Prospective study reveals a microbiome signature that predicts the occurrence of post-operative enterocolitis in Hirschsprung disease (HSCR) patients

Tang, Weibing; Su, Yang; Yuan, Chen; Zhang, Yuqing; Zhou, Lingling; Peng, Lei; Wang, Pin; Chen, Guanglin; Li, Yang; Li, Hongxing; Zhi, Zhengke; Chang, Hang; Hang, Bo; Mao, Jian‐Hua; Snijders, Antoine M.; Xia, Yankai

doi:10.1080/19490976.2020.1711685

Cited by 30 publications

(42 citation statements)

References 34 publications

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“…In this study, several gut microbiome derived metabolites and fermentation pathways, as a direct reflection of gut microbiome functionality, were established to be discriminating for the fecal metabolome of HD patients compared to their healthy siblings. Indeed, involvement of the gut microbiome in the pathogenesis of post-operative HD complications is in line with previously published reports 11 , 12 . This can be viewed as a consequence of the (partial) colon resection, as the latter drastically changes the intestinal microenvironment required for maintaining a healthy microbiome.…”

Section: Discussionsupporting

confidence: 91%

“…To date, several studies have focused on the long-term post-surgical complications of HD and factors that might explain HAEC etiology and incidents. Increasing evidence points towards microbiome alterations as a cause or contributing factor in the development of enterocolitis in HD patients 11 , 12 . Moreover, a distinctly different gut microbial pattern has been demonstrated in HAEC patients, even after symptom remission, suggesting that enterocolitis may either be caused by or result in a disruption of the patient’s uniquely adapted intestinal microbiome 13 .…”

Section: Introductionmentioning

confidence: 99%

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Disparities in the gut metabolome of post-operative Hirschsprung's disease patients

Plekhova

Paepe

Renterghem

et al. 2021

Sci Rep

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Hirschsprung's disease (HD) is a congenital structural abnormality of the colon seen in approximately 1 to 5000 live births. Despite surgical correction shortly after presentation, up to 60% of patients will express long-term gastrointestinal complaints, including potentially life-threatening Hirschsprung-associated enterocolitis (HAEC). In this study fecal samples from postoperative HD patients (n = 38) and their healthy siblings (n = 21) were analysed using high-resolution liquid chromatography—mass spectrometry aiming to further unravel the nature of the chronic gastrointestinal disturbances. Furthermore, within the patient group, we compared the faecal metabolome between patients with and without a history of HAEC as well as those diagnosed with short or long aganglionic segment. Targeted analysis identified several individual metabolites characteristic for all HD patients as well as those with a history of HAEC and long segment HD. Moreover, multivariate models based on untargeted data established statistically significant (p < 0.05) differences in comprehensive faecal metabolome in the patients’ cohort as a whole and in patients with a history of HAEC. Pathway analysis revealed the most impact on amino sugar, lysine, sialic acid, hyaluronan and heparan sulphate metabolism in HD, as well as impaired tyrosine metabolism in HAEC group. Those changes imply disruption of intestinal mucosal barrier due to glycosaminoglycan breakdown and dysbiosis as major metabolic changes in patients’ group and should be further explored for potential diagnostic or treatment targets.

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Section: Discussionsupporting

confidence: 91%

Section: Introductionmentioning

confidence: 99%

Disparities in the gut metabolome of post-operative Hirschsprung's disease patients

Plekhova

Paepe

Renterghem

et al. 2021

Sci Rep

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“…Although direct evidence for a role of the immune system in the onset of HSCR is absent, RET and its pathway members are expressed by type 3 innate lymphoid cells (ILC3) and are involved in the organogenesis of intestinal Payer's patches [60,61]. Additionally, while it is clear that HSCR patients present with intestinal dysbiosis [62], further investigation would enlighten the paradoxical proposition of whether dysbiosis can contribute to HSCR, or if it is a consequence of impaired elimination mechanisms due to defective intestinal motility [63,64]. The role of microbes in HSCR pathogenesis is intriguing, yet not entirely surprising, since collective efforts have explored and divulged the important contribution of the gut microbiome in fine-tuning the ENS development and homeostasis [65][66][67][68][69][70][71][72], and vice versa [73].…”

Section: Enteric Neuropathiesmentioning

confidence: 99%

The enteric nervous system in gastrointestinal disease etiology

Holland

Bon-Frauches

Keszthelyi

et al. 2021

Cell. Mol. Life Sci.

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A highly conserved but convoluted network of neurons and glial cells, the enteric nervous system (ENS), is positioned along the wall of the gut to coordinate digestive processes and gastrointestinal homeostasis. Because ENS components are in charge of the autonomous regulation of gut function, it is inevitable that their dysfunction is central to the pathophysiology and symptom generation of gastrointestinal disease. While for neurodevelopmental disorders such as Hirschsprung, ENS pathogenesis appears to be clear-cut, the role for impaired ENS activity in the etiology of other gastrointestinal disorders is less established and is often deemed secondary to other insults like intestinal inflammation. However, mounting experimental evidence in recent years indicates that gastrointestinal homeostasis hinges on multifaceted connections between the ENS, and other cellular networks such as the intestinal epithelium, the immune system, and the intestinal microbiome. Derangement of these interactions could underlie gastrointestinal disease onset and elicit variable degrees of abnormal gut function, pinpointing, perhaps unexpectedly, the ENS as a diligent participant in idiopathic but also in inflammatory and cancerous diseases of the gut. In this review, we discuss the latest evidence on the role of the ENS in the pathogenesis of enteric neuropathies, disorders of gut–brain interaction, inflammatory bowel diseases, and colorectal cancer.

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“…Several studies have reported that the microbial community extensively impacts host health by influencing intestinal epithelial cell proliferation, local and systemic immunity, and metabolism. Intestinal dysbacteriosis is associated with obesity, inflammatory bowel disease (IBD), nonalcoholic fatty liver disease, and metabolic syndrome [ 1 – 4 ]. Diet, environment, and host genetics influence the composition of the gut microbiota, and contribute to the high compositional diversity between individuals, which are comparable to unique fingerprints [ 5 – 8 ].…”

Section: Introductionmentioning

confidence: 99%

Isolation and genomic characterization of five novel strains of Erysipelotrichaceae from commercial pigs

Liu

Zhou

et al. 2021

BMC Microbiol

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Background Members of the Erysipelotrichaceae family have a high abundance in the intestinal tract of mammals, and have been reported to be associated with host metabolic disorders and inflammatory diseases. In our previous study, we found that the abundance of Erysipelotrichaceae strains in the cecum was associated with the concentration of N-acetylgalactosamine (GalNAc). However, only a few members of Erysipelotrichaceae have been isolated and cultured, and their main characteristics, genomic information and the functional capacity of carbohydrate metabolism remain unknown. Results In this study, we tested 10 different kinds of commercially available media and successfully isolated five Erysipelotrichaceae strains from healthy porcine feces. The five isolates were Gram-positive, and their colonies on Gifu anaerobic medium (GAM) or modified GAM were approximately 0.25–1.0 mm in diameter, and they were circular, white, convex, moist, translucent, and contained colony margins. These isolates were subjected to Oxford Nanopore and Illumina whole-genome sequencing, genome assembly, and annotation. Based on whole-genome sequences, the five strains belong to Erysipelotrichaceae bacterium OH741_COT-311, Eubacterium sp. AM28–29, and Faecalitalea cylindroides. The GC content of the five strains ranged from 34.1 to 37.37%. Functional annotation based on the Kyoto encyclopedia of genes and genomes pathways revealed tens to hundreds of strain-specific proteins among different strains, and even between the strains showing high 16S rRNA gene sequence identity. Prediction analysis of carbohydrate metabolism revealed different capacities for metabolizing carbohydrate substrates among Erysipelotrichaceae strains. We identified that genes related to the GalNAc metabolism pathway were enriched in the genomes of all five isolates and 16 Erysipelotrichaceae strains downloaded from GenBank, suggesting the importance of GalNAc metabolism in Erysipelotrichaceae strains. Polysaccharide utilization loci (PUL) analysis revealed that the strains of Erysipelotrichaceae may have the ability to utilize plant polysaccharides. Conclusions The present study not only reports the successful isolation of novel Erysipelotrichaceae strains that enrich the cultured strains of Erysipelotrichaceae, but also provided the genome information of Erysipelotrichaceae strains for further studying the function roles of Erysipelotrichaceae in host phenotypes.

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Prospective study reveals a microbiome signature that predicts the occurrence of post-operative enterocolitis in Hirschsprung disease (HSCR) patients

Cited by 30 publications

References 34 publications

Disparities in the gut metabolome of post-operative Hirschsprung's disease patients

Disparities in the gut metabolome of post-operative Hirschsprung's disease patients

The enteric nervous system in gastrointestinal disease etiology

Isolation and genomic characterization of five novel strains of Erysipelotrichaceae from commercial pigs

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