Allosteric inhibition of PTP1B by bromocatechol-chalcone derivatives

被引：0

作者：

Gao, Chenxia ^{[1
]}

Hu, Wenpeng ^{[1
]}

Xu, Feng ^{[3
]}

Lin, Yuxi ^{[1
]}

Chen, Jiashu ^{[1
]}

Shi, Dayong ^{[1
,2
]}

Xing, Pan ^{[1
]}

Zhu, Jiqiang ^{[1
,4
]}

Li, Xiangqian ^{[1
,2
]}

机构：

[1] Shandong Univ, State Key Lab Microbial Technol, Qingdao 266237, Shandong, Peoples R China

[2] Qingdao Marine Sci & Technol Ctr, Lab Marine Drugs & Bioprod, Qingdao 266237, Shandong, Peoples R China

[3] Qingdao Univ, Affiliated Hosp, Qingdao 266000, Shandong, Peoples R China

[4] Shandong Linghai Biotechnol Co Ltd, Jinan 250299, Shandong, Peoples R China

来源：

EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY | 2025年 / 282卷

关键词：

Type 2 diabetes mellitus; PTP1B; Allosteric inhibitors; BB site; Bromocatechol-chalcone; TYROSINE-PHOSPHATASE; 1B; FLAVONOIDS;

D O I：

10.1016/j.ejmech.2024.117053

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

Development of allosteric inhibitors may be a viable strategy to discover hypoglycemic drugs targeting PTP1B. Allosteric inhibitors occupying the BB site that is a hydrophobic pocket restrict the WPD loop in an open conformation, preventing the physiological dephosphorylation reaction. Toward the BB site, sixty bromocatechol-chalcone derivatives were designed and synthesized as allosteric inhibitors of PTP1B against diabetes mellitus. The most potent compound LXQ-87 (C8) inhibited PTP1B noncompetitively with an IC50 value of 1.061 +/- 0.202 mu M. Oral administration of LXQ-87 reduces the fasting blood glucose level and improves glucose tolerance and dyslipidemia in BKS db/db mice suffering from T2DM. LXQ-87 alleviates insulin resistance and promotes cellular glucose uptake by directly binding to intracellular PTP1B.

引用

页数：19

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