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不同来源小鼠真核病毒组的特征分析

Characterization of the Eukaryotic Virome of Mice from Different Sources.

作者信息

Zhang Chunye, Burch Matt, Wylie Kristine, Herter Brandi, Franklin Craig L, Ericsson Aaron C

机构信息

Department of Veterinary Pathobiology, University of Missouri, Columbia, MO 65211, USA.

Department of Pediatrics, Washington University, St. Louis, MO 63110, USA.

出版信息

Microorganisms. 2021 Sep 30;9(10):2064. doi: 10.3390/microorganisms9102064.

Abstract

Accumulating studies show that the host microbiome influences the development or progression of many diseases. The eukaryotic virome, as a key component of the microbiome, plays an important role in host health and disease in humans and animals, including research animals designed to model human disease. To date, the majority of research on the microbiome has focused on bacterial populations, while less attention has been paid to the viral component. Members of the eukaryotic virome interact with the commensal bacterial microbiome through trans-kingdom interactions, and influence host immunity and disease phenotypes as a collective microbial ecosystem. As such, differences in the virome may affect the reproducibility of animal models, and supplementation of the virome may enhance the translatability of animal models of human disease. However, there are minimal empirical data regarding differences in the virome of mice from different commercial sources. Our hypotheses were that the mice obtained from pet store sources and lab mice differ in their eukaryotic virome, and that lab mice from different sources would also have different viromes. To test this hypothesis, the ViroCap platform was used to characterize the eukaryotic virome in multiple tissues of mice from different sources including three sources of laboratory mice and two pet stores. As expected, pet store mice harbored a much greater diversity within the virome compared to lab mice. This included an ostensibly novel norovirus strain identified in one source of these mice. Viruses found in both laboratory and pet store populations included four strains of endogenous retroviruses and murine astrovirus with the latter being restricted to one source of lab mice. Considering the relatively high richness virome within different samples from healthy humans, these data suggest that mouse models from alternative sources may be more translational to the human condition. Moreover, these data demonstrate that, by characterizing the eukaryotic murine virome from different sources, novel viruses may be identified for use as field strains in biomedical research.

摘要

越来越多的研究表明,宿主微生物群会影响许多疾病的发生或发展。真核病毒组作为微生物群的关键组成部分,在人类和动物(包括用于模拟人类疾病的实验动物)的宿主健康和疾病中发挥着重要作用。迄今为止,大多数关于微生物群的研究都集中在细菌群体上,而对病毒成分的关注较少。真核病毒组的成员通过跨界相互作用与共生细菌微生物群相互作用,并作为一个集体微生物生态系统影响宿主免疫和疾病表型。因此,病毒组的差异可能会影响动物模型的可重复性,补充病毒组可能会提高人类疾病动物模型的可转化性。然而,关于不同商业来源小鼠病毒组差异的实证数据极少。我们的假设是,从宠物店获得的小鼠和实验室小鼠的真核病毒组不同,并且来自不同来源的实验室小鼠也会有不同的病毒组。为了验证这一假设,我们使用ViroCap平台对来自不同来源(包括三种实验室小鼠来源和两家宠物店)的小鼠多个组织中的真核病毒组进行了表征。正如预期的那样,与实验室小鼠相比,宠物店小鼠的病毒组具有更高的多样性。这包括在其中一个来源的这些小鼠中发现的一种表面上全新的诺如病毒株。在实验室和宠物店小鼠群体中都发现的病毒包括四种内源性逆转录病毒株和鼠星状病毒,后者仅限于一种实验室小鼠来源。考虑到健康人类不同样本中病毒组的丰富度相对较高,这些数据表明来自其他来源的小鼠模型可能更适合转化为人类疾病模型。此外,这些数据表明,通过表征来自不同来源的真核小鼠病毒组,可以鉴定出新的病毒用作生物医学研究中的野外毒株。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ebbb/8538372/a7cba7772438/microorganisms-09-02064-g001.jpg

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