卤代类肟作为单胺氧化酶-B 抑制剂用于治疗帕金森病的新型化合物:合成、生化和分子动力学研究。
Halogenated class of oximes as a new class of monoamine oxidase-B inhibitors for the treatment of Parkinson's disease: Synthesis, biochemistry, and molecular dynamics study.
机构信息
College of Pharmacy, Department of Pharmaceutical Chemistry, Jouf University, Sakaka 72341, Al Jouf, Saudi Arabia.
Department of Pharmacy, and Research Institute of Life Pharmaceutical Sciences, Sunchon National University, Suncheon 57922, Republic of Korea.
出版信息
Comput Biol Chem. 2023 Aug;105:107899. doi: 10.1016/j.compbiolchem.2023.107899. Epub 2023 Jun 1.
Oximes are the promising structural scaffold for inhibiting monoamine oxidase (MAO)-B. Eight chalcone-based oxime derivatives were synthesized by microwave-assisted technique, and their ability to inhibit human MAO (hMAO) enzymes were tested. All compounds showed higher inhibitory activity of hMAO-B than hMAO-A. In the CHBO subseries, CHBO4 most potently inhibited hMAO-B with an IC value of 0.031 μM, followed by CHBO3 (IC = 0.075 μM). In the CHFO subseries, CHFO4 showed the highest inhibition of hMAO-B with an IC value of 0.147 μM. Compound CHBO4 had the highest selectivity index (SI) value of 1290.3. However, CHBO3 and CHFO4 showed relatively low SI values of 27.7 and 19.2, respectively. The -Br substituent in the CHBO subseries at the para-position in the B-ring showed higher hMAO-B inhibition than the -F substituent in the CHFO subseries. In both series, hMAO-B inhibition increased with the substituents at para-position in A-ring (-F > -Br > -Cl > -H in order). Compound CHBO4 (-F in A-ring and -Br in B-ring) was 12.6-times potent than the substituents-reversed compound CHFO3 (-Br in A-ring and -F in B-ring; IC = 0.391 μM). In the kinetic study, K values of CHBO4 and CHFO4 for hMAO-B were 0.010 ± 0.005 and 0.040 ± 0.007 μM, respectively, with competitive inhibitions. Reversibility experiments showed that CHBO4 and CHFO4 were reversible hMAO-B inhibitors. In the cytotoxicity test using the Vero cells by the MTT technique, CHBO4 had low toxicity with an IC value of 128.8 µg/mL. In HO-induced cells, CHBO4 significantly reduced cell damage by scavenging reactive oxygen species (ROS). Molecular docking and dynamics showed the stable binding mode of the lead molecule CHBO4 on the active site of hMAO-B. These results suggest that CHBO4 is a potent reversible, competitive, and selective hMAO-B inhibitor and can be used as a treatment agent for neurological disorders.
肟类化合物是抑制单胺氧化酶(MAO)-B 的有前途的结构支架。通过微波辅助技术合成了 8 种查尔酮肟衍生物,并测试了它们抑制人 MAO(hMAO)酶的能力。所有化合物对 hMAO-B 的抑制活性均高于 hMAO-A。在 CHBO 亚系列中,CHBO4 对 hMAO-B 的抑制作用最强,IC 值为 0.031 μM,其次是 CHBO3(IC = 0.075 μM)。在 CHFO 亚系列中,CHFO4 对 hMAO-B 的抑制作用最高,IC 值为 0.147 μM。化合物 CHBO4 的选择性指数(SI)值最高,为 1290.3。然而,CHBO3 和 CHFO4 的 SI 值相对较低,分别为 27.7 和 19.2。B 环对位的 CHBO 亚系列中的-Br 取代基比 CHFO 亚系列中的-F 取代基对 hMAO-B 的抑制作用更强。在这两个系列中,A 环对位取代基(-F > -Br > -Cl > -H)的增加使 hMAO-B 的抑制作用增强。化合物 CHBO4(A 环为-F,B 环为-Br)比取代基相反的化合物 CHFO3(A 环为-Br,B 环为-F;IC = 0.391 μM)强 12.6 倍。在动力学研究中,CHBO4 和 CHFO4 对 hMAO-B 的 K 值分别为 0.010±0.005 和 0.040±0.007 μM,均为竞争性抑制。可逆性实验表明,CHBO4 和 CHFO4 是可逆的 hMAO-B 抑制剂。在 MTT 技术测定的 Vero 细胞毒性试验中,CHBO4 的 IC 值为 128.8 µg/mL,毒性较低。在 HO 诱导的细胞中,CHBO4 通过清除活性氧(ROS)显著减少细胞损伤。分子对接和动力学研究表明,先导分子 CHBO4 在 hMAO-B 的活性部位具有稳定的结合模式。这些结果表明,CHBO4 是一种有效的、可逆的、竞争性的、选择性的 hMAO-B 抑制剂,可作为治疗神经紊乱的药物。
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