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Pharmacological evaluation of HM41322 a novel SGLT1/2 dual inhibitor in vitro and in vivo

机译:新型SGLT1 / 2双重抑制剂HM41322的体内外药理学评价

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摘要

HM41322 is a novel oral sodium-glucose cotransporter (SGLT) 1/2 dual inhibitor. In this study, the in vitro and in vivo pharmacokinetic and pharmacologic profiles of HM41322 were compared to those of dapagliflozin. HM41322 showed a 10-fold selectivity for SGLT2 over SGLT1. HM41322 showed an inhibitory effect on SGLT2 similar to dapagliflozin, but showed a more potent inhibitory effect on SGLT1 than dapagliflozin. The maximum plasma HM41322 level after single oral doses at 0.1, 1, and 3 mg/kg were 142, 439, and 1830 ng/ml, respectively, and the T1/2 was 3.1 h. HM41322 was rapidly absorbed and reached the circulation within 15 min. HM41322 maximized urinary glucose excretion by inhibiting both SGLT1 and SGLT2 in the kidney. HM41322 3 mg/kg caused the maximum urinary glucose excretion in normoglycemic mice (19.32±1.16 mg/g) at 24 h. In normal and diabetic mice, HM41322 significantly reduced glucose excursion. Four-week administration of HM41322 in db/db mice reduced HbA1c in a dose dependent manner. Taken together, HM41322 showed a favorable preclinical profile of postprandial glucose control through dual inhibitory activities against SGLT1 and SGLT2.
机译:HM41322是新型口服钠-葡萄糖共转运蛋白(SGLT)1/2双重抑制剂。在这项研究中,HM41322的体外和体内药代动力学和药理学特征与达格列净进行了比较。 HM41322对SGLT2的选择性是SGLT1的10倍。 HM41322对达帕格列净的SGLT2具有抑制作用,但对达达格列净的SGLT1具有更强的抑制作用。单次口服0.1、1和3 mg / kg后的最大血浆HM41322水平分别为142、439和1830 ng / ml,T1 / 2为3.1小时。 HM41322被迅速吸收并在15分钟内达到循环。 HM41322通过抑制肾脏中的SGLT1和SGLT2来最大化尿液葡萄糖排泄。 HM41322 3 mg / kg在24 h引起正常血糖小鼠最大尿糖排泄(19.32±1.16 mg / g)。在正常和糖尿病小鼠中,HM41322显着降低了葡萄糖偏移。在db / db小鼠中四周服用HM41322可以剂量依赖性降低HbA1c。两者合计,HM41322通过对SGLT1和SGLT2的双重抑制活性显示了良好的餐前血糖控制的临床前概况。

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