比较归化小鼠模型设置揭示肠道黏膜不同的影响取决于微生物的经验。

Discovery immunology Pub Date : 2025-02-01 eCollection Date: 2025-01-01 DOI:10.1093/discim/kyaf002
Henriette Arnesen, Signe Birkeland, Harriet Stendahl, Klaus Neuhaus, David Masopust, Preben Boysen, Harald Carlsen
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引用次数: 0

摘要

关于临床前小鼠模型转化价值的担忧已经通过引入各种“归化”研究小鼠的方法得到解决,这些方法为它们提供了更多样化的微生物组和生理免疫反应。我们之前已经证明,“feralized”小鼠,即在类似农家院、微生物丰富的环境中饲养的近亲繁殖的实验室小鼠,表现出肠道微生物群的变化、成熟的免疫表型和降低的结直肠癌严重程度。类似的研究偶尔涉及与野生或宠物店饲养的小鼠共同居住,作为微生物供体整合特定物种的共生体和病原体。在多大程度上,这些不同的微生物暴露实践对所产生的小鼠表型至关重要尚不清楚。方法:在这里,我们首次对不同的归化实验小鼠的方法进行了并排比较:与野生捕获的家鼠合住,仅在类似农家院的栖息地进行归化,或将两者结合起来,以常规清洁实验小鼠为参考。结果:独立于该方法,归化的结肠粘膜微生物群被几种幽门螺杆菌定植,归化小鼠的结肠肠上皮细胞显示编码抗菌肽、粘液成分和活性氧产生酶的基因表达升高。他们进一步显示结肠固有层的常驻记忆T细胞和肠系膜淋巴结的效应记忆T细胞显著增加。这些参数最显著的变化发生在与野生捕获的小鼠共同饲养的小鼠中,而孵育的小鼠表现出介于实验室小鼠和共同饲养的小鼠之间的表型。结论:这些发现增强了我们对归化模型的建立及其对肠道屏障和免疫系统的影响的理解,从而有助于未来决定如何利用归化小鼠模型。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Comparison of naturalization mouse model setups uncover distinct effects on intestinal mucosa depending on microbial experience.

Introduction: Concerns regarding the translational value of preclinical mouse models have been addressed by introducing various approaches of 'naturalizing' research mice, which provide them with more diverse microbiomes and physiological immune responses. We have previously shown that 'feralized' mice, that is, inbred laboratory mice raised in a farmyard-like, microbe-rich environment exhibit a shifted gut microbiota, matured immunophenotype, and reduced severity of colorectal cancer. Similar studies occasionally involve co-housing with wild or pet-store-raised mice as microbial donors integrating species-specific commensals and pathogens. To what extent these different practices of microbial exposure are crucial for the resulting mouse phenotype remains unclear.

Methods: Here, we present the first side-by-side comparison of different methods to naturalize laboratory mice: co-housing with wild-caught house mice, feralization in a farmyard-like habitat only, or a combination of the two, with conventional clean laboratory mice as a reference.

Results: Independent of the method, the naturalized colon-mucosa microbiota, was colonized by several Helicobacter species, and the colonic intestinal epithelial cells of naturalized mice displayed elevated expression of genes encoding antimicrobial peptides, mucus components, and reactive-oxygen-species-producing enzymes. They further showed significantly increased resident memory T cells in the colonic lamina propria and effector memory T cells in the mesenteric lymph nodes. The most pronounced changes of these parameters occurred in mice co-housed with wild-caught mice, while feralized mice displayed phenotypes that were intermediate between laboratory and co-housed mice.

Conclusion: These findings enhance our understanding of naturalization model setups and effects on the gut barrier and immune system, thereby aiding future decisions on the utilization of naturalized mouse models.

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