通过单个甲基实现高度选择性 MERTK 抑制剂。

Highly Selective MERTK Inhibitors Achieved by a Single Methyl Group.

机构信息

Center for Integrative Chemical Biology and Drug Discovery, Division of Chemical Biology and Medicinal Chemistry , UNC Eshelman School of Pharmacy , Chapel Hill , North Carolina 27599 , United States.

Meryx, Inc. , 450 West Drive , Chapel Hill , North Carolina 27599 , United States.

出版信息

J Med Chem. 2018 Nov 21;61(22):10242-10254. doi: 10.1021/acs.jmedchem.8b01229. Epub 2018 Nov 5.

DOI:10.1021/acs.jmedchem.8b01229

PMID:30347155

Abstract

Although all kinases share the same ATP binding pocket, subtle differences in the residues that form the pocket differentiate individual kinases' affinity for ATP competitive inhibitors. We have found that by introducing a single methyl group, the selectivity of our MERTK inhibitors over another target, FLT3, was increased up to 1000-fold (compound 31). Compound 19 was identified as an in vivo tool compound with subnanomolar activity against MERTK and 38-fold selectivity over FLT3 in vitro. The potency and selectivity of 19 for MERTK over FLT3 were confirmed in cell-based assays using human cancer cell lines. Compound 19 had favorable pharmacokinetic properties in mice. Phosphorylation of MERTK was decreased by 75% in bone marrow leukemia cells from mice treated with 19 compared to vehicle-treated mice.

摘要

尽管所有激酶都具有相同的 ATP 结合口袋，但形成口袋的残基的细微差异区分了各个激酶对 ATP 竞争抑制剂的亲和力。我们发现，通过引入单个甲基基团，我们的 MERTK 抑制剂相对于另一个靶标 FLT3 的选择性提高了 1000 倍（化合物 31）。化合物 19 被鉴定为具有体内工具化合物活性，对 MERTK 的活性为亚纳摩尔，对 FLT3 的体外选择性为 38 倍。在使用人癌细胞系的基于细胞的测定中，确认了 19 对 MERTK 的效力和选择性超过 FLT3。化合物 19 在小鼠中的药代动力学特性良好。与用载体处理的小鼠相比，用 19 处理的小鼠骨髓白血病细胞中的 MERTK 磷酸化降低了 75％。

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通过单个甲基实现高度选择性 MERTK 抑制剂。

Highly Selective MERTK Inhibitors Achieved by a Single Methyl Group.

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