首页> 美国卫生研究院文献>American Journal of Physiology - Gastrointestinal and Liver Physiology >Preterm infant gut microbiota affects intestinal epithelial development in a humanized microbiome gnotobiotic mouse model
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Preterm infant gut microbiota affects intestinal epithelial development in a humanized microbiome gnotobiotic mouse model

机译:早产儿肠道菌群在人源化微生物组致生性小鼠模型中影响肠道上皮发育

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摘要

Development of the infant small intestine is influenced by bacterial colonization. To promote establishment of optimal microbial communities in preterm infants, knowledge of the beneficial functions of the early gut microbiota on intestinal development is needed. The purpose of this study was to investigate the impact of early preterm infant microbiota on host gut development using a gnotobiotic mouse model. Histological assessment of intestinal development was performed. The differentiation of four epithelial cell lineages (enterocytes, goblet cells, Paneth cells, enteroendocrine cells) and tight junction (TJ) formation was examined. Using weight gain as a surrogate marker for health, we found that early microbiota from a preterm infant with normal weight gain (MPI-H) induced increased villus height and crypt depth, increased cell proliferation, increased numbers of goblet cells and Paneth cells, and enhanced TJs compared with the changes induced by early microbiota from a poor weight gain preterm infant (MPI-L). Laser capture microdissection (LCM) plus qRT-PCR further revealed, in MPI-H mice, a higher expression of stem cell marker Lgr5 and Paneth cell markers Lyz1 and Cryptdin5 in crypt populations, along with higher expression of the goblet cell and mature enterocyte marker Muc3 in villus populations. In contrast, MPI-L microbiota failed to induce the aforementioned changes and presented intestinal characteristics comparable to a germ-free host. Our data demonstrate that microbial communities have differential effects on intestinal development. Future studies to identify pioneer settlers in neonatal microbial communities necessary to induce maturation may provide new insights for preterm infant microbial ecosystem therapeutics.
机译:婴儿小肠的发育受细菌定植的影响。为了促进在早产儿中建立最佳微生物群落,需要了解早期肠道菌群对肠道发育的有益功能。这项研究的目的是使用gnotobiotic小鼠模型调查早期早产儿微生物群对宿主肠道发育的影响。进行了肠道发育的组织学评估。检查了四个上皮细胞谱系(肠上皮细胞,杯状细胞,Paneth细胞,肠内分泌细胞)的分化和紧密连接(TJ)的形成。使用体重增加作为健康的替代指标,我们发现正常体重增加(MPI-H)的早产儿的早期菌群会引起绒毛高度和隐窝深度增加,细胞增殖增加,杯状细胞和Paneth细胞数量增加,以及与体重增加较差的早产儿(MPI-L)早期菌群引起的变化相比,TJ增强。激光捕获显微切割术(LCM)和qRT-PCR进一步揭示,在MPI-H小鼠中,隐窝群体中干细胞标记物Lgr5和Paneth细胞标记物Lyz1和Cryptdin5的表达更高,而杯状细胞和成熟肠细胞标记物的表达更高。绒毛种群中的Muc3。相反,MPI-L微生物群不能诱导上述变化,并且表现出与无菌宿主相当的肠道特性。我们的数据表明,微生物群落对肠道发育具有不同的影响。未来研究确定诱导成熟所需的新生儿微生物群落中的先驱定居者,可能为早产儿微生物生态系统治疗提供新的见解。

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