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高效且可重现的大鼠肠道内蓝氏贾第鞭毛虫属感染实验

Efficient and reproducible experimental infections of rats with Blastocystis spp.

机构信息

Université Clermont Auvergne, 3iHP, CNRS, Laboratoire Microorganismes: Génome et Environnement, Clermont-Ferrand, France.

Université Clermont Auvergne, 3iHP, Inserm U1107, NeuroDol, Clermont-Ferrand, France.

出版信息

PLoS One. 2018 Nov 19;13(11):e0207669. doi: 10.1371/journal.pone.0207669. eCollection 2018.

Abstract

Although Blastocystis spp. infect probably more than 1 billion people worldwide, their clinical significance is still controversial and their pathophysiology remains poorly understood. In this study, we describe a protocol for an efficient and reproducible model of chronic infection in rats, laying the groundwork for future work to evaluate the pathogenic potential of this parasite. In our experimental conditions, we were unable to infect rats using vacuolar forms of an axenically cultivated ST4 isolate, but we successfully established chronic infections of 4 week-old rats after oral administration of both ST3 and ST4 purified cysts isolated from human stool samples. The infection protocol was also applied to 4 week-old C57BL/9, BALB/C and C3H mice, but any mouse was found to be infected by Blastocystis. Minimal cyst inoculum required for rat infection was higher with ST3 (105) than with ST4 (102). These results were confirmed by co-housing experiments highlighting a higher contagious potential of ST4 in rats compared to ST3. Finally, experiments mimicking fecal microbiota transfer from infected to healthy animals showed that Blastocystis spp. could easily infect a new host, even though its intestinal microbiota is not disturbed. In conclusion, our results provide a well-documented and robust rat model of Blastocystis chronic infection, reproducing "natural" infection. This model will be of great interest to study host parasite interactions and to better evaluate clinical significance of Blastocystis.

摘要

尽管 Blastocystis spp. 可能感染了全球超过 10 亿人,但它们的临床意义仍存在争议,其病理生理学仍知之甚少。在本研究中,我们描述了一种在大鼠中进行慢性感染的有效且可重复的模型方案,为评估该寄生虫的致病潜力奠定了基础。在我们的实验条件下,我们无法使用 ST4 体外培养的空泡形式感染大鼠,但我们成功地通过口服来自人类粪便样本的 ST3 和 ST4 纯化囊泡,建立了 4 周龄大鼠的慢性感染。该感染方案也应用于 4 周龄的 C57BL/9、BALB/C 和 C3H 小鼠,但没有一种小鼠被 Blastocystis 感染。与 ST4(102)相比,用于大鼠感染的最小囊泡接种物需要更高的 ST3(105)。这些结果通过共饲养实验得到了证实,该实验突出了 ST4 在大鼠中比 ST3 具有更高的传染性。最后,模拟从感染动物到健康动物的粪便微生物群转移的实验表明,Blastocystis spp. 可以很容易地感染新宿主,即使其肠道微生物群没有受到干扰。总之,我们的结果提供了一种经过充分记录和稳健的大鼠 Blastocystis 慢性感染模型,复制了“自然”感染。该模型将非常有助于研究宿主-寄生虫相互作用,并更好地评估 Blastocystis 的临床意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/db8e/6242359/cf89ecaf2d9f/pone.0207669.g001.jpg

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