UMR/CNRS 7199, Faculte de pharmacie, Universite Louis Pasteur, 67404 Illkirch, France.
J Med Chem. 2010 Jan 14;53(1):178-90. doi: 10.1021/jm900872z.
We describe here the biological screening of a collection of natural occurring triterpenoids against the G protein-coupled receptor TGR5, known to be activated by bile acids and which mediates some important cell functions. This work revealed that betulinic (1), oleanolic (2), and ursolic acid (3) exhibited TGR5 agonist activity in a selective manner compared to bile acids, which also activated FXR, the nuclear bile acid receptor. The most potent natural triterpenoid betulinic acid was chosen as a reference compound for an SAR study. Hemisyntheses were performed on the betulinic acid scaffold, and we focused on structural modifications of the C-3 alcohol, the C-17 carboxylic acid, and the C-20 alkene. In particular, structural variations around the C-3 position gave rise to major improvements of potency exemplified with derivatives 18 dia 2 (RG-239) and 19 dia 2. The best derivative was tested in vitro and in vivo, and its biological profile is discussed.
我们在这里描述了对一系列天然存在的三萜类化合物对 G 蛋白偶联受体 TGR5 的生物筛选,已知 TGR5 被胆汁酸激活,并介导一些重要的细胞功能。这项工作表明,与激活核胆汁酸受体 FXR 的胆汁酸相比,白桦脂酸(1)、齐墩果酸(2)和熊果酸(3)以选择性方式表现出 TGR5 激动剂活性。最有效的天然三萜白桦脂酸被选为 SAR 研究的参考化合物。在白桦脂酸骨架上进行了半合成,我们专注于 C-3 醇、C-17 羧酸和 C-20 烯烃的结构修饰。特别是,C-3 位置的结构变化导致了效力的显著提高,例如衍生物 18 dia 2(RG-239)和 19 dia 2。对最佳衍生物进行了体外和体内测试,并讨论了其生物学特性。
