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Differential Effects of Oral Exposure to Naturally-Occurring and Synthetic Deoxynivalenol Congeners on Proinflammatory Cytokine and Chemokine mRNA Expression in the Mouse

机译:口服天然和合成的脱氧雪腐酚同源物对小鼠促炎细胞因子和趋化因子mRNA表达的影响

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摘要

The foodborne mycotoxin deoxynivalenol (DON) induces a ribotoxic stress response in mononuclear phagocytes that mediate aberrant multi-organ upregulation of TNF-α, interleukins and chemokines in experimental animals. While other DON congeners also exist as food contaminants or pharmacologically-active derivatives, it is not known how these compounds affect expression of these cytokine genes in vivo. To address this gap, we compared in mice the acute effects of oral DON exposure to that of seven relevant congeners on splenic expression of representative cytokine mRNAs after 2 and 6 h. Congeners included the 8-ketotrichothecenes 3-acetyldeoxynivalenol (3-ADON), 15-acetyldeoxynivalenol (15-ADON), fusarenon X (FX), nivalenol (NIV), the plant metabolite DON-3-glucoside (D3G) and two synthetic DON derivatives with novel satiety-inducing properties ( and ). DON markedly induced transient upregulation of TNF-α IL-1β, IL-6, CXCL-2, CCL-2 and CCL-7 mRNA expression. The two ADONs also evoked mRNA expression of these genes but to a relatively lesser extent. FX induced more persistent responses than the other DON congeners and, compared to DON, was: 1) more potent in inducing IL-1β mRNA, 2) approximately equipotent in the induction of TNF-α and CCL-2 mRNAs, and 3) less potent at upregulating IL-6, CXCL-2, and CCL-2 mRNAs. ’s effects were similar to NIV, the least potent 8-ketotrichothecene, while D3G and were largely incapable of eliciting cytokine or chemokine mRNA responses. Taken together, the results presented herein provide important new insights into the potential of naturally-occurring and synthetic DON congeners to elicit aberrant mRNA upregulation of cytokines associated with acute and chronic trichothecene toxicity.
机译:食源性霉菌毒素脱氧雪腐酚(DON)在单核吞噬细胞中诱导核糖毒性应激反应,介导实验动物中TNF-α,白介素和趋化因子的异常多器官上调。尽管其他DON同系物也以食物污染物或药理活性衍生物形式存在,但尚不知道这些化合物如何影响这些细胞因子基因在体内的表达。为了解决这个差距,我们在小鼠中比较了口服DON与7种相关同源物对2小时和6小时后代表性细胞因子mRNA脾表达的急性影响。同类物包括8-酮三丁醚3-乙酰基脱氧雪茄烯醇(3-ADON),15-乙酰基脱氧雪茄烯醇(15-ADON),富沙隆X(FX),nivalenol(NIV),植物代谢物DON-3-葡萄糖苷(D3G)和两个合成的DON具有新颖的饱腹感特性(和)的衍生物。 DON明显诱导TNF-αIL-1β,IL-6,CXCL-2,CCL-2和CCL-7 mRNA表达的瞬时上调。这两个ADON也引起这些基因的mRNA表达,但是程度相对较小。与DON相比,FX诱导的持久性反应更高,并且与DON相比,具有以下优势:1)诱导IL-1βmRNA的能力更强; 2)TNF-α和CCL-2 mRNA的诱导能力大致相同,以及3)更少在上调IL-6,CXCL-2和CCL-2 mRNA方面很有效。其作用类似于NIV,即效力最弱的8-ketotrichothececene,而D3G则几乎无法引起细胞因子或趋化因子mRNA反应。两者合计,本文呈现的结果提供了重要的新见解,揭示了天然和合成的DON同源物引发与急性和慢性天花粉毒性相关的细胞因子的异常mRNA上调的潜力。

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