贝特类药物和他汀类药物协同增加PPARα/RXRα的转录活性，并降低NFκB的反式激活作用。

Fibrate and statin synergistically increase the transcriptional activities of PPARalpha/RXRalpha and decrease the transactivation of NFkappaB.

作者信息

Inoue Ikuo, Itoh Fumiaki, Aoyagi Shigemi, Tazawa Shigeki, Kusama Hiroshi, Akahane Masuo, Mastunaga Toshiyuki, Hayashi Kenji, Awata Takuya, Komoda Tugikazu, Katayama Sigehiro

机构信息

Fourth Department of Internal Medicine, Saitama Medical School, 38 Morohongo, Moroyama, Iruma-gun, Saitama 350-0495, Japan.

出版信息

Biochem Biophys Res Commun. 2002 Jan 11;290(1):131-9. doi: 10.1006/bbrc.2001.6141.

DOI:10.1006/bbrc.2001.6141

PMID:11779144

Abstract

In this study, we used a coactivator-dependent receptor-ligand interaction assay (CARLA), which is a semifunctional in vitro assay, to determine whether hypolipidemic drugs are ligands for the three peroxisome proliferator-activated receptor isotypes (PPARalpha, delta, and gamma). We also evaluated the transcriptional activities of the three PPAR isotypes by transient transfection assays. We found that bezafibrate was a ligand for PPARalpha, delta, and gamma in the CARLA and that bezafibrate induced transcriptional activation of PPARalpha/RXRalpha, PPARdelta/RXRalpha, and PPARgamma/RXRalpha. Although the 3-hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase inhibitors cerivastatin, fluvastatin, and pitavastatin were not ligands for these three nuclear receptors in the CARLA, they induced transcriptional activation of PPARalpha/RXRalpha, PPARdelta/RXRalpha, and PPARgamma2/RXRalpha. Moreover, cerivastatin, fluvastatin, and pitavastatin synergistically and dose-dependently increased the transcriptional activation of PPARalpha/RXRalpha induced by bezafibrate. In addition, the cerivastatin-induced transcriptional activation of PPARalpha/RXRalpha was decreased by addition of mevalonate, farnesol, geranylgeraniol, or cholesterol and by co-transfection with sterol regulatory element-binding protein-1 (SREBP-1). Moreover, concomitant administration of statins and fibrates also decreased the transactivation of nuclear factor kappaB (NFkappaB) and the activation of NFkappaB by mitogen-activated protein kinase kinase kinase (MEKK) also decreased the transactivation of PPARalpha/RXRalpha.

摘要

在本研究中，我们使用了一种依赖共激活因子的受体 - 配体相互作用测定法（CARLA），这是一种半功能性体外测定法，以确定降血脂药物是否为三种过氧化物酶体增殖物激活受体亚型（PPARα、δ和γ）的配体。我们还通过瞬时转染测定法评估了这三种PPAR亚型的转录活性。我们发现，在CARLA中，苯扎贝特是PPARα、δ和γ的配体，并且苯扎贝特可诱导PPARα/RXRα、PPARδ/RXRα和PPARγ/RXRα的转录激活。尽管3 - 羟基 - 3 - 甲基戊二酰辅酶A（HMG - CoA）还原酶抑制剂西立伐他汀、氟伐他汀和匹伐他汀在CARLA中不是这三种核受体的配体，但它们可诱导PPARα/RXRα、PPARδ/RXRα和PPARγ2/RXRα的转录激活。此外，西立伐他汀、氟伐他汀和匹伐他汀协同且剂量依赖性地增加了苯扎贝特诱导的PPARα/RXRα的转录激活。另外，添加甲羟戊酸、法尼醇、香叶基香叶醇或胆固醇以及与固醇调节元件结合蛋白 - 1（SREBP - 1）共转染可降低西立伐他汀诱导的PPARα/RXRα的转录激活。此外，他汀类药物和贝特类药物联合给药也可降低核因子κB（NFκB）的反式激活，并且丝裂原活化蛋白激酶激酶激酶（MEKK）对NFκB的激活也可降低PPARα/RXRα的反式激活。

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贝特类药物和他汀类药物协同增加PPARα/RXRα的转录活性，并降低NFκB的反式激活作用。

Fibrate and statin synergistically increase the transcriptional activities of PPARalpha/RXRalpha and decrease the transactivation of NFkappaB.

作者信息

Inoue Ikuo, Itoh Fumiaki, Aoyagi Shigemi, Tazawa Shigeki, Kusama Hiroshi, Akahane Masuo, Mastunaga Toshiyuki, Hayashi Kenji, Awata Takuya, Komoda Tugikazu, Katayama Sigehiro

机构信息

Fourth Department of Internal Medicine, Saitama Medical School, 38 Morohongo, Moroyama, Iruma-gun, Saitama 350-0495, Japan.

出版信息

Biochem Biophys Res Commun. 2002 Jan 11;290(1):131-9. doi: 10.1006/bbrc.2001.6141.

DOI:10.1006/bbrc.2001.6141

PMID:11779144

Abstract

摘要

贝特类药物和他汀类药物协同增加PPARα/RXRα的转录活性，并降低NFκB的反式激活作用。

Fibrate and statin synergistically increase the transcriptional activities of PPARalpha/RXRalpha and decrease the transactivation of NFkappaB.

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贝特类药物和他汀类药物协同增加PPARα/RXRα的转录活性，并降低NFκB的反式激活作用。

Fibrate and statin synergistically increase the transcriptional activities of PPARalpha/RXRalpha and decrease the transactivation of NFkappaB.

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