University of Ljubljana, Faculty of Pharmacy, Aškerčeva 7, 1000 Ljubljana, Slovenia.
University of Ljubljana, Faculty of Pharmacy, Aškerčeva 7, 1000 Ljubljana, Slovenia.
Bioorg Chem. 2022 Feb;119:105581. doi: 10.1016/j.bioorg.2021.105581. Epub 2021 Dec 25.
The therapeutic indications for monoamine oxidases A and B (MAO-A and MAO-B) inhibitors that have emerged from biological studies on animal and cellular models of neurological and oncological diseases have focused drug discovery projects upon identifying reversible MAO inhibitors. Screening of our in-house academic compound library identified two hit compounds that inhibit MAO-B with IC values in micromolar range. Two series of indole (23 analogues) and 3-(benzyloxy)benzyl)piperazine (16 analogues) MAO-B inhibitors were derived from hits, and screened for their structure-activity relationships. Both series yielded low micromolar selective inhibitors of human MAO-B, namely indole 2 (IC = 12.63 ± 1.21 µM) and piperazine 39 (IC = 19.25 ± 4.89 µM), which is comparable to selective MAO-B inhibitor isatin (IC = 6.10 ± 2.81 µM), yet less potent in comparison to safinamide (IC = 0.029 ± 0.002 µM). Selective MAO-B inhibitors 2, 14, 38 and 39 exhibited favourable permeation of the blood-brain barrier and low cytotoxicity in the human neuroblastoma cell line SH-SY5Y.
单胺氧化酶 A 和 B(MAO-A 和 MAO-B)抑制剂的治疗指征已经从神经和肿瘤疾病的动物和细胞模型的生物学研究中显现出来,这些研究集中在发现可逆 MAO 抑制剂上。对我们内部学术化合物库的筛选确定了两种具有抑制 MAO-B 的 IC 值在微摩尔范围内的有效化合物。从这些有效化合物中衍生出了两个吲哚(23 个类似物)和 3-(苯氧基)苄基)哌嗪(16 个类似物)MAO-B 抑制剂系列,并对其进行了构效关系筛选。这两个系列都产生了对人 MAO-B 的低微摩尔选择性抑制剂,即吲哚 2(IC = 12.63 ± 1.21 μM)和哌嗪 39(IC = 19.25 ± 4.89 μM),与选择性 MAO-B 抑制剂色氨酸(IC = 6.10 ± 2.81 μM)相当,但与沙非酰胺(IC = 0.029 ± 0.002 μM)相比,其效力较低。选择性 MAO-B 抑制剂 2、14、38 和 39 在人神经母细胞瘤细胞系 SH-SY5Y 中表现出良好的血脑屏障通透性和低细胞毒性。
