首页> 美国卫生研究院文献>Nutrients >Dietary Gluten-Induced Gut Dysbiosis Is Accompanied by Selective Upregulation of microRNAs with Intestinal Tight Junction and Bacteria-Binding Motifs in Rhesus Macaque Model of Celiac Disease
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Dietary Gluten-Induced Gut Dysbiosis Is Accompanied by Selective Upregulation of microRNAs with Intestinal Tight Junction and Bacteria-Binding Motifs in Rhesus Macaque Model of Celiac Disease

机译:饮食性谷蛋白诱导的肠内营养不良与在乳糜泻的恒河猕猴模型中具有肠道紧密连接和细菌结合基序的microRNA选择性上调相伴。

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摘要

The composition of the gut microbiome reflects the overall health status of the host. In this study, stool samples representing the gut microbiomes from 6 gluten-sensitive (GS) captive juvenile rhesus macaques were compared with those from 6 healthy, age- and diet-matched peers. A total of 48 samples representing both groups were studied using V4 16S rRNA gene DNA analysis. Samples from GS macaques were further characterized based on type of diet administered: conventional monkey chow, i.e., wheat gluten-containing diet (GD), gluten-free diet (GFD), barley gluten-derived diet (BOMI) and reduced gluten barley-derived diet (RGB). It was hypothesized that the GD diet would lower the gut microbial diversity in GS macaques. This is the first report illustrating the reduction of gut microbial alpha-diversity (p < 0.05) following the consumption of dietary gluten in GS macaques. Selected bacterial families (e.g., Streptococcaceae and Lactobacillaceae) were enriched in GS macaques while Coriobacteriaceae was enriched in healthy animals. Within several weeks after the replacement of the GD by the GFD diet, the composition (beta-diversity) of gut microbiome in GS macaques started to change (p = 0.011) towards that of a normal macaque. Significance for alpha-diversity however, was not reached by the day 70 when the feeding experiment ended. Several inflammation-associated microRNAs (miR-203, -204, -23a, -23b and -29b) were upregulated (p < 0.05) in jejunum of 4 biopsied GS macaques fed GD with predicted binding sites on 16S ribosomal RNA of Lactobacillus reuteri (accession number: ), Prevotella stercorea () and Streptococcus luteciae () that were overrepresented in feces. Additionally, claudin-1, a validated tight junction protein target of miR-29b was significantly downregulated in jejunal epithelium of GS macaques. Taken together, we predict that with the introduction of effective treatments in future studies the diversity of gut microbiomes in GS macaques will approach those of healthy individuals. Further studies are needed to elucidate the regulatory pathways of inflammatory miRNAs in intestinal mucosa of GS macaques and to correlate their expression with gut dysbiosis.
机译:肠道微生物组的组成反映了宿主的整体健康状况。在这项研究中,代表6个面筋敏感(GS)圈养幼年猕猴的肠道微生物组的粪便样品与来自6个健康,年龄和饮食匹配的同龄人的粪便样品进行了比较。使用V4 16S rRNA基因DNA分析研究了代表两组的总共48个样品。 GS猕猴的样品还根据所用饮食的类型进行了表征:常规的猴饲料,即含小麦面筋的饮食(GD),无面筋的饮食(GFD),大麦面筋衍生的饮食(BOMI)和低筋大麦-衍生饮食(RGB)。据推测,GD饮食会降低GS猕猴的肠道微生物多样性。这是第一份报告,显示了食用GS猕猴食用面筋后肠道微生物α多样性降低(p <0.05)。选定的细菌家族(例如链球菌科和乳杆菌科)富含GS猕猴,而结肠杆菌科则富含健康动物。用GFD饮食替代GD后的几周内,GS猕猴中肠道微生物组的组成(β多样性)开始向正常猕猴变化(p = 0.011)。但是,到喂养实验结束的第70天,仍没有达到α多样性的意义。在饲喂GD的4例活检GS猕猴的空肠中,几种炎症相关的microRNA(miR-203,-204,-23a,-23b和-29b)被上调(p <0.05),其在路氏乳杆菌的16S核糖体RNA上具有预测的结合位点(登记号:),粪便中的斯特雷沃氏菌(stervo preella stercorea)和褐变链球菌(streptococcus luteciae)()。此外,claodin-1(一种经过验证的miR-29b紧密连接蛋白靶标)在GS猕猴的空肠上皮中显着下调。两者合计,我们预测,随着未来研究的有效治疗的引入,GS猕猴中肠道微生物群的多样性将接近健康个体。需要进一步的研究以阐明GS猕猴肠道黏膜中炎性miRNA的调控途径,并将其表达与肠道营养不良相关联。

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