Neha Upadhyay, Kalpana Tilekar, Piotr Mrowka, Pramodkumar Gupta3, Virupaksha A Bastikar, Kaustubh Wagle and C S Ramaa
Bharati Vidyapeeth�s College of Pharmacy, India
Medical University of Warsaw, Poland
D Y Patil University, India
Amity University, India
Scientific Tracks Abstracts: Med chem (Los Angeles)
Introduction: Contribution of antidiabetic Thiazolidinediones (TZDs) to cancer therapy has been evidenced by numerous in-vitro and in-vivo studies. While TZDs are known to stimulate PPAR-�³ receptor, they also have multiple PPAR�³ independent effects and the specific role of PPAR�³ activation in the anticancer effects of TZDs is still under investigation. Also, several reports show the correlation between full activation of PPAR�³ and associated adverse effects. This prompted us to develop TZD analogues as partial PPAR�³ agonists and evaluate their anticancer potential. Methods: We designed series of novel TZDs based on, QSAR model, Docking analysis and Molecular properties study. Further we synthesized and structurally characterized them by 1H-NMR, 13C-NMR, FTIR and Mass spectroscopy. Results & Discussion: In the present work, a QSAR model was developed and validated using 25 TZD derivatives synthesized in our laboratory earlier, showing antiproliferative activity against K 562 cell lines, by using experimental and computational study and analysis. The predicted activities by our QSAR models were very close to those experimentally observed, indicating that these models can be safely applied for prediction of more effective hits having the same skeletal framework. We used this model to design new series of 5-naphthylidene-2,4- TZDs and predicted their antiproliferative activity. The molecules from the series, obeying Lipinskiâ��s rule of five were subjected to docking analysis using VLife protocol. The molecules displaying desired interactions as that of partial agonists of PPAR�³ were further taken for synthesis and evaluated for primary cytotoxic effects on several cancerous cell lines.
Neha Upadhyay has completed her Post-graduation in Pharmaceutical Chemistry from Bombay College of Pharmacy, Mumbai. She is working as a Junior Research Fellow (JRF) on a project funded by DST, India. She has registered for PhD in Pharmaceutical Sciences at Bharati Vidyapeeth’s College of Pharmacy, Navi Mumbai, India.
E-mail: upadhyayneha16@gmail.com
Medicinal Chemistry received 6627 citations as per Google Scholar report
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