Novel heteroaryl phosphonicdiamides PTPs inhibitors as anti-hyperglycemic agents |
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| Authors: | Kuruva Chandra Sekhar Rasheed Syed Madhava Golla Jyothi Kumar MV Nanda Kumar Yellapu Appa Rao Chippada Naga Raju Chamarthi |
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| Affiliation: | .Department of Chemistry, Sri Venkateswara University, Tirupati, 517 502 India ;.Department of Biotechnology, Sri Venkateswara University, Tirupati, 517 502 India ;.Biomedical informatics Center, Vector Control Research Centre, Indian Council of Medical Research, Puducherry, 605006 India ;.Department of Biochemistry, Sri Venkateswara University, Tirupati, 517 502 India |
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| Abstract: | BackgroundChronic and oral administration of benzylamine improves glucose tolerance. Picolylamine is a selective functional antagonist of the human adenosine A2B receptor. Phosphonic diamide derivatives enhance the cellular permeability and in turn their biological activities.MethodsA series of heteroaryl phosphonicdiamide derivatives were designed as therapeutics to control and manage type2 diabetes. Initially defined Lipinski parameters encouraged them as safer drugs. Molecular docking of these compounds against Protein tyrosine phosphatase (PTP), the potential therapeutic target of type 2 diabetes, revealed their potential binding ability explaining their anti-diabetic activity in terms of PTP inhibition. Human intestinal absorption, Caco-2 cell permeability, MDCK cell permeability, BBB penetration, skin permeability and plasma protein binding abilities of the title compounds were calculated by PreADMET server. A convenient method has been developed for the synthesis of title compounds through the formation of 1-ethoxy-N,N’-bis(4-fluorobenzyl/pyridin-3-ylmethyl)phosphinediamine by the reaction of 4-fluorobenzylamine/ 3-picolylamine with ethyldichlorophosphite, subsequently reacted with heteroaryl halides using lanthanum(III) chloride as a catalyst.ResultsAll the compounds exhibited significant in vitro anti-oxidant activity and in vivo evaluation in streptozotocin induced diabetic rat models revealed that the normal glycemic levels were observed on 12th day by 9a and 20th day by 5b, 5c, 9e and 9f. The remaining compounds also exhibited normal glycemic levels by 25th day.ConclusionThe results from molecular modeling, in vitro and in vivo studies are suggesting them as safer and effective therapeutic agents against type2 diabetes.Graphical AbstractOpen in a separate windowDevelopment of PTPs inhibitors.Electronic supplementary materialThe online version of this article (doi:10.1186/s40199-014-0076-3) contains supplementary material, which is available to authorized users. |
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