A triad of gut dysbiosis, dysregulated immunity, and 'leaky' gut characterize HCMV associated neonatal cholestasis.

IF 4.3 3区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Gut Pathogens Pub Date : 2024-11-14 DOI:10.1186/s13099-024-00663-3
Kalyani Karandikar, Gauri Bhonde, Harsha Palav, Varsha Padwal, Shilpa Velhal, Jacintha Pereira, Himali Meshram, Akshat Goel, Ira Shah, Vainav Patel, Vikrant M Bhor
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Abstract

Background: Gut microbiome dysbiosis and related immune dysfunction have been associated with the pathogenesis of Human Cytomegalovirus (HCMV) infection in infants with neonatal cholestasis (NC) as previously reported by us. However, the interaction of a perturbed microbiome, HCMV infection, and dysregulated immunity leading to exacerbation of disease severity has not been investigated so far. In this study, we examined the association of gut microbiome, host inflammatory and homeostatic markers that are likely to govern increased pathogenesis of NC in HCMV infected IgM positive infants (N = 15) compared to IgM negative (N = 15) individuals. Stool samples of HCMV infected infants and age-matched healthy controls (N = 10) were assessed for gut bacteria-derived metabolites like short-chain fatty acids (SCFAs), Lipopolysaccharide (LPS), cytokines and markers of gut barrier integrity. Data were correlated with previously determined gut microbiome composition and frequency of immune cell subsets. Finally, validation of clinical potential was undertaken by principal component analysis (PCA) of integrated data to delineate the spectrum of clinical pathology.

Results: Significantly lower levels of SCFAs and elevated fecal levels of soluble inflammatory mediators were observed in IgM positive HCMV infected infants. Further, increased plasma LPS levels and markers of gut permeability, suggestive of microbial translocation due to a 'leaky gut' were observed in HCMV infected IgM positive group. PCA of integrated data revealed clearly disparate profiles representative of IgM positive, IgM negative, and uninfected healthy states.

Conclusion: Our results suggest the utility of an integrated approach involving dysregulated microbiome-immune axis for gaining a better understanding of pathogenesis associated with HCMV infection in NC.

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与 HCMV 相关的新生儿胆汁淤积症的特点是肠道菌群失调、免疫调节失调和 "渗漏 "肠道三合一。
背景:肠道微生物群失调和相关的免疫功能障碍与新生儿胆汁淤积症(NC)婴儿感染人类巨细胞病毒(HCMV)的发病机制有关,我们以前也曾报道过。然而,迄今为止,尚未研究过紊乱的微生物组、HCMV 感染和免疫功能失调之间的相互作用会导致疾病严重程度加剧。在本研究中,我们研究了肠道微生物组、宿主炎症和同源性标记物之间的关联,与 IgM 阴性(15 例)的个体相比,这些标记物可能会增加 HCMV 感染 IgM 阳性婴儿 NC 的发病机理。对 HCMV 感染婴儿和年龄匹配的健康对照组(10 例)的粪便样本进行了肠道细菌衍生代谢物评估,如短链脂肪酸 (SCFA)、脂多糖 (LPS)、细胞因子和肠道屏障完整性标记物。数据与之前确定的肠道微生物组组成和免疫细胞亚群频率相关联。最后,通过对综合数据进行主成分分析(PCA)来验证临床潜力,以划分临床病理范围:结果:在 IgM 阳性的 HCMV 感染婴儿中观察到 SCFAs 水平显著降低,粪便中可溶性炎症介质水平升高。此外,在 IgM 阳性的 HCMV 感染组中还观察到血浆 LPS 水平和肠道通透性标志物升高,这表明 "肠道渗漏 "导致微生物易位。综合数据的 PCA 显示了 IgM 阳性、IgM 阴性和未感染健康状态的明显不同特征:我们的研究结果表明,采用微生物组-免疫轴失调的综合方法可以更好地了解 NC 中与 HCMV 感染相关的发病机制。
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来源期刊
Gut Pathogens
Gut Pathogens GASTROENTEROLOGY & HEPATOLOGY-MICROBIOLOGY
CiteScore
7.70
自引率
2.40%
发文量
43
期刊介绍: Gut Pathogens is a fast publishing, inclusive and prominent international journal which recognizes the need for a publishing platform uniquely tailored to reflect the full breadth of research in the biology and medicine of pathogens, commensals and functional microbiota of the gut. The journal publishes basic, clinical and cutting-edge research on all aspects of the above mentioned organisms including probiotic bacteria and yeasts and their products. The scope also covers the related ecology, molecular genetics, physiology and epidemiology of these microbes. The journal actively invites timely reports on the novel aspects of genomics, metagenomics, microbiota profiling and systems biology. Gut Pathogens will also consider, at the discretion of the editors, descriptive studies identifying a new genome sequence of a gut microbe or a series of related microbes (such as those obtained from new hosts, niches, settings, outbreaks and epidemics) and those obtained from single or multiple hosts at one or different time points (chronological evolution).
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