Targeting Alzheimer's disease with novel dual-function 3,5-diaryl-4,5-dihydro-1H-pyrazole-1-carbothioamide derivatives

Aikaterini Katsogiannou , Danai Karta , Antonio Di Stefano , Sena Oner , Mehmet Enes Arslan , Adil Mardinoglu , Hasan Turkez , Stamatia Vassiliou , Ivana Cacciatore
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Abstract

In the field of medicinal chemistry, the versatility of the thiosemicarbazone scaffold makes it a promising platform for the development of next-generation pharmaceuticals. In this paper the thiosemicarbazone scaffold was explored to obtain novel series of derivatives: a) thiosemicarbazones 1531, and 33 containing a linear thiosemicarbazone scaffold, b) 3438 and 4464 containing pyrazoline ring, and c) 3943 containing the dihydropyrimidine cycle. Among these, compounds 21, 23, 26, 3335, 37, 38, 44, 57, 61, and 62 demonstrated no significant cytotoxic effects on HDFa cells at concentrations up to 500 μg/mL. Importantly, compounds 21, 23, 26, 33, 34, 35, and 37 exhibited significant protective effects against neurotoxicity induced by beta-amyloid peptide (1-42) in differentiated SHSY-5Y cell cultures. Enzymatic assays targeting BACE1 and AChE revealed modest inhibitory activity in compounds 21, 23, and 34, 37, respectively. The identification of compounds with inhibitory effects and neuroprotective activity against beta-amyloid peptide (1-42) offers a platform for further optimization and refinement of these compounds to enhance their potency and selectivity.

Abstract Image

用新型双功能 3,5-二芳基-4,5-二氢-1H-吡唑-1-硫代甲酰胺衍生物治疗阿尔茨海默病
在药物化学领域,硫代氨基脲支架的多功能性使其成为开发下一代药物的一个前景广阔的平台。本文通过对硫代氨基羰基支架的探索,获得了一系列新型衍生物:a) 含有线性硫代氨基羰基支架的硫代氨基羰基 15-31 和 33;b) 含有吡唑啉环的 34-38 和 44-64;c) 含有二氢嘧啶循环的 39-43。其中,化合物 21、23、26、33-35、37、38、44、57、61 和 62 在浓度高达 500 μg/mL 时对 HDFa 细胞没有明显的细胞毒性作用。重要的是,在分化的 SHSY-5Y 细胞培养物中,化合物 21、23、26、33、34、35 和 37 对 beta 淀粉样肽(1-42)诱导的神经毒性具有明显的保护作用。针对 BACE1 和 AChE 的酶测定显示,化合物 21、23 和 34、37 分别具有适度的抑制活性。对β-淀粉样肽(1-42)具有抑制作用和神经保护活性的化合物的鉴定为进一步优化和改进这些化合物以提高其效力和选择性提供了一个平台。
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