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Comparison of in vitro-cytotoxicity of kava as a function of cultivar, plant part and extraction solvent

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piper_methysticum_9 Preparations from kava (Piper methysticum) have been banned based on the suspicion of adverse liver effects. To date, no convincing proof has been given to substantiate the danger of a relevant toxicity.
We systematically tested kava extracts prepared with acetone or ethanol from two different cultivars, both used for kava extract production: Ava Laau from Samoa, a “noble kava”, and Palisi from Vanuatu, a “Tudei kava” (“two-day” lasting effect). We also tested the influence of aerial parts (stem peelings) on toxicity.

Methods: Extracts were prepared and characterized by the working group of Prof. Nahrstedt at the University of Münster (Germany). Kava plant material was obtained from cultivations. Extracts were tested in HepG2 and Hep3B liver cells, using the MTT test, the Rezasurin blue assay, quantification of LDH leakage and measurements of intracellular ATP and GSH contents.

Results: Only gradual differences in cytotoxicity were found. The sequence of toxicity for ethanolic extracts was roots (noble) < peelings (noble) ≤ roots (Tudei) < peelings (Tudei). In the case of extracts prepared with acetone the toxicity of the Tudei-material was partly reversed: peelings (Tudei) < roots (Tudei). In no case were the EC50 values in a relevant dosage range (1250 to >5000 µg/ml for roots, 800 to >5000 µg/ml for peelings in the MTT test and rezasurin blue assay, with the highest toxicity found with Tudei peelings in the rezasurin blue test in Hep 3B cells).

Conclusions: No hint on relevant liver cell toxicity was found in this battery of in vitro models.

Download: Comparison of in vitro-cytotoxicity of kava as a function of cultivar, plant part and extraction... (191.52 kB 2009-05-22 12:08:17).
Poster: 54rd Annual Congress of the Society for Medicinal Plant Research, Helsinki (Finland), August 28 - September 2, 2006

 

Last Updated ( Thursday, 11 June 2009 00:54 )  

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