Structure based virtual screening of anticanerous polyphenolic phytocompounds against G-protein coupled receptor and identification of potent antagonist ligand(s) through molecular docking

Daisy Pitchai; Rajalakshmi Manikkam; Sr Lilly V; Revathi Singaram

doi:10.6026/97320630006226

Structure based virtual screening of anticanerous polyphenolic phytocompounds against G-protein coupled receptor and identification of potent antagonist ligand(s) through molecular docking

Bioinformation. 2011;6(6):226-8. doi: 10.6026/97320630006226. Epub 2011 Jun 6.

Authors

Daisy Pitchai¹, Rajalakshmi Manikkam, Sr Lilly V, Revathi Singaram

Affiliation

¹ PG & Research Department of Biotechnology & Bioinformatics, Holy Cross College, Tiruchirappalli, India.

Abstract

Design of potential drug-like candidates for cancer is of interest in recent years. We used 60 compounds which are known to have the potential to down regulate Nuclear Factor kappaB (NFκB) for this study. The compounds were assessed for Lipinski's RO5 and ADMET properties. Allixin, anethole, capsaicin, linearol and syringic acid satisfied both Lipinski's RO5 and ADMET properties. These compounds showed strong molecular interaction with receptor GPCR55 indicating they have ability to block GPCR55. Thus, their role in anticellular proliferation and induction of apoptosis is implied.

Keywords: ADMET properties; Cancer; GPCR55; Lipinski's RO5; NFκB; anticellular proliferation; apoptosis; polyphenolic phytocompounds.