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粪便生物标志物作为衡量衣索比亚阿迪斯阿贝巴非正规住区婴儿肠道病原体感染的指标。

Stool biomarkers as measures of enteric pathogen infection in infants from Addis Ababa informal settlements.

机构信息

Department of Epidemiology, University of Michigan School of Public Health, Ann Arbor, Michigan, United States of America.

Rutgers Global Health Institute & Department of Biostatistics and Epidemiology School of Public Health Rutgers, The State University of New Jersey, New Brunswick, New Jersey, United States of America.

出版信息

PLoS Negl Trop Dis. 2023 Feb 21;17(2):e0011112. doi: 10.1371/journal.pntd.0011112. eCollection 2023 Feb.

Abstract

Frequent enteric infections in children may be an important cause of growth faltering; however, we do not fully understand the mechanisms by which pathogen infections and the physiological responses to these infections result in poorer growth. Commonly used protein fecal biomarkers (anti-alpha trypsin, neopterin, and myeloperoxidase) provide broad immunological information on an inflammatory response; however, they do not provide information on non-immune processes (e.g., gut integrity) that may be important indicators of chronic end states such as environmental enteric dysfunction (EED). To explore how additional biomarkers will better inform which physiological pathways (both immune and non-immune) are impacted by pathogen exposure we added to the traditional panel of 3 protein fecal biomarkers 4 novel fecal mRNA transcript biomarkers (sucrase isomaltase, caudal homeobox 1, S100A8, and mucin 12) and analyzed stool samples from infants living in informal settlements in Addis Ababa, Ethiopia. To test how this expanded biomarker panel captures distinct pathogen exposure processes we used two different scoring systems. First, we used a theory-based approach to assign each biomarker to specific physiological attributes based on prior understanding of each biomarker. Second, we used data reduction methods to categorize biomarkers and then assign physiological attributes to those categories. We used linear models to examine the association between the derived biomarker scores (based on mRNA and protein levels) and stool pathogen gene counts to determine pathogen specific effects on gut physiology and immune responses. Inflammation scores were positively associated with Shigella and enteropathogenic E.Coli (EPEC) infection, while gut integrity scores were negatively associated with Shigella, EPEC and, shigatoxigenic E.coli (STEC) infection. Our expanded panel of biomarkers hold promise as tools to measure systemic outcomes of enteric pathogen infection. mRNA biomarkers complement established protein biomarkers by providing important cell-specific physiological and immunological consequences of pathogen carriage that can lead to chronic end states such as EED.

摘要

儿童频繁发生肠道感染可能是生长迟缓的一个重要原因;然而,我们还不完全了解病原体感染及其对这些感染的生理反应导致生长不良的机制。常用的蛋白质粪便生物标志物(抗-α胰蛋白酶、新蝶呤和髓过氧化物酶)提供了广泛的免疫信息,反映了炎症反应;但是,它们不能提供非免疫过程(例如肠道完整性)的信息,而这些信息可能是环境肠道功能障碍(EED)等慢性终末状态的重要指标。为了探讨其他生物标志物如何更好地告知哪些生理途径(免疫和非免疫)受到病原体暴露的影响,我们在传统的 3 种蛋白质粪便生物标志物中增加了 4 种新型粪便 mRNA 转录物生物标志物(蔗糖异麦芽糖酶、尾型同源盒 1、S100A8 和粘蛋白 12),并分析了生活在埃塞俄比亚亚的斯亚贝巴非正式住区的婴儿的粪便样本。为了检验这个扩展的生物标志物组合如何捕捉到不同的病原体暴露过程,我们使用了两种不同的评分系统。首先,我们根据对每个生物标志物的先前了解,使用基于理论的方法将每个生物标志物分配到特定的生理属性。其次,我们使用数据减少方法对生物标志物进行分类,然后将生理属性分配给这些类别。我们使用线性模型来检验基于 mRNA 和蛋白质水平得出的生物标志物得分与粪便病原体基因计数之间的关联,以确定病原体对肠道生理和免疫反应的特定影响。炎症评分与志贺氏菌和肠致病性大肠杆菌(EPEC)感染呈正相关,而肠道完整性评分与志贺氏菌、EPEC 和产志贺毒素大肠杆菌(STEC)感染呈负相关。我们扩展的生物标志物组合有望成为衡量肠道病原体感染全身后果的工具。mRNA 生物标志物通过提供病原体携带的重要细胞特异性生理和免疫后果来补充已建立的蛋白质生物标志物,这些后果可能导致 EED 等慢性终末状态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/20b9/9983878/9f60891da036/pntd.0011112.g001.jpg

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