Institut de Recherche en Santé Digestive (IRSD), INSERM UMR-1220, Purpan Hospital, CS60039, University of Toulouse, INSERM, INRAE, ENVT, UPS, 31024, Toulouse Cedex 03, France.
M2iSH, Université Clermont Auvergne, UMR1071 INSERM, USC INRAE 1382, Clermont-Ferrand, France.
Part Fibre Toxicol. 2023 Nov 23;20(1):45. doi: 10.1186/s12989-023-00555-5.
Perinatal exposure to titanium dioxide (TiO), as a foodborne particle, may influence the intestinal barrier function and the susceptibility to develop inflammatory bowel disease (IBD) later in life. Here, we investigate the impact of perinatal foodborne TiO exposure on the intestinal mucosal function and the susceptibility to develop IBD-associated colitis. Pregnant and lactating mother mice were exposed to TiO until pups weaning and the gut microbiota and intestinal barrier function of their offspring was assessed at day 30 post-birth (weaning) and at adult age (50 days). Epigenetic marks was studied by DNA methylation profile measuring the level of 5-methyl-2'-deoxycytosine (5-Me-dC) in DNA from colic epithelial cells. The susceptibility to develop IBD has been monitored using dextran-sulfate sodium (DSS)-induced colitis model. Germ-free mice were used to define whether microbial transfer influence the mucosal homeostasis and subsequent exacerbation of DSS-induced colitis.
In pregnant and lactating mice, foodborne TiO was able to translocate across the host barriers including gut, placenta and mammary gland to reach embryos and pups, respectively. This passage modified the chemical element composition of foetus, and spleen and liver of mothers and their offspring. We showed that perinatal exposure to TiO early in life alters the gut microbiota composition, increases the intestinal epithelial permeability and enhances the colonic cytokines and myosin light chain kinase expression. Moreover, perinatal exposure to TiO also modifies the abilities of intestinal stem cells to survive, grow and generate a functional epithelium. Maternal TiO exposure increases the susceptibility of offspring mice to develop severe DSS-induced colitis later in life. Finally, transfer of TiO-induced microbiota dysbiosis to pregnant germ-free mice affects the homeostasis of the intestinal mucosal barrier early in life and confers an increased susceptibility to develop colitis in adult offspring.
Our findings indicate that foodborne TiO consumption during the perinatal period has negative long-lasting consequences on the development of the intestinal mucosal barrier toward higher colitis susceptibility. This demonstrates to which extent environmental factors influence the microbial-host interplay and impact the long-term mucosal homeostasis.
作为一种食物源颗粒,围产期暴露于二氧化钛(TiO)可能会影响肠道屏障功能,并增加日后患炎症性肠病(IBD)的易感性。在这里,我们研究了围产期食物源 TiO 暴露对肠道黏膜功能和发展 IBD 相关结肠炎易感性的影响。在哺乳期的母亲暴露于 TiO 中,直至幼仔断奶,然后在出生后 30 天(断奶)和成年期(50 天)评估其后代的肠道微生物群和肠道屏障功能。通过测量结肠上皮细胞 DNA 中 5-甲基-2'-脱氧胞嘧啶(5-Me-dC)的水平来研究 DNA 甲基化谱中的表观遗传标记。使用葡聚糖硫酸钠(DSS)诱导的结肠炎模型监测发展 IBD 的易感性。使用无菌小鼠来定义微生物转移是否会影响黏膜稳态,并随后加剧 DSS 诱导的结肠炎。
在怀孕和哺乳期的小鼠中,食物源 TiO 能够穿过宿主屏障,包括肠道、胎盘和乳腺,分别到达胚胎和幼仔。这种转移改变了胎儿、母亲及其后代的脾脏和肝脏的化学元素组成。我们表明,生命早期围产期暴露于 TiO 会改变肠道微生物群组成,增加肠道上皮通透性,并增强结肠细胞因子和肌球蛋白轻链激酶的表达。此外,围产期暴露于 TiO 还会改变肠道干细胞的存活、生长和生成功能性上皮的能力。母亲 TiO 暴露增加了后代小鼠在生命后期发展严重 DSS 诱导结肠炎的易感性。最后,将 TiO 诱导的微生物失调转移到怀孕的无菌小鼠中,会影响生命早期肠道黏膜屏障的稳态,并使成年后代更容易发生结肠炎。
我们的研究结果表明,围产期摄入食物源 TiO 对肠道黏膜屏障的发育产生负面影响,增加了患结肠炎的易感性。这表明环境因素在多大程度上影响微生物与宿主的相互作用,并影响长期的黏膜稳态。
Zotero 插件
