. The total AnxA3 protein is down-regulated in RCC cultures as confirmed also in tissues by tissue microarray. Two AnxA3 transcripts that differ for alternative splicing of exon III have been also detected. Real-time PCR quantification in 19 matched cortex/RCC cultures confirms the down-regulation of longer isoform in RCC cells. The characteristic expression pattern of AnxA3 in normal and tumor renal cells, documented in our primary cultures, may open new insight in RCC management.

摘要

已成功建立了 60 例肾细胞癌(RCC)和正常肾皮质组织的原代细胞培养,效率高(超过 70%)且可重复性好,并进行了广泛的特征描述。这些培养物由超过 90%的正常或肿瘤管状细胞组成,对于 Annexin A3(AnxA3)的分子特征分析非常重要,因为之前在 RCC 细胞中从未广泛研究过 AnxA3,尽管 AnxA3 在一些癌症中具有预后相关性,并被认为参与了缺氧诱导因子-1 通路。对 20 对匹配的皮质/RCC 培养物裂解物进行的 Western blot 分析显示,AnxA3 蛋白有两种 36 和 33 kDa 的蛋白条带,二维 Western blot 显示出多个特异性蛋白斑点。在 RCC 培养物中,36 kDa 同工型显著下调,33 kDa 同工型上调。此外,肿瘤培养物中两种 AnxA3 同工型定量表达模式的反转与缺氧诱导因子-1alpha 表达相关。正如组织微阵列分析所证实的,RCC 培养物中的总 AnxA3 蛋白也下调。还检测到通过外显子 III 选择性剪接而不同的两种 AnxA3 转录本。在 19 对匹配的皮质/RCC 培养物中的实时 PCR 定量证实了 RCC 细胞中较长同工型的下调。在我们的原代培养物中,正常和肿瘤肾细胞中 AnxA3 的特征表达模式可能为 RCC 管理提供新的见解。

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