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Abstract

Several 'classical' protein tyrosine phosphatases are attractive therapeutic targets, including PTP1B for obesity and Type II diabetes; SHP2 for cancer and Lyp for rheumatoid arthritis. Progress has been made in identifying a broad range of chemically distinct inhibitors; however, developing selective and cell-permeable clinically useful compounds has proved challenging. Here the ongoing challenges and recent significant advances in the field are reviewed. Key novel compounds are highlighted and a perspective on the future of phosphatase inhibitor development is presented.

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PubMed ID:: 21426149

DOI:: 10.4155/fmc.10.241

ScienceOpen disciplines: Chemistry

Keywords: Animals,Autoimmune Diseases,drug therapy,enzymology,Diabetes Mellitus, Type 2,Drug Discovery,methods,Enzyme Inhibitors,chemistry,pharmacology,therapeutic use,Humans,Models, Molecular,Neoplasms,Obesity,Protein Tyrosine Phosphatases,antagonists & inhibitors,metabolism

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ScienceOpen disciplines: Chemistry

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