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Hoxc8 下调 Mgl1 肿瘤抑制基因的表达,并降低其对细胞黏附的伴随功能。

Hoxc8 downregulates Mgl1 tumor suppressor gene expression and reduces its concomitant function on cell adhesion.

机构信息

Department of Anatomy, Embryology Laboratory, Brain Korea 21 Project for Medical Science, Yonsei University College of Medicine, Seoul 120-752, Korea.

出版信息

Mol Cells. 2011 Sep;32(3):273-9. doi: 10.1007/s10059-011-0069-8. Epub 2011 Jul 15.

Abstract

Hoxc8 is a homeobox gene family member, which is essential for growth and differentiation. Mgl1, a mouse homologue of the Drosophila tumor suppressor gene lgl, was previously identified as a possible target of Hoxc8. However, the biological effects and underlying molecular mechanism of Hoxc8 regulation on Mgl1 has not been fully established. The endogenous expression patterns of Hoxc8 were inversely correlated with those of Mgl1 in different types of cells and tissues. Here we showed that Hoxc8 overexpression downregulated the Mgl1 mRNA expression. Characterization of the ~2 kb Mgl1 promoter region revealed that the upstream sequence contains several putative Hox core binding sites and chromatin immunoprecipitation assay confirmed that Hoxc8 directly binds to the 5' upstream region of Mgl1. The promoter activity of this region was diminished by Hoxc8 expression but resumed by knockdown of Hoxc8 using siRNA against Hoxc8. Functional study of Mgl1 in C3H10T1/2 cells revealed a significant reduction in cell adhesion upon expression of Hoxc8. Taken together, our data suggest that Hoxc8 downregulates Mgl1 expression via direct binding to the promoter region, which in turn reduces cell adhesion and concomitant cell migration.

摘要

Hoxc8 是同源盒基因家族的一员,对于生长和分化至关重要。Mgl1 是果蝇肿瘤抑制基因 lgl 的小鼠同源物,先前被鉴定为 Hoxc8 的可能靶标。然而,Hoxc8 对 Mgl1 的调控的生物学效应和潜在分子机制尚未完全建立。在不同类型的细胞和组织中,Hoxc8 的内源性表达模式与 Mgl1 的表达模式呈负相关。在这里,我们表明 Hoxc8 的过表达下调了 Mgl1 mRNA 的表达。对~2kb 的 Mgl1 启动子区域的特征分析表明,上游序列包含几个推定的 Hox 核心结合位点,染色质免疫沉淀测定证实 Hoxc8 直接结合到 Mgl1 的 5'上游区域。该区域的启动子活性被 Hoxc8 的表达减弱,但通过针对 Hoxc8 的 siRNA 敲低 Hoxc8 后恢复。在 C3H10T1/2 细胞中对 Mgl1 的功能研究表明,表达 Hoxc8 后细胞黏附显著减少。总之,我们的数据表明,Hoxc8 通过直接结合启动子区域下调 Mgl1 的表达,从而降低细胞黏附和伴随的细胞迁移。

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