Second generation benzofuranone ring substituted noscapine analogs: synthesis and biological evaluation.

Ram Chandra Mishra, Prasanthi Karna, Sushma Reddy Gundala, Vaishali Pannu, Richard A Stanton, Kamlesh Kumar Gupta, M Hope Robinson, Manu Lopus, Leslie Wilson, Maged Henary, Ritu Aneja

Department of Biology, Georgia State University, Atlanta, GA 30303, United States.

Journal Article: Biochemical pharmacology (impact factor: 4.25). 07/2011; 82(2):110-21. DOI: 10.1016/j.bcp.2011.03.029

Abstract

Microtubules, composed of α/β tubulin heterodimers, represent a validated target for cancer chemotherapy. Thus, tubulin- and microtubule-binding antimitotic drugs such as taxanes and vincas are widely employed for the chemotherapeutic management of various malignancies. Although quite successful in the clinic, these drugs are associated with severe toxicity and drug resistance problems. Noscapinoids represent an emerging class of microtubule-modulating anticancer agents based upon the parent molecule noscapine, a naturally occurring non-toxic cough-suppressant opium alkaloid. Here we report in silico molecular modeling, chemical synthesis and biological evaluation of novel analogs derived by modification at position-7 of the benzofuranone ring system of noscapine. The synthesized analogs were evaluated for their tubulin polymerization activity and their biological activity was examined by their antiproliferative potential using representative cancer cell lines from varying tissue-origin [A549 (lung), CEM (lymphoma), MIA PaCa-2 (pancreatic), MCF-7 (breast) and PC-3 (prostate)]. Cell-cycle studies were performed to explore their ability to halt the cell-cycle and induce subsequent apoptosis. The varying biological activity of these analogs that differ in the nature and bulk of substituent at position-7 was rationalized utilizing predictive in silico molecular modeling.

Source: PubMed

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Keywords

benzofuranone ring system
 
biological evaluation
 
chemotherapeutic management
 
drug resistance problems
 
emerging class
 
induce subsequent apoptosis
 
MIA PaCa-2
 
microtubule-binding antimitotic drugs
 
microtubule-modulating anticancer agents
 
novel analogs
 
occurring non-toxic cough-suppressant opium alkaloid
 
parent molecule noscapine
 
representative cancer cell lines
 
severe toxicity
 
silico molecular modeling
 
synthesized analogs
 
various malignancies
 
varying biological activity
 
varying tissue-origin [A549
 
α/β tubulin heterodimers