Pyridothiadiazine derivatives as aldose reductase inhibitors having antioxidant activity

Shaojuan Zhu; Shuzhen Zhang; Xin Hao; Xiangyu Qin; Shagufta Parveen; Shaoqi Yang; Bing Ma; Changjin Zhu

doi:10.1080/14756366.2016.1178638

Pyridothiadiazine derivatives as aldose reductase inhibitors having antioxidant activity

Shaojuan Zhu, Shuzhen Zhang, Xin Hao, Xiangyu Qin, Shagufta Parveen, Shaoqi Yang, Bing Ma, Changjin Zhu^*

^*此作品的通讯作者

化学与化工学院

Beijing Institute of Technology

科研成果: 期刊稿件 › 文章 › 同行评审

6 引用（Scopus）

摘要

A series of aldose reductase (ALR2) inhibitors based on pyridothiadiazine were prepared and evaluated for their activities in ALR2 inhibition, DPPH scavenging, and MDA inhibition. Comparison studies were carried out between analogs having either hydroxyl or methoxy groups substituted on the N2-benzyl side chains of the compounds. Most of the hydroxy-substituted compounds were found to be more potent compared to their methoxy-substituted analogs with respect to DPPH inhibition (>93%) and MDA inhibition (>73%). However, ALR2 inhibitory activity was found to be affected by the electron-withdrawing substituent at the C7 position in addition to the effect of the N2-substituted benzyl group. These results provide an array of multifunctional ALR2 inhibitors possessing capacities both for ALR2 inhibition and as antioxidants.

源语言	英语
页（从-至）	126-130
页数	5
期刊	Journal of Enzyme Inhibition and Medicinal Chemistry
卷	31
DOI	https://doi.org/10.1080/14756366.2016.1178638
出版状态	已出版 - 1 11月 2016

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abstract = "A series of aldose reductase (ALR2) inhibitors based on pyridothiadiazine were prepared and evaluated for their activities in ALR2 inhibition, DPPH scavenging, and MDA inhibition. Comparison studies were carried out between analogs having either hydroxyl or methoxy groups substituted on the N2-benzyl side chains of the compounds. Most of the hydroxy-substituted compounds were found to be more potent compared to their methoxy-substituted analogs with respect to DPPH inhibition (>93%) and MDA inhibition (>73%). However, ALR2 inhibitory activity was found to be affected by the electron-withdrawing substituent at the C7 position in addition to the effect of the N2-substituted benzyl group. These results provide an array of multifunctional ALR2 inhibitors possessing capacities both for ALR2 inhibition and as antioxidants.",

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author = "Shaojuan Zhu and Shuzhen Zhang and Xin Hao and Xiangyu Qin and Shagufta Parveen and Shaoqi Yang and Bing Ma and Changjin Zhu",

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AU - Zhu, Shaojuan

AU - Zhang, Shuzhen

AU - Hao, Xin

AU - Qin, Xiangyu

AU - Parveen, Shagufta

AU - Yang, Shaoqi

AU - Ma, Bing

AU - Zhu, Changjin

PY - 2016/11/1

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N2 - A series of aldose reductase (ALR2) inhibitors based on pyridothiadiazine were prepared and evaluated for their activities in ALR2 inhibition, DPPH scavenging, and MDA inhibition. Comparison studies were carried out between analogs having either hydroxyl or methoxy groups substituted on the N2-benzyl side chains of the compounds. Most of the hydroxy-substituted compounds were found to be more potent compared to their methoxy-substituted analogs with respect to DPPH inhibition (>93%) and MDA inhibition (>73%). However, ALR2 inhibitory activity was found to be affected by the electron-withdrawing substituent at the C7 position in addition to the effect of the N2-substituted benzyl group. These results provide an array of multifunctional ALR2 inhibitors possessing capacities both for ALR2 inhibition and as antioxidants.

AB - A series of aldose reductase (ALR2) inhibitors based on pyridothiadiazine were prepared and evaluated for their activities in ALR2 inhibition, DPPH scavenging, and MDA inhibition. Comparison studies were carried out between analogs having either hydroxyl or methoxy groups substituted on the N2-benzyl side chains of the compounds. Most of the hydroxy-substituted compounds were found to be more potent compared to their methoxy-substituted analogs with respect to DPPH inhibition (>93%) and MDA inhibition (>73%). However, ALR2 inhibitory activity was found to be affected by the electron-withdrawing substituent at the C7 position in addition to the effect of the N2-substituted benzyl group. These results provide an array of multifunctional ALR2 inhibitors possessing capacities both for ALR2 inhibition and as antioxidants.

KW - Aldose reductase inhibitors

KW - antioxidant activity

KW - pyridothiadiazine derivatives

KW - structure-activity relationships

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Pyridothiadiazine derivatives as aldose reductase inhibitors having antioxidant activity

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