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Synthesis,activity and molecular modeling of a new series of chromones as low molecular weight protein tyrosine phosphatase inhibitors
Authors:Marco Forghieri  Christian Laggner  Paolo Paoli  Thierry Langer  Giampaolo Manao  Guido Camici  Lucia Bondioli  Fabio Prati  Luca Costantino
Institution:1. Department of Chemistry, University of Modena and R.E., Via G. Campi 183, 41100 Modena, Italy;2. Department of Pharmaceutical Chemistry, Institute of Pharmacy and Center for Molecular Biosciences (CMBI), University of Innsbruck, Innrain 52c, A-6020 Innsbruck, Austria;3. Department of Biochemical Sciences, University of Florence, Viale Morgagni 50, 50134 Florence, Italy;4. Prestwick Chemical Inc., Bld. Gonthier d’Andernach, 67400 Strasbourg-Illkirch, France;5. Center of Excellence for Scientific Research DENOThe, Viale Morgagni 44, 50134 Florence, Italy;6. Department of Pharmaceutical Sciences, University of Modena and R.E., Via G. Campi 183, 41100 Modena, Italy
Abstract:Protein tyrosine phosphatases (PTP) are crucial elements in eukaryotic signal transduction. Several reports suggested that the LMW-PTP family has oncogenic relevance. Moreover, LMW-PTP has been recognized as a negative regulator of insulin-mediated mitotic and metabolic signaling. Thus, inhibition of the LMW-PTP can be considered an attractive approach for the design of new therapeutic agents for the treatment of type II diabetes and for new antitumoral drugs. To date very few (and weak) inhibitors of LMW-PTP have been identified. On the basis of the reported weak activity of some flavonoids on phosphatases, we discovered a lead that originated a new class of highly active LMW-PTP inhibitors; these compounds inhibit also PTP-1B and are active in cellular assays. Docking experiments and SAR highlighted the possible binding mode of these compounds to the enzyme, putting the background for the future optimization of their inhibitory activity and selectivity towards the closely related enzyme PTP-1B.
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