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雄性和雌性小鼠经口暴露于苯扎氯铵后,肠道微生物群和胆汁酸谱呈现出性别依赖性改变。

Oral Exposure to Benzalkonium Chlorides in Male and Female Mice Reveals Sex-Dependent Alteration of the Gut Microbiome and Bile Acid Profile.

作者信息

Lopez Vanessa A, Lim Joe L, Seguin Ryan P, Dempsey Joseph L, Kunzman Gabrielle, Cui Julia Y, Xu Libin

出版信息

bioRxiv. 2024 May 16:2024.05.13.593991. doi: 10.1101/2024.05.13.593991.

Abstract

Benzalkonium chlorides (BACs) are commonly used disinfectants in a variety of consumer and food-processing settings, and the COVID-19 pandemic has led to increased usage of BACs. The prevalence of BACs raises the concern that BAC exposure could disrupt the gastrointestinal microbiota, thus interfering with the beneficial functions of the microbes. We hypothesize that BAC exposure can alter the gut microbiome diversity and composition, which will disrupt bile acid homeostasis along the gut-liver axis. In this study, male and female mice were exposed orally to d -C12- and d -C16-BACs at 120 µg/g/day for one week. UPLC-MS/MS analysis of liver, blood, and fecal samples of BAC-treated mice demonstrated the absorption and metabolism of BACs. Both parent BACs and their metabolites were detected in all exposed samples. Additionally, 16S rRNA sequencing was carried out on the bacterial DNA isolated from the cecum intestinal content. For female mice, and to a lesser extent in males, we found that treatment with either d -C12- or d -C16-BAC led to decreased alpha diversity and differential composition of gut bacteria with notably decreased actinobacteria phylum. Lastly, through a targeted bile acid quantitation analysis, we observed decreases in secondary bile acids in BAC-treated mice, which was more pronounced in the female mice. This finding is supported by decreases in bacteria known to metabolize primary bile acids into secondary bile acids, such as the families of Ruminococcaceae and Lachnospiraceae. Together, these data signify the potential impact of BACs on human health through disturbance of the gut microbiome and gut-liver interactions.

摘要

苯扎氯铵(BACs)是在各种消费和食品加工环境中常用的消毒剂,而新冠疫情导致了BACs使用量的增加。BACs的广泛使用引发了人们对接触BACs可能破坏胃肠道微生物群,从而干扰微生物有益功能的担忧。我们推测,接触BACs会改变肠道微生物群的多样性和组成,进而破坏肠-肝轴上的胆汁酸稳态。在本研究中,雄性和雌性小鼠口服给予120μg/g/天的d -C12-和d -C16-BACs,持续一周。对接受BAC处理的小鼠的肝脏、血液和粪便样本进行超高效液相色谱-串联质谱(UPLC-MS/MS)分析,证明了BACs的吸收和代谢。在所有暴露样本中均检测到了母体BACs及其代谢产物。此外,对从盲肠肠内容物中分离出的细菌DNA进行了16S rRNA测序。对于雌性小鼠,在雄性小鼠中程度稍轻,我们发现用d -C12-或d -C16-BAC处理会导致肠道细菌的α多样性降低和组成差异,其中放线菌门显著减少。最后,通过靶向胆汁酸定量分析,我们观察到接受BAC处理的小鼠中次级胆汁酸减少,这在雌性小鼠中更为明显。已知将初级胆汁酸代谢为次级胆汁酸的细菌(如瘤胃球菌科和毛螺菌科)数量减少,支持了这一发现。总之,这些数据表明BACs可能通过干扰肠道微生物群和肠-肝相互作用对人类健康产生潜在影响。

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