ISSN: 2320-480X
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The Journal of Phytopharmacology, 2021;10(1):48-55 ;   DOI:10.31254/phyto.2021.10110

Review Article

Synthesis, Isolation, and Biological Evaluation of a New Active Quinone Methide Derived Curcuminoid

Tomer Sinai1 , Brijesh Singh2 , Amnon C Sintov1 , Shimon Ben-Shabat2

1. Department of Biomedical Engineering, Ben Gurion University of the Negev, Be’er Sheva, Israel
2. Department of Biochemistry and Pharmacology, Ben Gurion University of the Negev, Be’er Sheva, Israel

*Author to whom correspondence should be addressed.

Received: 25th November, 2020 / Accepted: 15th January, 2021

Abstract


A new curcuminoid, quinone methide cyclopentadione (QMC), was synthesized by oxidation of curcumin (CUR) in the presence of potassium ferricyanide, and further isolated and analyzed. QMC was found to be a relatively water-soluble curcuminoid, and more stable than CUR in citric-phosphate buffer solutions. Unlike CUR, QMC possesses a pH-independent stability. In plasma, QMC was degraded by 50% after 8 hours and reached 30% of its initial concentration after 48h, while CUR was thoroughly decomposed. It has been demonstrated that QMC has a similar anti-proliferative activity as CUR in three different cancer cell lines- MCF-7, PC3 and HT29. Molecular examination of QMC in cancer cells exhibited similar effect to CUR on two transcription factors, Nrf-2 and NF-?B. An anti-inflammatory activity of QMC was demonstrated by measuring MCP-1 secretion levels in TNF?-induced human keratinocytes cell culture, which had been pre-treated with either CUR or QMC. This report presents the advantages of the new quinone methide derived curcuminoid and its pharmaceutical potential as an alternative to the poorly soluble curcumin.

Keywords

Curcumin; Quinone methide cyclopentadione; Cell proliferation; Anti-inflammatory activity; Oxidation.


HOW TO CITE THIS ARTICLE

Sinai T, Singh B, Sintov AC, Shabat SB. Synthesis, Isolation, and Biological Evaluation of a New Active Quinone Methide Derived Curcuminoid. J Phytopharmacol 2021; 10(1):48-55.

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