Department of Medicinal Chemistry, Organic Pharmaceutical Chemistry, BMC, Uppsala University, P.O. Box 574, SE-751 23 Uppsala, Sweden.
J Med Chem. 2012 Mar 22;55(6):2724-36. doi: 10.1021/jm201620t. Epub 2012 Mar 13.
In an effort to identify a new class of druglike HIV-1 protease inhibitors, four different stereopure β-hydroxy γ-lactam-containing inhibitors have been synthesized, biologically evaluated, and cocrystallized. The impact of the tether length of the central spacer (two or three carbons) was also investigated. A compound with a shorter tether and (3R,4S) absolute configuration exhibited high activity with a K(i) of 2.1 nM and an EC(50) of 0.64 μM. Further optimization by decoration of the P1' side chain furnished an even more potent HIV-1 protease inhibitor (K(i) = 0.8 nM, EC(50) = 0.04 μM). According to X-ray analysis, the new class of inhibitors did not fully succeed in forming two symmetric hydrogen bonds to the catalytic aspartates. The crystal structures of the complexes further explain the difference in potency between the shorter inhibitors (two-carbon spacer) and the longer inhibitors (three-carbon spacer).
为了鉴定一类新的类似药物的 HIV-1 蛋白酶抑制剂,我们合成了四种不同的立体纯的含有β-羟基γ-内酰胺的抑制剂,对其进行了生物学评价,并进行了共结晶。我们还研究了中心连接基团(两个或三个碳原子)的连接长度的影响。具有较短连接基团和(3R,4S)绝对构型的化合物表现出很高的活性,其 K(i)值为 2.1 nM,EC(50)值为 0.64 μM。通过对 P1'侧链的进一步修饰,得到了一种更有效的 HIV-1 蛋白酶抑制剂(K(i) = 0.8 nM,EC(50) = 0.04 μM)。根据 X 射线分析,新型抑制剂并没有完全成功地与催化天冬氨酸形成两个对称的氢键。复合物的晶体结构进一步解释了较短抑制剂(两个碳原子的连接基团)和较长抑制剂(三个碳原子的连接基团)之间效力的差异。
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