Antimelanoma activities of chimeric thiazole–androstenone derivatives

Author:

Chambers Steven A.1,Newman Mathew1,Frangie Melissa M.1,Savenka Alena V.2,Basnakian Alexei. G.2,Alam Mohammad A.1ORCID

Affiliation:

1. Department of Chemistry and Physics, College of Science and Mathematics, Arkansas State University, Jonesboro, AR 72467, USA

2. Department of Pharmacology and Toxicology, University of Arkansas for Medical Sciences, and Central Arkansas Veterans Healthcare System, Little Rock, AR 72205, USA

Abstract

The discovery of chimeric anti-melanoma agents is reported. These molecules are potent growth suppressors of melanoma cells in vitro with growth inhibition of 50% (GI 50 ) values as low as 1.32 µM. Compounds were more toxic to melanoma cells in vitro than commonly used anti-melanoma agent dacarbazine as measured by TUNEL assay. They induced both caspase-independent apoptosis evident by colocalization of TUNEL with endonuclease G (EndoG) and caspase-mediated apoptosis measured by colocalization of TUNEL with caspase-activated DNase (CAD). In addition, compounds 3 and 5 strongly induced oxidative injury to melanoma cells as measured by TUNEL colocalization with heme oxygenase-1 (HO1). Dacarbazine induced only caspase-independent apoptosis, which may explain why it is less cytotoxic to melanoma cells than compounds 3 , 4 and 5 .

Funder

Arkansas INBRE program

Cancer Institute at the University of Arkansas for Medical Sciences

NCI

National Institute of General Medical Sciences (NIGMS), National Institutes of Health

NIH

Winthrop

ABI

Publisher

The Royal Society

Subject

Multidisciplinary

Reference27 articles.

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3. NCI. 2016 Melanoma Skin Cancer. See http://www.cancer.org/cancer/skincancer-melanoma/detailedguide/melanoma-skin-cancer-key-statistics.

4. Synthesis and Biological Evaluation of New Quinoxaline Derivatives of ICF01012 as Melanoma-Targeting Probes

5. Thiazole-containing compounds as therapeutic targets for cancer therapy

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