Jiangsu Simcere Pharmaceutical Research Institute and Jiangsu Key Laboratory of Molecular Targeted Antitumor Drug Research, No 699-18 Xuan Wu Avenue, Xuan Wu District, Nanjing 210042, PRC.
J Med Chem. 2010 Mar 11;53(5):1990-9. doi: 10.1021/jm901407s.
A series of novel dipeptidyl boronic acid proteasome inhibitors composed of beta-amino acids were synthesized, in vitro and in vivo biologically evaluated, and theoretically modeled for the first time. From the screened racemic compounds in enzyme, 4i was the most active. The IC(50) value of its pure enantiomer 4q was 9.6 nM, 36-fold more active than its isomer 4p and as active as the marketed bortezomib in inhibiting human 20S proteasome. This candidate also showed good activities with IC(50) values nearly less than 5 microM against several human solid and hematologic tumor cell lines. Safety evaluation in vivo with zebrafish and Sprague-Dawley (SD) rats showed that the candidate 4q was less toxic than bortezomib. Pharmacokinetic profiles suggested candidate 4q showed a more plasma exposure and longer half-life than bortezomib. Docking results indicated that 4q nearly interacted with 20S proteasome in a similar way as bortezomib.
首次合成了一系列由β-氨基酸组成的新型二肽硼酸蛋白酶体抑制剂,对其进行了体外和体内生物评价,并进行了理论模拟。在酶筛选的外消旋化合物中,4i 是最活跃的。其纯对映异构体 4q 的 IC50 值为 9.6 nM,比其异构体 4p 活性高 36 倍,与市售硼替佐米抑制人 20S 蛋白酶体的活性相当。该候选药物对多种人实体瘤和血液肿瘤细胞系也表现出良好的活性,IC50 值接近 5μM。用斑马鱼和 Sprague-Dawley(SD)大鼠进行的体内安全性评估表明,候选药物 4q 的毒性比硼替佐米低。药代动力学研究表明,候选物 4q 比硼替佐米具有更高的血浆暴露量和更长的半衰期。对接结果表明,4q 与 20S 蛋白酶体的相互作用方式与硼替佐米非常相似。
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