邻位取代的唑类化合物作为血管内皮生长因子受体1和2的选择性双重抑制剂
ortho-Substituted azoles as selective and dual inhibitors of VEGF receptors 1 and 2.
作者信息
Kiselyov Alexander S, Piatnitski Evgueni L, Samet Alexander V, Kisliy Victor P, Semenov Victor V
机构信息
Small Molecule Drug Discovery, Chemical Diversity, Inc., 11558 Sorrento Valley Road, San Diego, CA 92121, USA.
出版信息
Bioorg Med Chem Lett. 2007 Mar 1;17(5):1369-75. doi: 10.1016/j.bmcl.2006.11.087. Epub 2006 Dec 2.
We have developed a series of novel potent ortho-substituted azole derivatives active against kinases VEGFR-1 and VEGFR-2. Both specific and dual ATP-competitive inhibitors of VEGFR-2 were identified. Kinase activity and selectivity could be controlled by varying the arylamido substituents at the azole ring. The most specific molecule (17) displayed > 10-fold selectivity for VEGFR-2 over VEGFR-1. Compound activities in enzymatic and cell-based assays were in the range of activities for reported clinical and development candidates (IC50 < 100 nM), including Novartis' PTK787 (Vatalanib). High permeability of active compounds across the Caco-2 cell monolayer (> 30x10(-5) cm/min) is indicative of their potential for intestinal absorption upon oral administration.
我们开发了一系列新型强效的邻位取代唑衍生物,它们对激酶VEGFR-1和VEGFR-2具有活性。已鉴定出VEGFR-2的特异性和双重ATP竞争性抑制剂。通过改变唑环上的芳酰胺取代基,可以控制激酶活性和选择性。最具特异性的分子(17)对VEGFR-2的选择性比对VEGFR-1高10倍以上。在酶促和基于细胞的测定中,化合物的活性处于已报道的临床和开发候选药物(IC50 < 100 nM)的活性范围内,包括诺华公司的PTK787(瓦他拉尼)。活性化合物在Caco-2细胞单层上具有高渗透性(> 30x10(-5) cm/min),这表明它们口服给药后具有肠道吸收的潜力。
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