Abstract
Echinacea preparations, which are used for the prevention and treatment of upper respiratory infections, account for 10% of the dietary supplement market in the U.S., with sales totaling more than $100 million annually. In an attempt to shed light on Echinacea's mechanism of action, we evaluated the effects of a 75% ethanolic root extract of Echinacea purpurea, prepared in accord with industry methods, on cytokine and chemokine production from RAW 264.7 macrophage-like cells. We found that the extract displayed dual activities; the extract could itself stimulate production of the cytokine TNF-α, and also suppress production of TNF-α in response to stimulation with exogenous LPS. Liquid:liquid partitioning followed by normal-phase flash chromatography resulted in separation of the stimulatory and inhibitory activities into different fractions, confirming the complex nature of this extract. We also studied the role of alkylamides in the suppressive activity of this E. purpurea extract. Our fractionation method concentrated the alkylamides into a single fraction, which suppressed production of TNF-α, CCL3, and CCL5; however fractions that did not contain detectable alkylamides also displayed similar suppressive effects. Alkylamides, therefore, likely contribute to the suppressive activity of the extract but are not solely responsible for that activity. From the fractions without detectable alkylamides, we purified xanthienopyran, a compound not previously known to be a constituent of the Echinacea genus. Xanthienopyran suppressed production of TNF-α suggesting that it may contribute to the suppressive activity of the crude ethanolic extract. Finally, we show that ethanolic extracts prepared from E. purpurea plants grown under sterile conditions and from sterilized seeds, do not contain LPS and do not stimulate macrophage production of TNF-α, supporting the hypothesis that the macrophage-stimulating activity in E. purpurea extracts can originate from endophytic bacteria. Together, our findings indicate that ethanolic E. purpurea extracts contain multiple constituents that differentially regulate cytokine production by macrophages.
Highlights
Echinacea is the third most popular herbal medicine in the US, with annual sales of over $100 million [1]
In a study where we examined 17 E. purpurea root extracts, from plants grown on different farms, we found that despite high alkylamide levels, only a few suppressed production of the mediators PGE2 and TNF-α from RAW 264.7 cells stimulated with influenza A strain PR/8/34 [8]
TNF-αas was selected because it is a key inflammatory cytokine whose overproduction has been linked to several chronic and acute inflammatory disorders such as inflammatory bowel disease [22], psoriasis [23], and rheumatoid arthritis [24]
Summary
Echinacea is the third most popular herbal medicine in the US, with annual sales of over $100 million [1]. Barrett et al [4] failed to find an effect when Echinacea was used for several days to treat colds once symptoms had emerged. A confounding factor in interpreting the results of clinical trials is the complexity and variability of Echinacea products tested. Echinacea preparations used in clinical trials have been extracted from different species, different portions of the plant (containing different constituents), and by different processes. In the studies cited above, Jawad et al [3] used a commercial preparation referred to as “Echinaforce”, an ethanol extract of leaves (95%) and roots (5%) of E. purpurea, while the study conducted by Barrett et al [4] utilized roots from E. purpurea and E. angustifolia, that were ground whole and dispensed in pill form. There is currently a lack of knowledge regarding how to prepare Echinacea extracts with specific, desirable biological activities, and which constituents serve as appropriate biomarkers of these activities
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