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鉴定前列腺癌细胞系中 ETS-1 剪接变体 p42 和 p27。

Novel identification of the ETS-1 splice variants p42 and p27 in prostate cancer cell lines.

机构信息

Institute of Pathology, University Hospital Bonn, D-53127 Bonn, Germany.

出版信息

Oncol Rep. 2012 May;27(5):1321-4. doi: 10.3892/or.2012.1667. Epub 2012 Feb 1.

Abstract

ETS-1 is involved in cellular functions such as proliferation, migration, invasion, apoptosis and angiogenesis. The ETS-1 gene encodes three distinct proteins, ETS-1 p51 encoded by a full-length mRNA, ETS-1 p42 and ETS-1 p27 encoded by an alternatively spliced mRNA lacking exon VII and exons III-VI, respectively. ETS-1 p51, commonly considered to be the active form, has been studied in prostate cancer (PCa). However, the ETS-1 p42 and p27 variants have not yet been identified in PCa. Therefore, we aimed in this study at investigating whether the splice variants p42 and p27 are expressed in the androgen-dependent VCaP and LNCaP and the androgen-independent PC3 and DU-145 PCa cell lines. Using RT-PCR, we found the expression of both splice variants p42 and p27 at the mRNA level in the VCaP, LNCaP, PC3 and DU-145 PCa cell lines. We then confirmed the expression of ETS-1 p51 and its splice variants p42 and p27 at the protein level using an anti-ETS-1 antibody directed against the DNA-binding domain (DBD) in lysates prepared from the latter-mentioned cell lines, as well as in PC3 cell nuclear extract. Moreover, differences in the expression ratios of the ETS-1 splice variants within each cell line were also found. In conclusion, we have demonstrated for the first time the novel identification of the ETS-1 splice variants p42 and p27 in PCa cell lines. It is very likely that the role of ETS-1 p51 in PCa is significantly influenced by the presence of its splice variants ETS-1 p42 and p27 as competition, abundance, affinity, interactions and cross-talk among them will eventually determine the genes that will be targeted and subsequently affect cellular functions. Follow-up studies will need to address in functional terms, the roles of these splice variants in PCa cell lines, as well as their expression in PCa tissues and its correlation with clinical outcome.

摘要

ETS-1 参与细胞功能,如增殖、迁移、侵袭、凋亡和血管生成。ETS-1 基因编码三个不同的蛋白质,全长 mRNA 编码的 ETS-1 p51、缺失外显子 VII 和外显子 III-VI 的选择性剪接 mRNA 编码的 ETS-1 p42 和 ETS-1 p27。通常被认为是活性形式的 ETS-1 p51 已在前列腺癌 (PCa) 中进行了研究。然而,PCa 中尚未鉴定出 ETS-1 p42 和 p27 变体。因此,我们在这项研究中旨在研究剪接变体 p42 和 p27 是否在雄激素依赖性 VCaP 和 LNCaP 以及雄激素非依赖性 PC3 和 DU-145 PCa 细胞系中表达。使用 RT-PCR,我们在 VCaP、LNCaP、PC3 和 DU-145 PCa 细胞系中在 mRNA 水平上发现了两种剪接变体 p42 和 p27 的表达。然后,我们使用针对 DNA 结合结构域 (DBD) 的抗 ETS-1 抗体在上述细胞系的裂解物中以及在 PC3 细胞核提取物中证实了 ETS-1 p51 及其剪接变体 p42 和 p27 的表达。此外,还发现了每个细胞系中 ETS-1 剪接变体的表达比率差异。总之,我们首次在 PCa 细胞系中鉴定出 ETS-1 剪接变体 p42 和 p27。很可能 ETS-1 p51 在 PCa 中的作用会受到其剪接变体 ETS-1 p42 和 p27 的存在显著影响,因为它们之间的竞争、丰度、亲和力、相互作用和串扰最终将决定将靶向哪些基因,并随后影响细胞功能。后续研究需要从功能上解决这些剪接变体在 PCa 细胞系中的作用,以及它们在 PCa 组织中的表达及其与临床结果的相关性。

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