Insights into the inhibitory mechanism of triazole-based small molecules on phosphatidylinositol-4,5-bisphosphate binding pleckstrin homology domain |
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| Authors: | Sukhamoy Gorai Prasanta Ray Bagdi Rituparna Borah Debasish Paul Manas Kumar Santra Abu Taleb Khan Debasis Manna |
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| Institution: | 1. Department of Chemistry, Indian Institute of Technology Guwahati, Assam 781039, India;2. National Center for Cell Science, Pune 411007, Maharashtra, India;3. Alia University, DN 18, 8th Floor, Sector V, Kolkata 700091, India |
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| Abstract: | BackgroundPhosphatidylinositol 4,5-bisphosphate PI(4,5)P2] is an important regulator of several cellular processes and a precursor for other second messengers which are involved in cell signaling pathways. Signaling proteins preferably interact with PI(4,5)P2 through its pleckstrin homology (PH) domain. Efforts are underway to design small molecule-based antagonist, which can specifically inhibit the PI(4,5)P2/PH-domain interaction to establish an alternate strategy for the development of drug(s) for phosphoinositide signaling pathways.MethodsSurface plasmon resonance, molecular docking, circular dichroism, competitive Förster resonance energy transfer, isothermal titration calorimetric analyses and liposome pull down assay were used.ResultsIn this study, we employed 1,2,3-triazol-4-yl methanol containing small molecule (CIPs) as antagonists for PI(4,5)P2/PH-domain interaction and determined their inhibitory effect by using competitive-surface plasmon resonance analysis (IC50 ranges from 53 to 159 nM for PI(4,5)P2/PLCδ1-PH domain binding assay). We also used phosphatidylinositol 3,4,5-trisphosphate PI(3,4,5)P3], phosphatidylinositol 3,4-bisphosphate PI(3,4)P2], PI(4,5)P2 specific PH-domains to determine binding selectivity of the compounds. Various physicochemical analyses showed that the compounds have weak affect on fluidity of the model membrane but, strongly interact with the phospholipase C δ1 (PLCδ1)-PH domains. The 1,2,3-triazol-4-yl methanol moiety and nitro group of the compounds are essential for their exothermic interaction with the PH-domains. Potent compound can efficiently displace PLCδ1-PH domain from plasma membrane to cytosol in A549 cells.ConclusionsOverall, our studies demonstrate that these compounds interact with the PIP-binding PH-domains and inhibit their membrane recruitment.General significanceThese results suggest specific but differential binding of these compounds to the PLCδ1-PH domain and emphasize the role of their structural differences in binding parameters. These triazole-based compounds could be directly used/further developed as potential inhibitor for PH domain-dependent enzyme activity. |
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| Keywords: | Pleckstrin homology domains Phosphatidylinositols 1 2 3-Triazol-4-yl methanol substituent Inhibition of protein–lipid interactions Surface plasmon resonance-based competitive binding assay Cellular displacement assay |
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