首页> 美国卫生研究院文献>Microorganisms >Pro-Inflammatory Effects of NX-3 Toxin Are Comparable to Deoxynivalenol and not Modulated by the Co-Occurring Pro-Oxidant Aurofusarin
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Pro-Inflammatory Effects of NX-3 Toxin Are Comparable to Deoxynivalenol and not Modulated by the Co-Occurring Pro-Oxidant Aurofusarin

机译:NX-3毒素的促炎作用与脱氧雪腐烯醇相当并且不受共氧化剂Aurofusarin的调节

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摘要

The type A trichothecene NX-3, produced by certain strains, is similar to the mycotoxin deoxynivalenol (DON), with the exception that it lacks the carbonyl moiety at the C-8 position. NX-3 inhibits protein biosynthesis and induces cytotoxicity to a similar extent as DON, but so far, immunomodulatory effects have not been assessed. In the present study, we investigated the impact of NX-3 on the activity of the nuclear factor kappa B (NF-κB) signaling pathway in direct comparison to DON. Under pro-inflammatory conditions (IL-1β treatment), the impact on cytokine mRNA levels of NF-κB downstream genes was studied in human colon cell lines, comparing noncancer (HCEC-1CT) and cancer cells (HT-29). In addition, potential combinatory effects with the co-occurring secondary metabolite aurofusarin (AURO), a dimeric naphthoquinone known to induce oxidative stress, were investigated. NX-3 and DON (1 μM, 20 h) significantly activated a NF-κB regulated reporter gene to a similar extent. Both trichothecenes also enhanced transcript levels of the known NF-κB-dependent pro-inflammatory cytokines IL-8, IL-6, TNF-α and IL-1β. Comparing the colon cancer HT-29 and noncancer HCEC-1CT cells, significant differences in cytokine signaling were identified. In contrast, AURO did not affect NF-κB pathway activity and respective cytokine expression levels at the tested concentration. Despite its pro-oxidant potency, the combination with AURO did not significantly affect the immunomodulatory effects of the tested trichothecenes. Taken together, the present study reveals comparable potency of DON and NX-3 with respect to immunomodulatory and pro-inflammatory potential. Consequently, not only DON but also NX-3 should be considered as factors contributing to intestinal inflammatory processes.
机译:由某些菌株产生的A型单端孢霉菌NX-3与霉菌毒素脱氧雪腐烯醇(DON)相似,不同之处在于它在C-8位置缺少羰基部分。 NX-3抑制蛋白质的生物合成并诱导与DON相似的细胞毒性,但到目前为止,尚未评估其免疫调节作用。在本研究中,我们直接与DON进行了比较,研究了NX-3对核因子kappa B(NF-κB)信号通路活性的影响。在促炎条件下(IL-1β处理),在人结肠细胞系中研究了NF-κB下游基因对细胞因子mRNA水平的影响,比较了非癌(HCEC-1CT)和癌细胞(HT-29)。此外,还研究了与同时发生的次级代谢物aurofusarin(AURO)(一种已知会诱导氧化应激的二聚萘醌)的潜在组合作用。 NX-3和DON(1μM,20小时)以相似的程度显着激活了NF-κB调控的报告基因。两种单端孢菌烯还增强了已知的NF-κB依赖性炎性细胞因子IL-8,IL-6,TNF-α和IL-1β的转录水平。比较结肠癌HT-29细胞和非癌HCEC-1CT细胞,可以确定细胞因子信号传导的显着差异。相反,在测试浓度下,AURO不会影响NF-κB通路活性和相应的细胞因子表达水平。尽管具有促氧化剂作用,但与AURO的组合并没有显着影响所测试的单端孢菌毒素的免疫调节作用。综上所述,本研究揭示了DON和NX-3在免疫调节和促炎潜力方面具有可比性。因此,不仅DON,而且NX-3也应被认为是导致肠道炎症过程的因素。

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