Li Qun, Li Tongmei, Zhu Gui-Dong, Gong Jianchun, Claibone Akiyo, Dalton Chris, Luo Yan, Johnson Eric F, Shi Yan, Liu Xuesong, Klinghofer Vered, Bauch Joy L, Marsh Kennan C, Bouska Jennifer J, Arries Shannon, De Jong Ron, Oltersdorf Tilman, Stoll Vincent S, Jakob Clarissa G, Rosenberg Saul H, Giranda Vincent L
Cancer Research, GPRD, Abbott Laboratories, Abbott Park, IL 60064-6101, USA.
Bioorg Med Chem Lett. 2006 Mar 15;16(6):1679-85. doi: 10.1016/j.bmcl.2005.12.017. Epub 2006 Jan 5.
A novel series of Akt/PKB inhibitors derived from a screening lead (1) has been prepared. The novel trans-3,4'-bispyridinylethylenes described herein are potent inhibitors of Akt/PKB with IC(50) values in the low double-digit nanomolar range against Akt1. Compound 2q shows excellent selectivity against distinct families of kinases such as tyrosine kinases and CAMK, and displays poor to modest selectivity against closely related kinases in the AGC and CMGC families. The cellular activities including inhibition of cell growth and phosphorylation of downstream target GSK3 are also described. The X-ray structure of compound 2q complexed with PKA in the ATP binding site was determined.
已经制备了一系列源自筛选先导物(1)的新型Akt/PKB抑制剂。本文所述的新型反式-3,4'-双吡啶基乙烯是Akt/PKB的有效抑制剂,对Akt1的IC(50)值处于低两位数纳摩尔范围内。化合物2q对不同激酶家族如酪氨酸激酶和钙/钙调蛋白依赖性蛋白激酶(CAMK)表现出优异的选择性,而对AGC和CMGC家族中密切相关的激酶的选择性则较差至中等。还描述了其细胞活性,包括对细胞生长的抑制以及对下游靶标糖原合成酶激酶3(GSK3)磷酸化的影响。确定了化合物2q与蛋白激酶A(PKA)在ATP结合位点形成复合物的X射线晶体结构。
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