首页> 外文期刊>Annals of the New York Academy of Sciences >Differential Effects Of The New Glucocorticoidreceptor Antagonist Org 34517 And Ru486 (mifepristone) On Glucocorticoid Receptor nuclear Translocation In The Att20 Cell Line
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Differential Effects Of The New Glucocorticoidreceptor Antagonist Org 34517 And Ru486 (mifepristone) On Glucocorticoid Receptor nuclear Translocation In The Att20 Cell Line

机译:新型糖皮质激素受体拮抗剂Org 34517和Ru486(米非司酮)对Att20细胞系中糖皮质激素受体核转运的差异作用

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Glucocorticoid agonists bind to cytoplasmic glucocorticoid receptors (GRs) and subsequently translocate as an agonist-GR complex into the nucleus. In the nucleus the complex regulates the transcription of target genes. A number of GR antagonists (RU486, progesterone, RU40555) have also been shown to induce receptor translocation. These compounds should be regarded as partial agonists. For the nonselective progesterone receptor antagonists, RTI3021-012 and RTI3021-022, it was shown that GR antagonism is possible without the induction of GR translocation. In the present studies, the new GR antagonist, ORG 34517, was investigated for its potential to induce GR translocation and to antagonize corticosterone-induced GR translocation in the AtT20 (mouse pituitary) cell line. ORG 34517 was compared to RU486. In contrast to RU486, ORG 34517 (at doses up to 3 × 10~(-7) M) did not induce GR translocation, but was able to block corticosterone (3 × 10~(-8) M) induced GR translocation. ORG 34517 can be regarded as a true competitive GR antagonist without partial agonistic activities.
机译:糖皮质激素激动剂与细胞质糖皮质激素受体(GRs)结合,随后以激动剂GR复合物的形式转运到细胞核中。在细胞核中,复合物调节靶基因的转录。还已经显示出许多GR拮抗剂(RU486,孕酮,RU40555)诱导受体易位。这些化合物应被视为部分激动剂。对于非选择性孕激素受体拮抗剂RTI3021-012和RTI3021-022,显示出在没有诱导GR易位的情况下GR拮抗作用是可能的。在本研究中,研究了新的GR拮抗剂ORG 34517在AtT20(小鼠垂体)细胞系中诱导GR易位和拮抗皮质酮诱导的GR易位的潜力。将ORG 34517与RU486进行了比较。与RU486相反,ORG 34517(最高剂量为3×10〜(-7)M)不会诱导GR易位,但能够阻断皮质酮(3×10〜(-8)M)引起的GR易位。 ORG 34517被认为是真正的竞争性GR拮抗剂,没有部分激动作用。

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