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首页> 外文期刊>Molecular and Cellular Endocrinology >Natural variants of the beta isoform of the human glucocorticoid receptor do not alter sensitivity to glucocorticoids.
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Natural variants of the beta isoform of the human glucocorticoid receptor do not alter sensitivity to glucocorticoids.

机译:人糖皮质激素受体的β同工型的天然变体不会改变对糖皮质激素的敏感性。

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The beta isoform of the human glucocorticoid receptor, hGRbeta, is a product of alternative splicing of the hGR gene. The physiological function of this isoform is unknown up to now. Recent data are contradictory in that they either favor or argue against a role of hGRbeta as a repressor of the functional hGRalpha isoform. In the present study hGRbeta did not inhibit transcriptional activation of the MMTV-driven luciferase reporter gene by dexamethasone-activated hGRalpha in COS-1 cells. In addition, two naturally occurring variants of the hGRbeta isoform associated with altered sensitivity to glucocorticoids, termed hGRbeta-R23K and hGRbeta-N363S, did not repress hGRalpha, even when overexpressed 10-fold. We conclude that the hGRbeta isoform, as well as two of its natural variants, do not act as dominant negative inhibitors of hGRalpha function and that the beta isoform does not appear to play a role in the regulation of glucocorticoid sensitivity.
机译:人类糖皮质激素受体的β亚型hGRbeta是hGR基因选择性剪接的产物。到目前为止,这种亚型的生理功能尚不清楚。最近的数据是相互矛盾的,因为它们支持或反对hGRbeta作为功能性hGRalpha同工型的阻遏物的作用。在本研究中,hGRbeta不会抑制地塞米松激活的hGRalpha在COS-1细胞中对MMTV驱动的荧光素酶报道基因的转录激活。另外,与对糖皮质激素的敏感性改变相关的两个自然存在的hGRbeta亚型变体,即使被过度表达10倍,也不能抑制hGRalpha,这被称为hGRbeta-R23K和hGRbeta-N363S。我们得出的结论是,hGRbeta亚型以及其两个自然变异体均不充当hGRalpha功能的主要负性抑制剂,并且β亚型似乎在糖皮质激素敏感性的调节中不起作用。

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