Suh Young-Ger, Kim Nam-Jung, Koo Bon-Woong, Lee Kwang-Ok, Moon Sung-Hyun, Shin Dong-Hyung, Jung Jong-Wha, Paek Seung-Mann, Chang Dong-Jo, Li Funan, Kang Hyun-Jin, Le Tuong Vy Thi, Chae Yu Na, Shin Chang Yell, Kim Mi-Kyung, Lim Joong In, Ryu Jae-Sang, Park Hyun-Ju
College of Pharmacy, Seoul National University, San 56-1, Sillim-dong, Gwanak-gu, Seoul 151-742, South Korea.
J Med Chem. 2008 Oct 23;51(20):6318-33. doi: 10.1021/jm8003416. Epub 2008 Oct 1.
In an effort to develop dual PPARalpha/gamma activators with improved therapeutic efficacy, a series of diaryl alpha-ethoxy propanoic acid compounds comprising two aryl groups linked by rigid oxime ether or isoxazoline ring were designed and synthesized and their biological activities were examined. Most of the compounds possessing an oxime ether linker were more potent PPARgamma activators than the lead PPARalpha/gamma dual agonist, tesaglitazar in vitro. Compound 18, one of the derivatives with an oxime ether linker, was found to selectively transactivate PPARgamma (EC 50 = 0.028 microM) over PPARalpha (EC 50 = 7.22 microM) in vitro and lower blood glucose in db/ db mice more than muraglitazar after oral treatment for 11 days.
为了开发具有更高治疗效果的双PPARα/γ激动剂,设计并合成了一系列由刚性肟醚或异恶唑啉环连接两个芳基的二芳基α-乙氧基丙酸化合物,并检测了它们的生物活性。在体外,大多数具有肟醚连接子的化合物作为PPARγ激动剂比先导PPARα/γ双重激动剂替格列扎更有效。化合物18是具有肟醚连接子的衍生物之一,在体外被发现对PPARγ的选择性反式激活作用(EC50 = 0.028微摩尔)高于PPARα(EC50 = 7.22微摩尔),并且在对db/db小鼠口服治疗11天后,其降低血糖的效果比muraglitazar更好。
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