Integration of human microbiota (SIHUMIx) and zebrafish models reveals microbiome-mediated host responses to azoxystrobin.

IF 4.1 3区医学 Q2 TOXICOLOGY

Toxicological Sciences Pub Date : 2026-04-07 DOI:10.1093/toxsci/kfag022

Chloe Wray, Victor Castañeda-Monsalve, Beatrice Engelmann, Ulrike E Rolle-Kampczyk, Nicole Schweiger, Sebastian Gutsfeld, Debjyoti Ghosh, Siraz Kader, Charles R Tyler, Nico Jehmlich, Tamara Tal

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引用次数: 0

Abstract

The gut microbiome is essential for neurodevelopment via bidirectional gut-brain axis signaling, yet environmental chemicals can potentially disrupt this communication by altering community structure and xenobiotic metabolism. In this study, we investigated whether the fungicide azoxystrobin, a known metabolic disruptor, modulates microbiome composition and function to influence neurobehavior. We utilized a simplified human gut microbiota model (SIHUMIx) and a vertebrate host model (larval zebrafish) to elucidate microbiome-mediated mechanisms of xenobiotic neurotoxicity. SIHUMIx was exposed to azoxystrobin for 7 days at 10% of the acceptable daily intake, followed by recovery. Integrated metaproteomic and metabolomic analyses revealed functional reprogramming of the microbiota, characterized by upregulation of vitamin and cofactor biosynthesis, nutrient acquisition, and detoxification pathways, and decreases in carbohydrate fermentation and amino acid turnover, consistent with reduced short-chain fatty acid levels. Microbiome-depleted and SIHUMIx-inoculated larvae were exposed to azoxystrobin at 4 days post fertilization, and neurobehavioral outcomes were assessed after 24 h using the Visual and Acoustic Motor Response assay. Azoxystrobin exposure disrupted non-associative habituation learning independent of microbiome status but induced dark-phase hyperactivity only in colonized larvae, indicating a microbiome-dependent phenotype. Targeted metabolomics revealed lower serotonin levels in microbiome-depleted larvae relative to colonized controls and that azoxystrobin exposure reduced serotonin in colonized larvae toward depleted levels. These results suggest that microbiota-dependent serotonergic signaling may modulate host responses to azoxystrobin. This integrated ex vivo-in vivo approach supports the concept that the microbiome is a key determinant of neurotoxic responses and underscores the importance of incorporating microbiome-mediated effects into chemical risk assessment frameworks.

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人类微生物群（SIHUMIx）和斑马鱼模型的整合揭示了微生物组介导的宿主对氮氧嘧啶的反应。

肠道微生物组通过双向肠-脑轴信号传导对神经发育至关重要，但环境化学物质可能通过改变群落结构和外源代谢而潜在地破坏这种交流。在这项研究中，我们研究了杀菌剂氮唑菌酯（一种已知的代谢干扰物）是否会调节微生物组的组成和功能，从而影响神经行为。我们利用简化的人类肠道微生物群模型（SIHUMIx）和脊椎动物宿主模型（幼体斑马鱼）来阐明微生物群介导的外源神经毒性机制。SIHUMIx以每日可接受摄入量的10%暴露于偶氮嘧菌酯7天，随后恢复。综合元蛋白质组学和代谢组学分析显示，微生物群的功能重编程，其特征是维生素和辅助因子的生物合成、营养获取和解毒途径上调，碳水化合物发酵和氨基酸周转减少，与短链脂肪酸水平降低一致。在受精后4天，将微生物组耗尽和sihumix接种的幼虫暴露于偶氮嘧菌酯中，并在24小时后通过视觉和听觉运动反应试验评估神经行为结果。偶氮嘧菌酯暴露破坏了与微生物组状态无关的非联想习惯化学习，但仅在定植的幼虫中诱导暗相过动，表明微生物组依赖性表型。靶向代谢组学显示，与定植对照相比，微生物组缺失的幼虫血清素水平较低，偶氮虫酯暴露使定植幼虫血清素水平降低。这些结果表明，微生物依赖的血清素能信号可能调节宿主对氮嘧菌酯的反应。这种综合的体外-体内方法支持了微生物组是神经毒性反应的关键决定因素的概念，并强调了将微生物组介导的效应纳入化学风险评估框架的重要性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Toxicological Sciences 医学-毒理学

CiteScore

7.70

自引率

7.90%

发文量

118

审稿时长

1.5 months

期刊介绍： The mission of Toxicological Sciences, the official journal of the Society of Toxicology, is to publish a broad spectrum of impactful research in the field of toxicology. The primary focus of Toxicological Sciences is on original research articles. The journal also provides expert insight via contemporary and systematic reviews, as well as forum articles and editorial content that addresses important topics in the field. The scope of Toxicological Sciences is focused on a broad spectrum of impactful toxicological research that will advance the multidisciplinary field of toxicology ranging from basic research to model development and application, and decision making. Submissions will include diverse technologies and approaches including, but not limited to: bioinformatics and computational biology, biochemistry, exposure science, histopathology, mass spectrometry, molecular biology, population-based sciences, tissue and cell-based systems, and whole-animal studies. Integrative approaches that combine realistic exposure scenarios with impactful analyses that move the field forward are encouraged.