Institute of Life Sciences, Chongqing Medical University, Chongqing, 400032, The People's Republic of China.
Tianjin Institute of Industrial Biotechnology, Chinese Academy of Sciences, Tianjin, 300308, The People's Republic of China.
Microbiome. 2022 Dec 19;10(1):234. doi: 10.1186/s40168-022-01397-7.
Exposure to zearalenone (ZEN, a widespread Fusarium mycotoxin) causes reproductive toxicity and immunotoxicity in farm animals, and it then poses potential threats to human health through the food chain. A systematic understanding of underlying mechanisms on mycotoxin-induced toxicity is necessary for overcoming potential threats to farm animals and humans. The gastrointestinal tract is a first-line defense against harmful mycotoxins; however, it remains unknown whether mycotoxin (e.g., ZEN)-induced toxicity on the reproductive-immune axis is linked to altered gut microbial metabolites. In this study, using pigs (during the three phases) as an important large animal model, we investigated whether ZEN-induced toxicity on immune defense in the reproductive-immune axis was involved in altered gut microbial-derived metabolites. Moreover, we observed whether the regulation of gut microbial-derived metabolites through engineering ZEN-degrading enzymes counteracted ZEN-induced toxicity on the gut-reproductive-immune axis.
Here, we showed ZEN exposure impaired immune defense in the reproductive-immune axis of pigs during phase 1/2. This impairment was accompanied by altered gut microbial-derived metabolites [e.g., decreased butyrate production, and increased lipopolysaccharides (LPS) production]. Reduction of butyrate production impaired the intestinal barrier via a GPR109A-dependent manner, and together with increased LPS in plasma then aggravated the systemic inflammation, thus directly and/or indirectly disturbing immune defense in the reproductive-immune axis. To validate these findings, we further generated recombinant Bacillus subtilis 168-expressing ZEN-degrading enzyme ZLHY-6 (the Bs-Z6 strain) as a tool to test the feasibility of enzymatic removal of ZEN from mycotoxin-contaminated food. Notably, modified gut microbial metabolites (e.g., butyrate, LPS) through the recombinant Bs-Z6 strain counteracted ZEN-induced toxicity on the intestinal barrier, thus enhancing immune defense in the reproductive-immune axis of pigs during phase-3. Also, butyrate supplementation restored ZEN-induced abnormalities in the porcine small intestinal epithelial cell.
Altogether, these results highlight the role of gut microbial-derived metabolites in ZEN-induced toxicity on the gut-reproductive-immune axis. Importantly, targeting these gut microbial-derived metabolites opens a new window for novel preventative strategies or therapeutic interventions for mycotoxicosis associated to ZEN.
玉米赤霉烯酮(ZEN,一种广泛存在的镰刀菌真菌毒素)暴露会导致农场动物的生殖毒性和免疫毒性,然后通过食物链对人类健康构成潜在威胁。系统了解真菌毒素引起毒性的潜在机制对于克服对农场动物和人类的潜在威胁是必要的。胃肠道是抵御有害真菌毒素的第一道防线;然而,目前尚不清楚真菌毒素(例如 ZEN)对生殖免疫轴的毒性是否与改变的肠道微生物代谢物有关。在这项研究中,我们使用猪(在三个阶段)作为重要的大型动物模型,研究了 ZEN 对生殖免疫轴中免疫防御的毒性是否涉及改变的肠道微生物衍生代谢物。此外,我们观察了通过工程化 ZEN 降解酶来调节肠道微生物衍生代谢物是否可以抵抗 ZEN 对肠道-生殖-免疫轴的毒性。
在这里,我们表明 ZEN 暴露会损害猪在第 1/2 阶段生殖免疫轴中的免疫防御。这种损害伴随着肠道微生物衍生代谢物的改变[例如,丁酸产量减少,脂多糖(LPS)产量增加]。丁酸产量的减少通过 GPR109A 依赖的方式损害肠道屏障,同时血浆中 LPS 的增加加剧了全身炎症,从而直接和/或间接干扰生殖免疫轴中的免疫防御。为了验证这些发现,我们进一步生成了表达 ZEN 降解酶 ZLHY-6 的重组枯草芽孢杆菌 168(Bs-Z6 菌株),作为一种从真菌毒素污染的食物中酶去除 ZEN 的可行性的工具。值得注意的是,通过重组 Bs-Z6 菌株改变的肠道微生物代谢物(例如丁酸、LPS)可以抵抗 ZEN 对肠道屏障的毒性,从而增强猪在第 3 阶段生殖免疫轴中的免疫防御。此外,丁酸补充剂恢复了 ZEN 诱导的猪小肠上皮细胞异常。
总之,这些结果强调了肠道微生物衍生代谢物在 ZEN 诱导的肠道-生殖-免疫轴毒性中的作用。重要的是,针对这些肠道微生物衍生代谢物为与 ZEN 相关的真菌毒素病提供了新的预防策略或治疗干预的新窗口。
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