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首页> 外文期刊>Archives of pharmacal research >PAR-1622 is a selective peroxisome proliferator-activated receptor gamma partial activator with preserved antidiabetic efficacy and broader safety profile for fluid retention.
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PAR-1622 is a selective peroxisome proliferator-activated receptor gamma partial activator with preserved antidiabetic efficacy and broader safety profile for fluid retention.

机译:PAR-1622是一种选择性的过氧化物酶体增殖物激活的受体γ部分激活剂,具有抗糖尿病药的功效,并具有更广泛的液体保留安全性。

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Peroxisome proliferator-activated receptor (PPAR) gamma is known to be a key regulator of insulin resistance. PAR-1622 is a novel small molecule compound synthesized in Dong-A research center. In this study, we characterized the pharmacological profiles of PAR-1622, a selective partial activator of PPARgamma. In transient transactivation assays, PAR-1622 [(S)-2-ethoxy-3(4-(5-(4-(5-(methoxymethyl)isoxazol-3-yl)phenyl)-3-methylthiophen- 2-yl)methoxy)phenyl)propanoic acid] showed a partial activator against human PPARgamma with an EC(50) of 41 nM and a maximal response of 37% relative to the full agonist rosiglitazone without activating human PPARdelta. PAR-1622 was 56 folds more selective for human PPARgamma than for human PPARalpha (EC(50), 2304 nM), which means that it is a selective partial activator of PPARgamma. PAR-1622 also showed a partial activator against mouse PPARgamma with an EC(50) of 427 nM and a maximal response was 57% of that of rosiglitazone. INT-131, a selective PPARgamma partial agonist in clinical stage, also was a partial activator against human PPARgamma with an EC(50) of 83 nM and a maximal response achieved by INT-131 was 49% of that observed with full agonist rosiglitazone. In functional assays using human mesenchymal stem cells, PAR-1622 induced adipocyte differentiation, which was 3-fold more potent with a comparable maximum response compared to INT-131. Furthermore, PAR-1622 significantly improved hyperglycemia in db/db when orally administered at a dose of 1 mg/kg/day for 5 days. In hemodilution assays with Evans Blue, rosiglitazone significantly increased the plasma volume in ICR mice that were orally administered 30 mg/kg/day for 9 days; however, PAR-1622 showed no significant effects on plasma volume, similar to INT-131. These results suggest that PAR-1622 is a selective partial activator of PPARgamma and has excellent antihyperglycemic activities and a broad safety profile for fluid retention.
机译:过氧化物酶体增殖物激活受体(PPAR)γ是胰岛素抵抗的关键调节剂。 PAR-1622是由Dong-A研究中心合成的新型小分子化合物。在这项研究中,我们表征了PAR-1622(PPARγ的选择性部分激活剂)的药理特性。在瞬时反式激活分析中,PAR-1622 [(S)-2-乙氧基-3(4-(5-(4-(5-(甲氧基甲基)异恶唑-3-基)苯基)-3-甲基噻吩-2-基)甲氧基)苯基丙酸]显示了针对人PPARγ的部分活化剂,其EC(50)为41 nM,相对于完整的激动剂罗格列酮,最大响应为37%,而未激活人PPARδ。 PAR-1622对人PPARγ的选择性比对人PPARα的选择性高56倍(EC(50),2304 nM),这意味着它是PPARγ的选择性部分活化剂。 PAR-1622还显示了针对小鼠PPARγ的部分激活剂,其EC(50)为427 nM,最大响应为罗格列酮的57%。 INT-131是临床阶段的选择性PPARgamma部分激动剂,也是人PPARgamma的部分激活剂,EC(50)为83 nM,而INT-131达到的最大应答是罗格列酮全激动剂的49%。在使用人间充质干细胞的功能测定中,PAR-1622诱导脂肪细胞分化,与INT-131相比,其最大效力高3倍,具有可比的最大响应。此外,当以1 mg / kg /天的剂量口服5天时,PAR-1622可显着改善db / db中的高血糖。在使用Evans Blue进行的血液稀释测定中,罗格列酮显着增加了口服口服30 mg / kg / day连续9天的ICR小鼠的血浆容量;然而,与INT-131相似,PAR-1622对血浆容量没有显着影响。这些结果表明,PAR-1622是PPARgamma的选择性部分活化剂,具有出色的降血糖活性和对液体retention留的广泛安全性。

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