Since the LPS stimulated

Since the LPS stimulated selleck chemicals Gemcitabine THP 1 cell system is one of the most widely used models for macrophage activation, our findings on the differential effects of var ious phytocompounds on anti inflammatory activities may thus have a general application. In this study, we have used THP 1 cells that were not treated with LPS as an internal control. It is important to note here that the response of THP 1 to LPS obtained in the present study is in good agreement with various reports from previous studies. We then compared data obtained in the set from treatment with LPS only with the vehicle control set and further analyzed the gene expression patterns and the possible signaling pathways or potential interactions involved.

The study was hence designed as a pharmacogenomics approach for evaluation and classification of various anti inflam matory natural products, mainly phytochemicals with reputed medicinal bioactivities, into potentially clinically relevant or applicable subgroups. Shikonin and emodin resulted in significant inhibition of most of the inflamma tion responsive genes as early as 0. 5 h after treatment. Shikonin has previously been shown to exhibit anti inflammatory activity, and here we also observed shikonin suppression of the expression of a number of immune related genes, including TNF a, IL 1b and CCL4 genes. This suggests that shikonin can inhibit a group of genes that are associated with macro phage activation at the very early stage of inflammatory response. Following emodin treatment, approximately 30 genes were significantly down regulated even after 48 h.

However, there was less emodin inhibition of some chemotactic and cell migration gene expression, such as CCBP2 and CCL4 compared to shikonin. This suggests that emodin might down regulate inflammatory cytokines rather than immune cell recruit ment and cell migration. Recently, emodin has been shown to exert an anti inflammatory effect by inhibiting NF B activation and inflammatory cytokine expression. We suggest that both shikonin and emodin may strongly inhibit macrophage activation, but that chemo taxis and the recruitment of T lymphocytes are less affected by emodin. Further experiments are necessary to confirm this possibility. We analyzed possible signaling pathways and modula Anacetrapib tors using key node analysis of those genes significantly inhibited by shikonin and emodin treatments in LPS induced THP 1 cells at the 0. 5 h time point. The pattern of down regulated gene expression seen with shikonin at 0. 5 h suggested an increase in expression of Rad23A, which binds and delivers ubiquitinated proteins to the protea some, and subsequent inactivation of the p 300, tran scriptional co activator protein.

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