Abstract

Three scarce terpenes, psiadin, plectranthone and saudinolide, were obtained after chromatographic isolation and purification from the aerial parts of the respective plants. Their identities were established based on their spectral data. Their anticancer effects against two human colorectal carcinoma cell lines, CCL233 and CCL235, along with the potential molecular mechanisms of action, were explored. Psiadin and plectranthone exhibited marked growth inhibition on both cell lines in a time- and dose-dependent manner with minimal cytotoxicity against normal breast cells (HB2). The terpenes even showed superior activities to the tested standards. Flow cytometry showed apoptosis induction and alteration in the cell cycle in colorectal cancer cells treated with both compounds. Nevertheless, it was also found that both compounds inhibited NF-κB transcriptional activity, induced mitochondrial membrane potential depolarization and increased the percentage of reactive oxygen species in the treated cancer cells in a dose-dependent manner as well. Since the anticancer effect of psiadin on cancer cells was higher than that produced by plectranthone, only psiadin was tested to determine its possible targets. The results suggested a high degree of specificity of action affecting particular cellular processes in both cancer cells. In conclusion, both terpenes, in particular psiadin, showed significant discriminative therapeutic potential between cancer and normal cells, a value that is missing in current chemotherapies.

Highlights

  • Cancer is a huge health burden affecting almost every region worldwide, with estimations of 28 million new cases and a predicted 16 million cancer deaths by 2040 [1]

  • We report the chromatographic isolation and spectral identification of these three terpenes and the determination of their anticancer effects on two human colorectal carcinoma cell lines

  • The need for new anticancer agents has prompted the search for such agents from natural resources

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Summary

Introduction

Cancer is a huge health burden affecting almost every region worldwide, with estimations of 28 million new cases and a predicted 16 million cancer deaths by 2040 [1]. Colorectal cancer is the second most common cancer in women and the third in men, and accounts for about 9% of all cancer deaths [1]. Psiadin and plectranthone selectively inhibit colorectal carcinoma cells proliferation

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