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条件性维生素D受体缺失诱导真菌和古菌群落失调及代谢物改变。

Conditional Vitamin D Receptor Deletion Induces Fungal and Archaeal Dysbiosis and Altered Metabolites.

作者信息

Claypool Duncan J, Zhang Yong-Guo, Xia Yinglin, Sun Jun

机构信息

Department of Medicine, University of Illinois Chicago, Chicago, IL 60612, USA.

Department of Bioengineering, University of Illinois Chicago, Chicago, IL 60607, USA.

出版信息

Metabolites. 2024 Jan 1;14(1):32. doi: 10.3390/metabo14010032.

Abstract

A vitamin D receptor (VDR) deficiency leads to the dysbiosis of intestinal bacteria and is associated with various diseases, including cancer, infections, and inflammatory bowel disease. However, the impact of a VDR deficiency on fungi and archaea is unknown. We conditionally deleted the VDR in Paneth cells (VDR), intestinal epithelial cells (VDR), or myeloid cells (VDR) in mice and collected feces for shotgun metagenomic sequencing and untargeted metabolomics. We found that fungi were significantly altered in each knockout (KO) group compared to the VDR control. The VDR mice had the most altered fungi species (three depleted and seven enriched), followed by the VDR mice (six depleted and two enriched), and the VDR mice (one depleted and one enriched). The methanogen was enriched in the VDR and VDR mice and two further archaeal species ( and ) were enriched in the VDR mice compared to the Loxp group. Significant correlations existed among altered fungi, archaea, bacteria, and viruses in the KO mice. Functional metagenomics showed changes in several biologic functions, including decreased sulfate reduction and increased biosynthesis of cobalamin (vitamin B12) in VDR mice relative to VDR mice. Fecal metabolites were analyzed to examine the involvement of sulfate reduction and other pathways. In conclusion, a VDR deficiency caused the formation of altered fungi and archaea in a tissue- and sex-dependent manner. These results provide a foundation about the impact of a host factor (e.g., VDR deficiency) on fungi and archaea. It opens the door for further studies to determine how mycobiome and cross-kingdom interactions in the microbiome community and metabolites contribute to the risk of certain diseases.

摘要

维生素D受体(VDR)缺乏会导致肠道细菌生态失调,并与多种疾病相关,包括癌症、感染和炎症性肠病。然而,VDR缺乏对真菌和古菌的影响尚不清楚。我们有条件地删除了小鼠潘氏细胞(VDRΔPC)、肠上皮细胞(VDRΔIEC)或髓样细胞(VDRΔM)中的VDR,并收集粪便进行鸟枪法宏基因组测序和非靶向代谢组学分析。我们发现,与VDR对照相比,每个基因敲除(KO)组中的真菌都有显著变化。VDRΔPC小鼠的真菌种类变化最大(三种减少,七种增加),其次是VDRΔIEC小鼠(六种减少,两种增加),VDRΔM小鼠(一种减少,一种增加)。与Loxp组相比,产甲烷菌在VDRΔPC和VDRΔIEC小鼠中富集,另外两种古菌物种(和)在VDRΔM小鼠中富集。KO小鼠中,真菌、古菌、细菌和病毒的变化之间存在显著相关性。功能宏基因组学显示了几种生物学功能的变化,相对于VDRΔIEC小鼠,VDRΔPC小鼠中硫酸盐还原减少,钴胺素(维生素B12)生物合成增加。分析粪便代谢物以检查硫酸盐还原和其他途径的参与情况。总之,VDR缺乏以组织和性别依赖的方式导致真菌和古菌的形成发生改变。这些结果为宿主因素(如VDR缺乏)对真菌和古菌的影响提供了基础。它为进一步研究确定微生物群落中的真菌群落和跨界相互作用以及代谢物如何导致某些疾病的风险打开了大门。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7787/10819266/ca8a83b3c2f8/metabolites-14-00032-g001.jpg

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