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首页> 外文期刊>Molecular pharmacology. >Induction of estrogen receptor alpha expression with decoy oligonucleotide targeted to NFATc1 binding sites in osteoblasts.
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Induction of estrogen receptor alpha expression with decoy oligonucleotide targeted to NFATc1 binding sites in osteoblasts.

机译:靶向成骨细胞中NFATc1结合位点的诱饵寡核苷酸诱导雌激素受体α表达。

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摘要

The nuclear factor of activated T cell cytoplasmic 1 (NFATc1) is a member of the NFAT family and is strictly implicated in the growth and development of bone. Most studies have focused on the effects of NFATc1 activation on osteoclastogenesis. On the contrary, the specific roles of NFAT in osteoblast differentiation are not well understood and, in some instances, reports of its role are contradictory. In the present study, we demonstrated that NFATc1 was involved in the transcriptional regulation of human estrogen receptor alpha (ERalpha) gene in SaOS-2 osteoblastic like cells. NFATc1 was specifically recruited "in vivo" at C and F distal promoters of ERalpha gene. In addition, it is here identified as the negative transcription factor removed by the RA4-3'decoy oligonucleotide able to induce ERalpha expression in osteoblasts. Ca(2+)/calcineurin-NFAT-mediated signaling pathways and ERalpha-dependent signals are involved in diverse cellular reactions by regulating gene expression under both physiological and pathological conditions. Therefore, our data might be useful for proper manipulation of NFATc1- and ERalpha-mediated cellular reactions in different bone disorders, such as osteoporosis.
机译:活化的T细胞胞质1(NFATc1)的核因子是NFAT家族的成员,并严格参与骨骼的生长和发育。大多数研究集中于NFATc1激活对破骨细胞形成的影响。相反,人们对NFAT在成骨细胞分化中的具体作用还不甚了解,在某些情况下,有关其作用的报道相互矛盾。在本研究中,我们证明了NFATc1参与了SaOS-2成骨细胞样细胞中人类雌激素受体α(ERalpha)基因的转录调控。 NFATc1是专门在ERalpha基因的C和F远端启动子“体内”募集的。另外,在此被鉴定为由能够在成骨细胞中诱导ERα表达的RA4-3′诱饵寡核苷酸去除的负转录因子。 Ca(2 +)/ calcineurin-NFAT介导的信号通路和ERalpha依赖性信号通过调节生理和病理条件下的基因表达参与多种细胞反应。因此,我们的数据可能有助于在不同的骨病(例如骨质疏松症)中正确操纵NFATc1和ERalpha介导的细胞反应。

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