噻唑烷-2,4-二酮杂合物作为双α-淀粉酶和α-葡萄糖苷酶抑制剂:设计、合成及抗糖尿病评价
Thiazolidine-2,4-dione hybrids as dual alpha-amylase and alpha-glucosidase inhibitors: design, synthesis, and anti-diabetic evaluation.
作者信息
Singh Gurpreet, Singh Rajveer, Monga Vikramdeep, Mehan Sidharth
机构信息
Department of Pharmaceutical Chemistry, ISF College of Pharmacy, (Affiliated to IK Gujral Punjab Technical University, Kapurthala) GT Road, Ghal Kalan Moga-142001 Punjab India.
Research Scholar, IK Gujral Punjab Technical University Kapurthala Punjab India.
出版信息
RSC Med Chem. 2024 Jul 22;15(8):2826-2854. doi: 10.1039/d4md00199k. eCollection 2024 Aug 14.
Twelve 3,5-disubstituted-thiazolidine-2,4-dione (TZD) hybrids were synthesized using solution phase chemistry. Continuing our previous work, nine -modified ethyl vanillin (8a-i) derivatives were synthesized and reacted with the TZD core Knoevenagel condensation under primary reaction conditions to obtain final derivatives 9a-i. Additionally, three isatin-TZD hybrids (11a-c) were synthesized. The intermediates and final derivatives were characterized using H and C NMR spectroscopy, and the observed chemical shifts agreed with the proposed structures. The alpha-amylase and alpha-glucosidase inhibitory evaluation of newly synthesized derivatives revealed compounds 9F and 9G as the best dual inhibitors, with IC values of 9.8 ± 0.047 μM for alpha-glucosidase (9F) and 5.15 ± 0.0017 μM for alpha-glucosidase (9G), 17.10 ± 0.015 μM for alpha-amylase (9F), and 9.2 ± 0.092 μM for alpha-amylase (9G). The docking analysis of synthesized compounds indicated that compounds have a higher binding affinity for alpha-glucosidase as compared to alpha-amylase, as seen from docking scores ranging from -1.202 to -5.467 (for alpha-amylase) and -4.373 to -7.300 (for alpha-glucosidase). Further, the molecules possess a high LD value, typically ranging from 1000 to 1600 mg kg of body weight, and exhibit non-toxic properties. The cytotoxicity assay results on PANC-1 and INS-1 cells demonstrated that the compounds were devoid of significant toxicity against the tested cells. Compounds 9F and 9G showed high oral absorption, , oral absorption >96%, and their molecular dynamics simulation yielded results closely aligned with the observed docking outcomes. Finally, compounds 9F and 9G were evaluated for antidiabetic assessment by the induction of diabetes in Wistar rats using streptozotocin. Molecule 9G has been identified as the most effective anti-diabetic molecule due to its ability to modulate several biochemical markers in blood plasma and tissue homogenates. The results were further confirmed by histology investigations conducted on isolated pancreas, liver, and kidney.
采用溶液相化学方法合成了12种3,5 - 二取代噻唑烷 - 2,4 - 二酮(TZD)杂化物。延续我们之前的工作,合成了9种修饰的乙基香兰素(8a - i)衍生物,并使其在主要反应条件下与TZD核心进行Knoevenagel缩合反应,以获得最终衍生物9a - i。此外,还合成了3种异吲哚酮 - TZD杂化物(11a - c)。使用氢谱和碳谱核磁共振波谱对中间体和最终衍生物进行了表征,观察到的化学位移与所提出的结构相符。对新合成衍生物的α - 淀粉酶和α - 葡萄糖苷酶抑制活性评估显示,化合物9F和9G是最佳的双重抑制剂,α - 葡萄糖苷酶的IC值分别为9.8 ± 0.047 μM(9F)和5.15 ± 0.0017 μM(9G),α - 淀粉酶的IC值分别为17.10 ± 0.015 μM(9F)和9.2 ± 0.092 μM(9G)。合成化合物的对接分析表明,与α - 淀粉酶相比,化合物对α - 葡萄糖苷酶具有更高的结合亲和力,对接分数范围为 - 1.202至 - 5.467(α - 淀粉酶)和 - 4.373至 - 7.300(α - 葡萄糖苷酶)。此外,这些分子具有较高的半数致死量值,通常在1000至1600 mg/kg体重范围内,且表现出无毒特性。对PANC - 1和INS - 1细胞的细胞毒性测定结果表明,这些化合物对受试细胞没有明显毒性。化合物9F和9G显示出高口服吸收率(口服吸收>96%),并且它们的分子动力学模拟结果与观察到的对接结果紧密一致。最后,通过用链脲佐菌素诱导Wistar大鼠糖尿病来评估化合物9F和9G的抗糖尿病作用。分子9G由于能够调节血浆和组织匀浆中的多种生化标志物,已被确定为最有效的抗糖尿病分子。对分离的胰腺、肝脏和肾脏进行的组织学研究进一步证实了这些结果。
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