gov/home jsp) where the Functional Annotation Clustering tool was

gov/home.jsp) where the Functional Annotation Clustering tool was applied to generate clusters of overrepresented Gene Ontology (GO) terms (Huang et al., 2009). The data were Smad inhibitor analyzed in GraphPad Prism 5.00® software (GraphPad Software, Inc., San Diego, CA) using one-way analysis of variance (ANOVA) followed by Dunnett’s test for multiple comparisons or Student’s t-tests to compare two groups. Non-parametric data were compared using the Kruskal–Wallis test followed by Dunn’s test, and percent data from two groups were compared using the Mann–Whitney test. Data are expressed as the mean ± SD,

or as the median with range, and differences were considered statistically significant at p < 0.05. We performed transcriptome analysis on isolated splenic NK cells from 20 mice (5 mice/group) that were treated daily by gavage

for 14 days with ptaquiloside and/or selenium to identify transcripts that were associated with ptaquiloside-induced immunosuppression. The gene expression profiles from the Pt, PtSe and Se experimental groups, compared with the control group, showed 872, 302 and 489 altered genes, RGFP966 supplier respectively (Table 1). Of the up-regulated gene transcripts from all experimental groups, 123 were mapped to biological processes, from which we highlighted five, although, as shown in Fig. 2, none had high enrichment scores (≥1.3). The Pt and Se groups showed a very different pattern of distribution of differentially expressed genes in these 5 biological processes, whereas no particular biological process was favored in the PtSe group. The corresponding genes for each enriched GO term are listed in Table 2 and in Supplementary Table 1. When considering

gene transcripts that could be related to the immunosuppressive effects of ptaquiloside, we did not find genes directly related to this effect, but selected the genes metallothionein all 1 (Mt1) and metallothionein 2 (Mt2), which are involved in cellular ion homeostasis and act as zinc regulator that is essential to normal immune function. Ptaquiloside treatment increased the expression of these gene transcripts 2.9-fold (p < 0.001758) and 3.0-fold (p < 0.025148) compared with the control group, respectively. Supplementary Table S1.   The GO terms are over-represented among the genes whose expression was up regulated in the experimental groups vs. the control group. Each category biological process (GOTERM_BP_FAT) is represented by at least 3 genes. Of the down-regulated gene transcripts, 1174 were mapped to a wide range of biological processes. Transcripts with enrichment scores ≥1.3 for at least one of these groups are presented in Fig. 3. These data showed no specific biological process that was associated with ptaquiloside-induced immunosuppression in NK cells. The corresponding genes for each enriched GO term are listed in Supplementary Table 2. Supplementary Table S2.   The GO terms are over-represented among the genes whose expression was up regulated in the experimental groups vs. the control group.

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