首页> 外文期刊>Anticancer Research: International Journal of Cancer Research and Treatment >Expression of Aurora-B kinase and phosphorylated histone H3 in hepatocellular carcinoma.
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Expression of Aurora-B kinase and phosphorylated histone H3 in hepatocellular carcinoma.

机译:Aurora-B激酶和磷酸化组蛋白H3在肝细胞癌中的表达。

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BACKGROUND: Aurora-B, a chromosomal passenger protein forming a complex with INCENP (inner centromere protein) and survivin, regulates stable bipolar spindle-kinetochore attachment in mitosis and chromosome segregation and cytokinesis. It was recently documented that Aurora-B directly phosphorylated histone H3, not only at Ser10, but also at Ser28, which contributed to chromosome number instability and mitotic chromosome condensation. This study aimed at investigating the expression of Aurora-B kinase (Aurora-B) and phosphorylated histone H3 (H3-P) and their roles in hepatocellular carcinogenesis. MATERIALS AND METHODS: The expressions of Aurora-B and H3-P were examined in hepatocellular carcinoma (HCC) by immunohistochemistry. A hepatoblastoma cell line, HepG2, was targeted and the isolation and characterization of alternative variants of Aurora-B were carried out. The Aurora encoding protein was detected in COS-7 transfected with different Aurora transcripts by Western blot. Finally, the expression of Aurora-B and its variant forms was examined in 17 HCCs by RT-PCR. RESULTS: Immunohistochemically, Aurora-B was observed only in a few cases of HCC, while H3-P expression was more frequently detected in carcinoma foci than in non-carcinoma foci (p < 0.05). The isolation and characterization of two alternative variant forms of Aurora-B (termed Aurora-B1 and -B2) in the HepG2 cell line were successful. Aurora-B-transfected COS-7 cells expressed two different proteins, one of which was similar to the expression product of Aurora-B1 in size. Aurora-B transcripts were detected in 12 out of 17 (70.5%) HCC cases examined. Aurora-B2 was predominantly detected in 9 (52.9%) cases, while regular Aurora-B and Aurora-B1 were detected in 6 (35.2%) and 7 (41.1%) cases, respectively. CONCLUSION: Aberrant expression of Aurora-B and H3-P plays a role in hepatocarcinogenesis. Alterative splicing of Aurora-B produces different sizes of proteins in HCC. Temporally altered phosphorylation of histone-H3 in the entire cell cycle may up-regulate the entry of HCC into the cell cycle to enhance their proliferation.
机译:背景:Aurora-B是一种与INCENP(内部着丝粒蛋白)和survivin形成复合物的染色体客体蛋白,它在有丝分裂,染色体分离和胞质分裂中调节稳定的双极纺锤体-线粒体附着。最近有文献报道,Aurora-B不仅在Ser10处而且在Ser28处都直接磷酸化了组蛋白H3,这导致了染色体数目的不稳定性和有丝分裂染色体的缩合。这项研究旨在调查Aurora-B激酶(Aurora-B)和磷酸化组蛋白H3(H3-P)的表达及其在肝细胞癌变中的作用。材料与方法:采用免疫组织化学方法检测肝细胞癌中Aurora-B和H3-P的表达。靶向肝母细胞瘤细胞系HepG2,并对Aurora-B的其他变体进行了分离和表征。通过Western印迹在用不同Aurora转录物转染的COS-7中检测到Aurora编码蛋白。最后,通过RT-PCR检查了17个肝癌中Aurora-B及其变体形式的表达。结果:在免疫组织化学中,仅在少数HCC病例中观察到Aurora-B,而在癌灶中比在非癌灶中更频繁地检测到H3-P表达(p <0.05)。在HepG2细胞系中成功分离并鉴定了两种可选的Aurora-B变体形式(称为Aurora-B1和-B2)。 Aurora-B转染的COS-7细胞表达两种不同的蛋白质,其中一种与Aurora-B1的表达产物相似。在所检查的17例HCC病例中,有12例(70.5%)检测到Aurora-B转录本。在9例(52.9%)病例中主要检测到Aurora-B2,而在6例(35.2%)和7例(41.1%)病例中检测到常规Aurora-B和Aurora-B1。结论:Aurora-B和H3-P的异常表达在肝癌发生中起一定作用。 Aurora-B的可变剪接在HCC中产生不同大小的蛋白质。在整个细胞周期中,组蛋白-H3的磷酸化暂时改变可能会上调HCC进入细胞周期,从而增强其增殖。

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