Development of a novel nitro-derivative of noscapine for the potential treatment of drug-resistant ovarian cancer and T-cell lymphoma.

Ritu Aneja, Surya N Vangapandu, Manu Lopus, Ramesh Chandra, Dulal Panda, Harish C Joshi

Department of Cell Biology, Emory University School of Medicine, Laboratory for Drug Discovery and Research, 615 Michael St., Atlanta, GA 30322, USA.

Journal Article: Molecular Pharmacology (impact factor: 4.53). 07/2006; 69(6):1801-9. DOI: 10.1124/mol.105.021899

Abstract

We have shown previously that an antitussive plant alkaloid, noscapine, binds tubulin, displays anticancer activity, and has a safe pharmacological profile in humans. Structure-function analyses pointed to a proton at position-9 of the isoquinoline ring that can be modified without compromising tubulin binding activity. Thus, many noscapine analogs with different functional moieties at position-9 were synthesized. Those analogs that kill human cancer cells resistant to other antimicrotubule agents, vincas and taxanes, were screened. Here, we present one such analog, 9-nitro-noscapine (9-nitro-nos), which binds tubulin and induces apoptosis selectively in tumor cells (ovarian and T-cell lymphoma) resistant to paclitaxel, vinblastine, and teniposide. 9-Nitro-nos treatment at doses as high as 100 microM did not affect the cell cycle profile of normal human fibroblasts. This selectivity of 9-nitro-nos for cancer cells represents a unique edge over the other available antimitotics. 9-Nitro-nos perturbs the progression of cell cycle by mitotic arrest, followed by apoptotic cell death associated with increased caspase-3 activation and appearance of terminal deoxynucleotidyl transferase dUTP nick-end labeling-positive cells. Thus, we conclude that 9-nitro-nos has great potential to be a novel therapeutic agent for ovarian and T-cell lymphoma cancers, even those that have become drug-resistant to currently available chemotherapeutic drugs.

Source: PubMed

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Keywords

9-nitro-noscapine
 
antitussive plant alkaloid
 
apoptotic cell death
 
available chemotherapeutic drugs
 
cancer cells
 
caspase-3 activation
 
cell cycle profile
 
different functional moieties
 
displays anticancer activity
 
induces apoptosis
 
kill human cancer cells resistant
 
normal human fibroblasts
 
noscapine analogs
 
novel therapeutic agent
 
safe pharmacological profile
 
Structure-function analyses
 
T-cell lymphoma cancers
 
terminal deoxynucleotidyl transferase dUTP nick-end labeling-positive cells
 
tubulin binding activity
 
tumor cells