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产生外泌体的滤泡相关上皮细胞不参与从绵羊(Ovis aries)肠道摄取 PrPd:一项超微结构研究。

Exosome-producing follicle associated epithelium is not involved in uptake of PrPd from the gut of sheep (Ovis aries): an ultrastructural study.

机构信息

Department of Basic Sciences and Aquatic Medicine, Norwegian School of Veterinary Science, Oslo, Norway.

出版信息

PLoS One. 2011;6(7):e22180. doi: 10.1371/journal.pone.0022180. Epub 2011 Jul 18.

Abstract

In natural or experimental oral scrapie infection of sheep, disease associated prion protein (PrP(d)) often first accumulates in Peyer's patch (PP) follicles. The route by which infectivity reaches the follicles is unknown, however, intestinal epithelial cells may participate in intestinal antigenic presentation by delivering exosomes as vehicles of luminal antigens. In a previous study using an intestinal loop model, following inoculation of scrapie brain homogenate, inoculum associated PrP(d) was detected by light microscopy shortly (15 minutes to 3.5 hours) after inoculation in the villous lacteals and sub-mucosal lymphatics. No PrP(d) was located within the follicle-associated epithelium (FAE), sub-FAE domes or the PP follicles. To evaluate this gut loop model and the transportation routes in more detail, we used electron microscopy (EM) to study intestinal tissues exposed to scrapie or control homogenates for 15 minutes to 10 days. In addition, immuno-EM was used to investigate whether exosomes produced in the FAE may possess small amounts of PrP(d) that were not detectable by light microscopy. This study showed that the integrity of the intestinal epithelium was sustained in the intestinal loop model. Despite prominent transcytotic activity and exosome release from the FAE of the ileal PP in sheep, these structures were not associated with transportation of PrP(d) across the mucosa. The study did not determine how infectivity reaches the follicles of PPs. The possibility that the infectious agent is transported across the FAE remains a possibility if it occurs in a form that is undetectable by the methods used in this study. Infectivity may also be transported via lymph to the blood and further to all other lymphoid tissues including the PP follicles, but the early presence of PrP(d) in the PP follicles during scrapie infection argues against such a mechanism.

摘要

在绵羊自然或实验性口腔瘙痒感染中,疾病相关朊病毒蛋白(PrP(d))通常首先在派伊尔氏结(PP)滤泡中积累。然而,感染性物质到达滤泡的途径尚不清楚,但是肠上皮细胞可能通过将外泌体作为腔抗原的载体来参与肠抗原呈递。在先前使用肠环模型的研究中,在用瘙痒症脑匀浆接种后,在用绒毛乳糜管和黏膜下淋巴管在接种后 15 分钟至 3.5 小时内,通过光镜检测到接种物相关的 PrP(d)。在滤泡相关上皮(FAE)、FAE 下穹窿或 PP 滤泡中未发现 PrP(d)。为了更详细地评估该肠环模型和运输途径,我们使用电子显微镜(EM)研究了暴露于瘙痒症或对照匀浆 15 分钟至 10 天的肠组织。此外,免疫电镜用于研究 FAE 中产生的外泌体是否可能具有少量无法通过光镜检测到的 PrP(d)。本研究表明,在肠环模型中,肠上皮的完整性得以维持。尽管绵羊回肠 PP 的 FAE 中存在明显的转胞吞作用和外泌体释放,但这些结构与 PrP(d)穿过黏膜的运输无关。该研究并未确定感染性物质如何到达 PP 滤泡。如果感染剂以本研究中使用的方法无法检测到的形式穿过 FAE,则其穿过 FAE 进行运输的可能性仍然存在。感染性物质也可能通过淋巴运送到血液,进一步运送到包括 PP 滤泡在内的所有其他淋巴组织,但在瘙痒感染期间 PP 滤泡中早期存在 PrP(d)反对这种机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4c18/3138767/24e3955e0a34/pone.0022180.g001.jpg

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