Infants born to mothers with IBD present with altered gut microbiome that transfers abnormalities of the adaptive immune system to germ-free mice

Torres, Joana; Hu, Jianzhong; Seki, Akihiro; Eisele, Caroline; Nair, N. Unnikrishnan; Huang, Ruiqi; Tarassishin, Leonid; Jharap, Bindia; Côté-Daigneault, Justin; Mao, Qixing; Mogno, Ilaria; Britton, Graham J.; Uzzan, Mathieu; Chen, Ching-Lynn; Kornbluth, Asher; George, James; Legnani, Peter; Maser, Elana; Loudon, Holly; Stone, Joanne; Dubinsky, Marla; Faith, Jeremiah J.; Clemente, José C.; Mehandru, Saurabh; Colombel, Jean–Frédéric; Peter, Inga

doi:10.1136/gutjnl-2018-317855

Cited by 127 publications

(76 citation statements)

References 55 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Furthermore, we found abnormal levels of faecal bacterial metabolites in one of the healthy parents in two of three families with a child with CD, which could indicate that dysbiosis is a genetically or environmentally determined trait predisposing to intestinal inflammation in CD. [8] This is in agreement with recently published findings by Joossens et al [10] and Torres et al [11] Van Kruiningen correctly pointed out that extraintestinal manifestations of CD, such as in genitalia, lips or oral cavity, might precede or follow luminal disease. "That CD occurs in these locations, where there is no abscessation, fistulas or microbiome attests to the vascular basis of disease".…”

Section: To the Editorsupporting

confidence: 86%

On the Pathogenesis of Crohn´s Disease

Sundqvist¹,

Stenhammar²,

Tjellström³

et al. 2020

OBM HG

View full text Add to dashboard Cite

Section: To the Editorsupporting

confidence: 86%

On the Pathogenesis of Crohn´s Disease

Sundqvist¹,

Stenhammar²,

Tjellström³

et al. 2020

OBM HG

View full text Add to dashboard Cite

“…Imprinting of the immune system by the microbiota early in life Z Al Nabhani and G Eberl system. Similarly, alterations (dysbiosis) in the maternal microbiota can be transmitted to the offspring and determine immune reactivity in the long term, [34][35][36] an effect that we will discuss in a later chapter. Other compounds of dietary origin, the metabolism of which may be modulated by the microbiota, such as retinoic acid (RA), have significant effects on the developing fetal immune system.…”

Section: A Fetal Time Window?mentioning

confidence: 99%

Imprinting of the immune system by the microbiota early in life

2020

View full text Add to dashboard Cite

The ontogeny and maturation of the immune system is modulated by the microbiota. During fetal life, the mother's microbiota produces compounds that are transferred to the fetus and offspring, and enhance the generation of innate immune cells. After birth, the colonizing microbiota induces the development of intestinal lymphoid tissues and maturation of myeloid and lymphoid cells, and imprints the immune system with a reactivity level that persists long after weaning into adulthood. When the cross-talk between host and microbiota is perturbed early in life, a pathological imprinting may develop that is characterized by excessive immune reactivity in adulthood, which translates into increased susceptibility to inflammatory pathologies. In this review, we discuss the recent data that demonstrate the existence of a time window of opportunity early in life during which mice and human have to be exposed to microbiota in order to develop a balanced immune system. We also discuss the factors involved in imprinting, such as the microbiota, immune cells and stromal cells, as well as the nature of imprinting.Mucosal Immunology (2020) 13:183-189; https://doi.

show abstract

“…In accordance with this, it has been shown that dysbiosis of the intestinal ecosystem is correlated with a wide variety of diseases, including inflammatory bowel disease, allergy, cancer, autism, and metabolic syndrome (3,(5)(6)(7)(8)(9). Although it is difficult to determine whether such differences in gut microbiota are the cause or the result of these diseases, studies have demonstrated that change in microbiota or specific bacteria is actually involved in the onset, pathogenesis, and prevention of the diseases (10)(11)(12). Therefore, many efforts have been made to prevent the onset or alleviate the symptoms of the diseases by intervention to the gut microbiota (13)(14)(15)(16)(17).…”

Section: Introductionmentioning

confidence: 87%

Regulation of Gene Expression through Gut Microbiota-Dependent DNA Methylation in Colonic Epithelial Cells

et al. 2020

View full text Add to dashboard Cite

A huge number of commensal bacteria inhabit the intestine, which is equipped with the largest immune system in the body. Recently, the regulation of various physiological functions of the host by these bacteria has attracted attention. In this study, the effects of commensal bacteria on gene expression in colonic epithelial cells (CoECs) were investigated with focus on regulation of DNA methylation. RNA sequencing analyses of CoECs from conventional, germ-free, and MyD88 2/2 mice indicated that, out of the genes affected by commensal bacteria, those downregulated in a MyD88-independent manner were most frequently observed. Furthermore, when the 59 regions of genes downregulated by commensal bacteria in CoECs were captured using a customized array and immunoprecipitated with the anti-methyl cytosine Ab, a certain population of these genes was found to be highly methylated. Comprehensive analysis of DNA methylation in the 59 regions of genes in CoECs from conventional and germ-free mice upon pulldown assay with methyl-CpG-binding domain protein 2 directly demonstrated that DNA methylation in these regions was influenced by commensal bacteria. Actually, commensal bacteria were shown to control expression of Aldh1a1, which encodes a retinoic acid-producing enzyme and plays an important role in the maintenance of intestinal homeostasis via DNA methylation in the overlapping 59 region of Tmem267 and 3110070M22Rik genes in CoECs. Collectively, it can be concluded that regulation of DNA methylation in the 59 regions of a specific population of genes in CoECs acts as a mechanism by which commensal bacteria have physiological effects on the host.

show abstract

Infants born to mothers with IBD present with altered gut microbiome that transfers abnormalities of the adaptive immune system to germ-free mice

Cited by 127 publications

References 55 publications

On the Pathogenesis of Crohn´s Disease

On the Pathogenesis of Crohn´s Disease

Imprinting of the immune system by the microbiota early in life

Regulation of Gene Expression through Gut Microbiota-Dependent DNA Methylation in Colonic Epithelial Cells

Contact Info

Product

Resources

About