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Imiglitazar,250601-04-8

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  • ¥10780
  • MedChemExpress(MCE)已认证
  • 美国
  • HY-101649
  • 2025年12月05日
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    • 详细信息
    • 技术资料
    • 保存条件

      Please store the product under the recommended conditions in the Certificate of Analysis.

    • 英文名

      TAK-559

    • 库存

      货期:询盘

    • 供应商

      MedChemExpress LLC

    • CAS号

      250601-04-8

    • 规格

      1 mg

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    Imiglitazar

    CAS No. : 250601-04-8

    MCE 国际站:Imiglitazar

    产品活性:Imiglitazar (TAK559)是有效地人类PPARαPPARγ1双重激动剂,EC50值分为67 和31 nM。

    研究领域:Cell Cycle/DNA Damage  |  Vitamin D Related/Nuclear Receptor

    作用靶点:PPAR

    In Vitro: TAK-559 is a partial agonist for hPPARg1 with about 68% of maximal activation obtained with rosiglitazone, a known PPARγ agonist. PPARy is significantly activated at a high concentration (10 μM) of TAK-559. Competition-binding assays using radiolabeled ligand indicates that the transactivation of all hPPAR subtypes by TAK-559 is due to direct binding of TAK-559 to each subtype. TAK-559 also recruit the coactivator SRC-1 to each of hPPARγ1 and hPPARα, and to dissociate the corepressor NCoR from each of hPPARγ1 and hPPARα.TNFα- or IL-1β-induced THP-1 cell attachment to cultured endothelial cells is significantly reduced in the presence of 10 μM TAK-559. The secretion of monocyte chemoattractant protein-1 (MCP-1) from endothelial cells is reduced by 36% in the presence of 10 μM TAK-559, accompanied with the decreased mRNA expression in the cells. The proliferation and migration of cultured smooth muscle cells are significantly decreased in the presence of TAK-559.

    In Vivo: TAK-559 treatment results in significant elevation of circulating high-density lipoprotein (HDL) cholesterol levels, consisting of an increase in large HDL particles and a decrease in small dense HDL particles. Plasma triglyceride and apolipoprotein B-100 levels decrease, whereas apolipoprotein A-I increasesduring TAK-559 treatment. Hyperinsulinemia and insulin resistance are significantly corrected with the highest dose of 3.0 mg/kg per day in these prediabetic monkeys. In addition, no adverse effects on representative liver function parameters are observed during the study period.

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