A mucus layer derived from porcine intestinal organoid air-liquid interface monolayer attenuates swine enteric coronavirus infection by antiviral activity of Muc2.

IF 4.5 1区 生物学 Q1 BIOLOGY BMC Biology Pub Date : 2024-12-23 DOI:10.1186/s12915-024-02094-7
Ning Yang, Yang Li, Yifei Cai, Yuanyuan Liu, Yunhang Zhang, Yuguang Fu, Chen Tan, Luc Willems, Guangliang Liu
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Abstract

Background: The mucus layer provides the first defense that keeps the epithelium free from microorganisms. However, the effect of the small intestinal mucus layer on pathogen invasion is still poorly understood, especially for swine enteric coronavirus. To better understand virus‒mucus layer‒intestinal epithelium interactions, here, we developed a porcine intestinal organoid mucus‒monolayer model under air‒liquid interface (ALI) conditions.

Results: We successfully established a differentiated intestinal organoid monolayer model comprising various differentiated epithelial cell types and a mucus layer under ALI conditions. Mass spectrometry analysis revealed that the mucus derived from the ALI monolayer shared a similar composition to that of the native small intestinal mucus. Importantly, our results demonstrated that the ALI monolayer exhibited lower infectivity of both TGEV and PEDV than did the submerged monolayer. To further confirm the impact of ALI mucus on coronavirus infection, mucus was collected from the ALI monolayer culture system and incubated with the viruses. These results indicated that ALI mucus treatment effectively reduced the infectivity of TGEV and PEDV. Additionally, Mucin 2 (Muc2), a major component of native small intestinal mucus, was found to be abundant in the mucus derived from the ALI monolayer, as determined by mass spectrometry analysis. Our study confirmed the potent antiviral activity of Muc2 against TGEV and PEDV infection. Considering the sialylation of Muc2 and the known sialic acid-binding activity of coronavirus, further investigations revealed that the sialic acid residues of Muc2 play a potential role in inhibiting coronavirus infection.

Conclusions: We established the porcine intestinal organoid mucus monolayer as a novel and valuable model for confirming the pivotal role of the small intestinal mucus layer in combating pathogen invasion. In addition, our findings highlight the significance of sialic acid modification of Muc2 in blocking coronavirus infections. This discovery opens promising avenues for the development of tailor-made drugs aimed at preventing porcine enteric coronavirus invasion.

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猪肠道类器官气液界面单层粘液层通过Muc2的抗病毒活性减弱猪肠道冠状病毒感染。
背景:黏液层提供了保护上皮免受微生物侵害的第一道防线。然而,小肠黏液层对病原体侵袭的影响仍然知之甚少,特别是对猪肠道冠状病毒。为了更好地理解病毒-黏液层-肠上皮的相互作用,我们建立了一个气液界面(ALI)条件下的猪肠道类器官黏液-单层模型。结果:我们成功建立了ALI条件下由多种分化上皮细胞类型和黏液层组成的肠类器官单层分化模型。质谱分析显示,来自ALI单层的黏液与天然小肠黏液的成分相似。重要的是,我们的结果表明,ALI单分子膜对TGEV和PEDV的感染性都低于浸没的单分子膜。为了进一步证实ALI黏液对冠状病毒感染的影响,从ALI单层培养系统中收集黏液并与病毒孵育。这些结果表明,ALI黏液治疗可有效降低TGEV和PEDV的传染性。此外,通过质谱分析发现,黏液蛋白2 (Muc2)是天然小肠黏液的主要成分,在来自ALI单层的黏液中含量丰富。我们的研究证实了Muc2对TGEV和PEDV感染的有效抗病毒活性。考虑到Muc2的唾液酰化和已知的冠状病毒唾液酸结合活性,进一步的研究表明Muc2的唾液酸残基在抑制冠状病毒感染中具有潜在的作用。结论:我们建立了猪小肠类器官黏液单层模型,为证实小肠黏液层在抵抗病原体侵袭中的关键作用提供了一种新的、有价值的模型。此外,我们的研究结果强调了唾液酸修饰Muc2在阻断冠状病毒感染中的意义。这一发现为开发旨在预防猪肠道冠状病毒入侵的量身定制药物开辟了有希望的途径。
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来源期刊
BMC Biology
BMC Biology 生物-生物学
CiteScore
7.80
自引率
1.90%
发文量
260
审稿时长
3 months
期刊介绍: BMC Biology is a broad scope journal covering all areas of biology. Our content includes research articles, new methods and tools. BMC Biology also publishes reviews, Q&A, and commentaries.
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