基于咔唑的新型碳酰腙衍生物的合成及蛋白酪氨酸磷酸酶1B(PTP1B)抑制活性评价

合成出了一系列新型基于咔唑的单-/双-碳酰腙衍生物3和4.利用1H NMR、13C NMR、IR和元素分析对其进行了结构表征.评价了目标化合物对蛋白酪氨酸磷酸酶1B(PTP1B)的抑制活性,讨论了结构与活性的关系.实验结果显示,大部分化合物对PTP1B具有良好的抑制活性,其中1,5-双(9-丁基-3-咔唑基)亚甲基]碳酰腙(4c)的抑制活性最高,IC50=(4.81±0.41)mmol/L,且活性高于对照药物齐墩果酸.对目标化合物1-(9-庚基-3-咔唑基)亚甲基]碳酰腙(3f)和4c进行分子对接研究和密度泛函理论(DFT)计算.分子对接结果表明,化合物3f和4c结合到PTP1B酶由螺旋α3和α6形成的活性位点,与PTP1B酶通过氢键、极性、疏水和p-p等相互作用形成了稳定的复合物.

Synthesis and Protein Tyrosine Phosphatase 1B(PTP1B) Inhibitory Activity Evaluation of Novel Carbazole-Based Carbohydrazone Derivatives

A series of novel carbazole-based mono-/bis-carbohydrazone derivatives 3 and 4 were synthesized. Their structures were characterized by 1 H NMR, 13 C NMR, IR spectra and elemental analysis. The inhibitory activities of all synthesized compounds against protein tyrosine phosphatase 1 B(PTP1 B) were evaluated, and the structure-activity relationship was discussed.The results indicated that most of the compounds had good inhibitory activity against PTP1 B, and 1,5-bis(9-butyl-3-carbazolyl)methylene]carbohydrazone(4 c) showed the highest inhibitory activity against PTP1 B with IC50=(4.81±0.41) mmol/L and the activity was higher than that of the control drug oleanolic acid. Molecular docking and density functional theory(DFT)calculations of 3 f and 4 c were carried out. The results of molecular docking indicated that 1-(9-heptyl-3-carbazolyl)methylene]carbohydrazone(3 f) and 4 c bind to an active site of PTP1 B enzyme formed by the helices α3 and α6, and formed a stable complex respectively with PTP1 B enzyme by hydrogen bonds, polar, hydrophobic and p-p interactions.