A New Rare Halogenated Depside from Lichen and Study of its Anti‐Proliferative Activity

Author:

Bauri Ajoy K.1ORCID,Dionicio Ines Castro2ORCID,Arellano Eric Salinas2ORCID,Jeyaraj Jonathan G.2,Foro Sabine3ORCID,Carcache de Blanco Esperanza J.2ORCID

Affiliation:

1. Bio-Organic Division Bhabha Atomic Research Centre, Trombay Mumbai 400085 India

2. College of Pharmacy The Ohio State University Ohio Columbus OH-43210 USA

3. Institute of Materials Science Darmstadt University of Technology Alarich-Weiss-Strasse 2 D-64287 Darmstadt Germany

Abstract

AbstractLichens are a symbiotic association of algae and fungus, belonging to the family Parmeliaceae. Some lichen species are edible and used as an active ingredient for preparation of exotic spices as well as folklore medicine to cure different kinds of ailments. A specimen of lichen was collected from Munner in the Kerala State of South India for chemical profiling. Chemical analyses of the diethyl ether extract of the defatted lichen led to the isolation of six phenols 16 with variation of relative abundance. Amongst them, the relative abundance of compound 3 was the greatest (1 % of crude extract) and it was identified as atranorin. The structures of known compounds were confirmed by comparison of their 1H‐NMR, 13C NMR, and mass data with published values available in the literature. In vitro bioassay for anti‐proliferative activity of these compounds has been conducted against various human cancer cell lines in comparison with paclitaxel as control using SRB assay. Interestingly, a new compound 5 was found along with previously reported compounds from this lichen. This new compound was designated as fluoroatranorin 5 which was reported for the first time herein. The structural characterization of a new depside was determined by spectral methods such as 1H‐NMR, 13C NMR, 19F NMR, IR, LC‐HRESI‐MS, and LC–MS/MS study. Its structure was confirmed by single crystal X‐ray diffraction study. This new compound was designated as fluoroatranorin 5 which was reported first time herein. Anti‐proliferative activity of all these compounds was evaluated against six different cancer cell lines. The inhibitory activity, IC50 value of compounds 13 and 5 exhibited at 99.64, 102.04, 109.20, 53.0 and 2.4 μM on cancer cell lines HT‐29 (colon), Hela (cervical), HT‐29, HPAC (pancreas) and A2780 (ovarian cancer cell line) respectively in comparison with paclitaxel as control. The new compound 5 exhibited significant activity with IC50 value 2.4 μM on A2780 ovarian cancer cell line.

Publisher

Wiley

Reference60 articles.

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2. Vertical Distribution of Lichens on the Mountain, Aucellabjerg, Northeastern Greenland

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