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蛋白质酪氨酸磷酸酶抑制剂作为有前景的靶向治疗药物的应用。

Use of protein tyrosine phosphatase inhibitors as promising targeted therapeutic drugs.

作者信息

Heneberg P

机构信息

3rd Faculty of Medicine, Charles University in Prague, Czech Republic.

出版信息

Curr Med Chem. 2009;16(6):706-33. doi: 10.2174/092986709787458407.

DOI:10.2174/092986709787458407
PMID:19199933
Abstract

Protein tyrosine phosphatases (PTPs) are considered to be involved in the etiology of diabetes mellitus, neural diseases such as Alzheimer;s and Parkinson;s disease, regulation of allergy and inflammation, or they are even considered to be responsible for the pathogens; virulence in vivo. Since discovery of first PTP inhibitors such as dephostatin in early 90th years, the research moved on toward search for inhibitors specific for the individual PTP molecules. Currently, dozens of new PTP inhibitors are reported each year, ranging from natural products, natural product analogs, peptides, phosphonates, nonpeptidic inhibitors, mimotopes, metal-containing inhibitors, redox inhibitors, to simply silencing RNAs as widely used inhibitors of PTP expression. Several currently used drugs also show PTP inhibitory activity. Among them are sodium stibogluconate, phenylarsine oxide, alendronate, etidronate, vanadate, gallium nitrate, suramin, or aplidin. However, the market is still waiting for the first clinically approved selective PTP inhibitor. Here in this review are described inhibitors of activity or expression of the particular classical PTPs, with emphasis on specific inhibition of the respective PTP over the others. The inhibitors are not classified according to their chemical composition, but according to their biological activity, which should help to simplify search for inhibitors of particular classical PTPs. Even though PTP inhibitors are difficult to develop, lifting the fog of phosphatase inhibition is of the great market potential and further clinical impact.

摘要

蛋白酪氨酸磷酸酶(PTPs)被认为与糖尿病、阿尔茨海默病和帕金森病等神经疾病的病因有关,参与过敏和炎症的调节,甚至被认为与病原体在体内的毒力有关。自20世纪90年代初发现第一种PTP抑制剂如去磷酸他汀以来,研究朝着寻找针对单个PTP分子的抑制剂方向发展。目前,每年都有数十种新的PTP抑制剂被报道,范围从天然产物、天然产物类似物、肽、膦酸盐、非肽类抑制剂、模拟表位、含金属抑制剂、氧化还原抑制剂,到作为广泛使用的PTP表达抑制剂的简单沉默RNA。几种目前使用的药物也显示出PTP抑制活性。其中包括葡萄糖酸锑钠、苯胂酸氧化物、阿仑膦酸盐、依替膦酸盐、钒酸盐、硝酸镓、苏拉明或阿普立定。然而,市场仍在等待首个临床批准的选择性PTP抑制剂。本文综述了特定经典PTPs活性或表达的抑制剂,并重点介绍了对各自PTP相对于其他PTPs的特异性抑制。抑制剂不是根据其化学成分分类,而是根据其生物活性分类,这应有助于简化对特定经典PTPs抑制剂的搜索。尽管PTP抑制剂难以开发,但消除磷酸酶抑制的迷雾具有巨大的市场潜力和进一步的临床影响。

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