Department of Pharmacy - Center of Drug Research, Ludwig Maximilians-Universität München, Butenandtstr. 7, 81377 Munich, Germany.
Department of Pharmacy - Center of Drug Research, Ludwig Maximilians-Universität München, Butenandtstr. 7, 81377 Munich, Germany.
Bioorg Med Chem. 2019 Jul 1;27(13):2753-2763. doi: 10.1016/j.bmc.2019.05.001. Epub 2019 May 2.
In the present study, the concept of oxime library screening by MS Binding Assays was successfully extended to N-substituted lipophilic pyrrolidine-3-carboxylic acid derivatives in the pursuit of varying the amino acid motif in order to identify new inhibitors for GAT1 and to broaden structure-activity-relationships for this target, the most abundant GABA transporter in the central nervous system. For the screening, 28 different oxime sub-libraries were employed that were generated by simple condensation reaction of an excess of pyrrolidine-3-carboxylic acid derivatives carrying a hydroxylamine functionality with various sub-libraries each assembled of eight aldehydes with broadly varying chemical structures and functionalities. The compounds responsible for the activity of an oxime sub-library were identified by deconvolution experiments performed by employing single oximes. Binding affinities of the oxime hits were confirmed in full-scale competitive MS Binding Assays. Thereby, oxime derivatives with a 1,1'-biphenyl moiety were found as the first inhibitors of mGAT1 comprising a pyrrolidine-3-carboxylic acid motif with affinities in the submicromolar range.
在本研究中,通过 MS 结合分析成功扩展了肟库筛选的概念,以 N-取代的亲脂性吡咯烷-3-羧酸衍生物为研究对象,改变氨基酸结构,以寻找新的 GAT1 抑制剂,并拓宽该靶点(中枢神经系统中含量最丰富的 GABA 转运体)的结构-活性关系。为了进行筛选,使用了 28 种不同的肟亚库,通过过量的带有羟胺官能团的吡咯烷-3-羧酸衍生物与各种亚库(每个亚库由 8 种具有广泛变化的化学结构和官能团的醛组成)的简单缩合反应生成。通过使用单个肟进行解卷积实验,鉴定出负责肟亚库活性的化合物。肟命中物的结合亲和力通过全规模竞争性 MS 结合分析得到确认。因此,发现具有 1,1'-联苯部分的肟衍生物是包含吡咯烷-3-羧酸基序的 mGAT1 的第一个抑制剂,其亲和力在亚微摩尔范围内。
