单细胞转录组学揭示,早期生活中 BDE-99 的暴露会重新编程肠道-肝脏轴,以促进成年后期雄性小鼠的促炎代谢特征。
Single-cell transcriptomics unveiled that early life BDE-99 exposure reprogrammed the gut-liver axis to promote a proinflammatory metabolic signature in male mice at late adulthood.
机构信息
Department of Environmental and Occupational Health Sciences, University of Washington, Seattle, Washington 98105, USA.
Environmental Health and Microbiome Research Center (EHMBRACE), Seattle, Washington 98105, USA.
出版信息
Toxicol Sci. 2024 Jun 26;200(1):114-136. doi: 10.1093/toxsci/kfae047.
Polybrominated diphenyl ethers (PBDEs) are legacy flame retardants that bioaccumulate in the environment. The gut microbiome is an important regulator of liver functions including xenobiotic biotransformation and immune regulation. We recently showed that neonatal exposure to polybrominated diphenyl ether-99 (BDE-99), a human breast milk-enriched PBDE congener, up-regulated proinflammation-related and down-regulated drug metabolism-related genes predominantly in males in young adulthood. However, the persistence of this dysregulation into late adulthood, differential impact among hepatic cell types, and the involvement of the gut microbiome from neonatal BDE-99 exposure remain unknown. To address these knowledge gaps, male C57BL/6 mouse pups were orally exposed to corn oil (10 ml/kg) or BDE-99 (57 mg/kg) once daily from postnatal days 2-4. At 15 months of age, neonatal BDE-99 exposure down-regulated xenobiotic and lipid-metabolizing enzymes and up-regulated genes involved in microbial influx in hepatocytes. Neonatal BDE-99 exposure also increased the hepatic proportion of neutrophils and led to a predicted increase of macrophage migration inhibitory factor signaling. This was associated with decreased intestinal tight junction protein (Tjp) transcripts, altered gut environment, and dysregulation of inflammation-related metabolites. ScRNA-seq using germ-free (GF) mice demonstrated the necessity of a normal gut microbiome in maintaining hepatic immune tolerance. Microbiota transplant to GF mice using large intestinal microbiome from adults neonatally exposed to BDE-99 down-regulated Tjp transcripts and up-regulated several cytokines in large intestine. In conclusion, neonatal BDE-99 exposure reprogrammed cell type-specific gene expression and cell-cell communication in liver towards proinflammation, and this may be partly due to the dysregulated gut environment.
多溴联苯醚(PBDEs)是一种在环境中生物积累的传统阻燃剂。肠道微生物组是调节肝脏功能的重要因素,包括外来物生物转化和免疫调节。我们最近发现,新生期暴露于多溴联苯醚-99(BDE-99),一种富含人类母乳的 PBDE 同系物,会在成年早期主要上调雄性的促炎相关基因,并下调药物代谢相关基因。然而,这种失调是否会持续到老年期,以及在不同的肝细胞类型中的差异影响,以及肠道微生物组在新生期 BDE-99 暴露中的作用仍不清楚。为了解决这些知识空白,雄性 C57BL/6 幼鼠从出生后第 2-4 天每天口服玉米油(10ml/kg)或 BDE-99(57mg/kg)一次。在 15 个月大时,新生期 BDE-99 暴露下调了肝细胞中外来物和脂质代谢酶的表达,并上调了与微生物流入相关的基因。新生期 BDE-99 暴露还增加了肝脏中性粒细胞的比例,并导致巨噬细胞迁移抑制因子信号的预测增加。这与肠道紧密连接蛋白(Tjp)转录物的减少、肠道环境的改变和炎症相关代谢物的失调有关。使用无菌(GF)小鼠的 scRNA-seq 表明,正常的肠道微生物组对于维持肝脏免疫耐受是必要的。使用从新生期暴露于 BDE-99 的成年鼠的大肠微生物组进行的 GF 小鼠的微生物移植,下调了 Tjp 转录物,并在上肠中上调了几种细胞因子。总之,新生期 BDE-99 暴露会使肝脏中特定细胞类型的基因表达和细胞间通讯向促炎方向重新编程,而这可能部分是由于肠道环境的失调。
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