Alker D, Campbell S F, Cross P E
Pfizer Central Research, Sandwich, Kent, United Kingdom.
J Med Chem. 1991 Jan;34(1):19-24. doi: 10.1021/jm00105a004.
The preparation of 4-(2,3-dichlorophenyl)-3-(ethoxycarbonyl)-2-[(2-hydroxyethoxy)methyl]-5- (methoxycarbonyl)-6-methyl-1,4-dihydropyridine (2) is described, and its potent calcium antagonist activity on rat aorta (IC50 = 4 x 10(-9) M) and marked tissue selectivity in vitro for vascular smooth muscle over cardiac smooth muscle are established. In order to exploit the excellent in vitro profile of compound 2, a range of analogues were prepared but none were found to have superior calcium antagonist potency and tissue selectivity. Compound 2 has excellent in vivo activity in the anesthetized dog (ED50 = 12 micrograms/kg for reduction of CVR) and a plasma half-life in the conscious dog of 7.2 h. The pharmacokinetic parameters of 2 are compared to those determined for the structurally related compounds amlodipine and felodipine. The plasma clearance for 2 (9.6 mL/min/kg) is similar to that of amlodipine and is consistent with the extended 2-substituent hindering approach to the cytochrome P-450 enzyme responsible for oxidation of the DHP ring to the corresponding pyridine.
描述了4-(2,3-二氯苯基)-3-(乙氧羰基)-2-[(2-羟基乙氧基)甲基]-5-(甲氧羰基)-6-甲基-1,4-二氢吡啶(2)的制备方法,并确定了其对大鼠主动脉的强效钙拮抗剂活性(IC50 = 4×10(-9) M)以及在体外对血管平滑肌相对于心脏平滑肌具有显著的组织选择性。为了利用化合物2优异的体外特性,制备了一系列类似物,但未发现有具有更优钙拮抗剂效力和组织选择性的化合物。化合物2在麻醉犬中具有优异的体内活性(降低CVR的ED50 = 12微克/千克),在清醒犬中的血浆半衰期为7.2小时。将2的药代动力学参数与结构相关化合物氨氯地平和非洛地平所测定的参数进行了比较。2的血浆清除率(9.6毫升/分钟/千克)与氨氯地平相似,这与2位取代基的延长阻碍了负责将二氢吡啶环氧化为相应吡啶的细胞色素P-450酶的作用相一致。
