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慢性和急性肠产毒性大肠杆菌攻毒对断奶仔猪生长性能、肠道炎症、微生物组和代谢组的影响。

Effect of chronic and acute enterotoxigenic E. coli challenge on growth performance, intestinal inflammation, microbiome, and metabolome of weaned piglets.

机构信息

Department of Animal Science, Texas A&M University, College Station, TX, USA.

Center for Phage Technology, Texas A&M University, College Station, TX, USA.

出版信息

Sci Rep. 2022 Mar 23;12(1):5024. doi: 10.1038/s41598-022-08446-z.

Abstract

Post-weaning enteropathies in swine caused by pathogenic E. coli, such as post-weaning diarrhea (PWD) or edema disease (ED), remain a significant problem for the swine industry. Reduction in the use of antibiotics over concerns of antibiotic resistance and public health concerns, necessitate the evaluation of effective antibiotic alternatives to prevent significant loss of livestock and/or reductions in swine growth performance. For this purpose, an appropriate piglet model of pathogenic E. coli enteropathy is required. In this study, we attempted to induce clinical signs of post-weaning disease in a piglet model using a one-time acute or lower daily chronic dose of a pathogenic E. coli strain containing genes for both heat stable and labile toxins, as well as Shiga toxin. The induced disease state was monitored by determining fecal shedding and colonization of the challenge strain, animal growth performance, cytokine levels, fecal calprotectin, histology, fecal metabolomics, and fecal microbiome shifts. The most informative analyses were colonization and shedding of the pathogen, serum cytokines, metabolomics, and targeted metagenomics to determine dysbiosis. Histopathological changes of the gastrointestinal (GI) tract and tight junction leakage as measured by fecal calprotectin concentrations were not observed. Chronic dosing was similar to the acute regimen suggesting that a high dose of pathogen, as used in many studies, may not be necessary. The piglet disease model presented here can be used to evaluate alternative PWD treatment options.

摘要

断奶后猪的致病性大肠杆菌引起的肠病,如断奶后腹泻(PWD)或水肿病(ED),仍然是养猪业的一个重大问题。由于对抗生素耐药性和公众健康的担忧,减少抗生素的使用,因此需要评估有效的抗生素替代品,以防止牲畜大量损失和/或猪生长性能下降。为此,需要建立一种合适的致病性大肠杆菌肠病仔猪模型。在这项研究中,我们试图使用含有耐热和不稳定毒素以及志贺毒素基因的致病性大肠杆菌菌株,通过单次急性或较低的每日慢性剂量,在仔猪模型中诱导断奶后疾病的临床症状。通过确定粪便中病原体的脱落和定植、动物生长性能、细胞因子水平、粪便钙卫蛋白、组织学、粪便代谢组学和粪便微生物组变化来监测诱导的疾病状态。最具信息性的分析是病原体的定植和脱落、血清细胞因子、代谢组学和靶向宏基因组学,以确定菌群失调。未观察到胃肠道(GI)道的组织病理学变化和紧密连接渗漏,如粪便钙卫蛋白浓度所测量的。慢性给药与急性方案相似,这表明许多研究中使用的高剂量病原体可能不是必需的。这里提出的仔猪疾病模型可用于评估替代 PWD 治疗方案。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8d7c/8943154/79e182a82970/41598_2022_8446_Fig1_HTML.jpg

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