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感染改变新生犊牛肠道黏膜转录组:对上皮屏障和跨细胞转运系统的影响。

infection alters the intestinal mucosa transcriptome in neonatal calves: impacts on epithelial barriers and transcellular transport systems.

作者信息

Veshkini Arash, Kühn Christa, Dengler Franziska, Bachmann Lisa, Liermann Wendy, Helm Christiane, Ulrich Reiner, Delling Cora, Hammon Harald M

机构信息

Research Institute for Farm Animal Biology (FBN), Dummerstorf, Germany.

Friedrich-Loeffler-Institute, Greifswald-Insel Riems, Germany.

出版信息

Front Cell Infect Microbiol. 2024 Dec 4;14:1495309. doi: 10.3389/fcimb.2024.1495309. eCollection 2024.

Abstract

INTRODUCTION

is the most prevalent enteric protozoan parasite causing infectious diarrhea in neonatal calves worldwide with a direct negative impact on their health and welfare. This study utilized next-generation sequencing (NGS) to deepen our understanding of intestinal epithelial barriers and transport mechanisms in the pathophysiology of infectious diarrhea in neonatal calves, which could potentially unveil novel solutions for treatment.

METHODS

At day 1 of life, male Holstein-Friesian calves were either orally infected (n = 5) or not (control group, n = 5) with oocysts (in-house strain LE-01-Cp-15). On day 8 after infection, calves were slaughtered and jejunum mucosa samples were taken. The RNA was extracted from collected samples and subjected to sequencing. Differentially expressed genes (DEG) between the infected and CTRL groups were assessed using DESeq2 at a false discovery rate < 0.05 and used for gene ontology (GO) and pathway enrichment analysis in Cytoscape (v3.9.1).

RESULTS AND DISCUSSION

To study the pathophysiology of infectious diarrhea on intestinal permeability, 459 genes related to epithelial cell barrier integrity and paracellular and transmembrane transport systems were selected from 12,908 identified genes in mucus. Among, there were 61 increased and 109 decreased gene transcripts belonged to adhesion molecules (e.g. ADGRD1 and VCAM1), ATP-binding cassette (ABC, e.g. ABCC2 and ABCD1) and solute carrier (SLC, e.g. SLC28A2 and SLC38A3) transporters, and ion channels (e.g. KCNJ15). Our results suggest deregulation of cellular junctions and thus a possibly increased intestinal permeability, whereas deregulation of ABC and SLC transporters and ion channels may influence the absorption/secretion of amino acids, carbohydrates, fats, and organic compounds, as well as acid-based balance and osmotic hemostasis. Besides pathogen-induced gene expression alterations, part of the DEG may have been triggered or consequently affected by inflammatory mechanisms. The study provided a deeper understanding of the pathophysiology of infectious diarrhea in neonatal calves and the host-pathogen interactions at the transcript level. For further studies with a particular focus on the transport system, these results could lead to a new approach to elucidating pathophysiological regulatory mechanisms.

摘要

引言

是全球新生犊牛中引起感染性腹泻的最常见肠道原生动物寄生虫,对其健康和福利有直接负面影响。本研究利用下一代测序(NGS)来加深我们对新生犊牛感染性腹泻病理生理学中肠道上皮屏障和转运机制的理解,这可能会揭示新的治疗方法。

方法

在出生第1天,雄性荷斯坦 - 弗里生犊牛要么口服感染(n = 5),要么不感染(对照组,n = 5)卵囊(内部菌株LE - 01 - Cp - 15)。感染后第8天,屠宰犊牛并采集空肠黏膜样本。从采集的样本中提取RNA并进行测序。使用DESeq2以错误发现率<0.05评估感染组和对照组之间的差异表达基因(DEG),并用于在Cytoscape(v3.9.1)中进行基因本体(GO)和通路富集分析。

结果与讨论

为研究感染性腹泻对肠道通透性的病理生理学,从黏液中鉴定出的12,908个基因中选择了459个与上皮细胞屏障完整性以及细胞旁和跨膜转运系统相关的基因。其中,属于黏附分子(如ADGRD1和VCAM1)、ATP结合盒(ABC,如ABCC2和ABCD1)和溶质载体(SLC,如SLC28A2和SLC38A3)转运体以及离子通道(如KCNJ15)的基因转录本有61个增加,109个减少。我们的结果表明细胞连接失调,因此肠道通透性可能增加,而ABC和SLC转运体以及离子通道的失调可能影响氨基酸、碳水化合物、脂肪和有机化合物的吸收/分泌,以及酸碱平衡和渗透止血。除了病原体诱导的基因表达改变外,部分DEG可能已被炎症机制触发或因此受到影响。该研究提供了对新生犊牛感染性腹泻病理生理学以及转录水平上宿主 - 病原体相互作用的更深入理解。对于进一步特别关注转运系统的研究,这些结果可能会导致阐明病理生理调节机制的新方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b035/11656319/dfb5a9203bbf/fcimb-14-1495309-g001.jpg

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