| Literature DB >> 30220013 |
Prasad G Mahajan1, Nilam C Dige2, Balasaheb D Vanjare1, Hussain Raza3, Mubashir Hassan3, Sung-Yum Seo3, Seong-Karp Hong4, Ki Hwan Lee5.
Abstract
Herein, we design and synthesized new fluorescein based derivatives by insitu formation of fluorescein ester and further treated with corresponding hydrazide and amine to yield respective compounds i.e. FB1, FB2, FB3 and FB4. The spectral purity and characterization was done by using IR, NMR and Mass spectroscopies. The synthesized derivatives were examined for their photophysical properties by using variety of organic solvents and results were discussed in details. The structural diversity of synthesized compounds motivate us to evaluate these compounds for urease inhibition. The compound FB3 (IC50 = 0.0456 μM) shows 100 fold more active against Jack bean urease than standard drug thiourea (IC50 = 4.7455 μM). Other synthesized compounds showed potent activity. Free radical percentage scavenging assay further supported the capacity of compounds to urease inhibition. While, molecular docking simulations helps to examine the molecular interactions of active compounds FB1, FB2, FB3 and FB4 within the binding site of urease enzyme.Entities:
Keywords: Fluorescein derivatives; Molecular docking; Optical properties; Synthesis; Urease inhibitors
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Year: 2018 PMID: 30220013 DOI: 10.1007/s10895-018-2291-7
Source DB: PubMed Journal: J Fluoresc ISSN: 1053-0509 Impact factor: 2.217