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HOXA cluster gene expression during osteoblast differentiation involves epigenetic control

机译:Osteoblast分化期间的Hoxa Cluster基因表达涉及表观遗传控制

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摘要

The HOXA gene cluster is generally recognized as a pivotal mediator of positional identity in the skeletal system, expression of different orthologues conferring alternative locational phenotype of the vertebrate bone. Strikingly, however, the molecular mechanisms that regulate orthologue-specific expression of different HOXA cluster members in gestating osteoblasts remain largely obscure, but in analogy to the processes observed in acute lymphatic leukemia it is assumed that alternative methylation of HOXA promoter regions drives position specific expression patterns. In an effort to understand HOXA cluster gene expression in osteogenesis we characterize both expression and the epigenetic landscape of the HOXA gene cluster during in vitro osteoblast formation from mesenchymal precursors. We observe that osteoblast formation per se provokes strong upregulation of HOXA gene cluster expression, in particular of midcluster genes, and paradoxal downregulation of HOXA7 and HOXA10. These differences in expression appear related to promoter methylation. LnRNAs HOTAIR and HOTTIP, known to modulate HOXA expression, are also regulated by their promoter methylation processing, but do not correlate with HOXA cluster expression profile. We thus conclude that HOXA expression is profoundly regulated during osteoblast differentiation through canonical methylation-dependent mechanisms but not through the flanking lnRNAs.
机译:Hoxa基因簇通常被认为是骨骼系统中位置同一性的枢轴介质,不同的脊椎动物骨的替代位置表型的不同矫形表达。然而,引人注目地,调节在妊娠成骨细胞中的不同HOXA簇构件的正常表达的分子机制仍然很大程度上是模糊的,但类似于在急性淋巴性白血病中观察到的过程,假设Hoxa启动子区的替代甲基化驱动位置特异性表达模式。努力理解在骨发生中的霍尔达群体基因表达中,我们表征了在间充质前体的体外成骨细胞形成期间霍可纳基因簇的表达和表观遗传景观。我们观察到,骨质细胞形成本身激发了霍尔达基因簇表达的强烈上调,特别是中间簇基因,以及Hoxa7和Hoxa10的矛盾下调。表达的这些差异与启动子甲基化有关。 LNRNA Hotair和Hottip,已知调节Hoxa表达,也通过其启动子甲基化处理来调节,但与Hoxa簇表达谱系不相关。因此,我们得出结论,通过典型甲基化依赖性机制,在成骨细胞分化过程中,霍可亚表达在骨血细胞分化过程中进行了深刻的调节,而不是通过侧翼的LNRNA。

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