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Slow cycling intestinal stem cell and Paneth cell responses to Trichinella spiralis infection

机译:缓慢循环肠道干细胞和对Trichinella spiralis感染的Paneth细胞应答

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There is limited information regarding responses by slow cycling stem cells during T. spiralis-induced T-cell mediated intestinal inflammation and how such responses may relate to those of Paneth cells. Transgenic mice, in which doxycycline induces expression of histone 2B (H2B)-green fluorescent protein (GFP), were used. Following discontinuation of doxycycline ("chase" period), retention of H2B-GFP enabled the identification of slow cycling stem cells and long-lived Paneth cells. Inflammation in the small intestine (SI) was induced by oral administration of T. spiralis muscle larvae. Epithelia] retention of H2B-GFP per crypt cell position (cp) was studied following immunohistochemistry and using the Score and Wincrypts program. Compared to non-infected controls, there was significant reduction in the number of H2B-GFP-retaining stem cells in T. spiraiis-infected small intestines. H2B-GFP-retaining stem cells peaked at around cp 4 in control sections, but smaller peaks at higher cell positions (> 10) were seen in sections of inflamed small intestines. In the latter, there was a significant increase in the total number of Paneth cells, with significant reduction in H2B-GFP-retaining Paneth cells, but a marked increase in unlabelled (H2B-GFP-negative) Paneth cells. In conclusion, following T. spiralisinfection, putative slow cycling stem cell numbers were reduced. A marked increase in newly generated Paneth cells at the crypt base led to higher cell positions of the remaining slow cycling stem cells.
机译:通过在T.螺旋诱导的T细胞介导的肠炎症期间,通过缓慢循环干细胞的反应有限的信息有限。这种反应如何与甘蔗细胞的响应有关。使用转基因小鼠,其中,使用过辛杂环素诱导组蛋白2B(H2B)-Green荧光蛋白(GFP)的表达。在十二生酶停止后(“追逐”时期),H2B-GFP的保留使得能够鉴定缓慢的循环干细胞和长寿的Paneth细胞。小肠(Si)中的炎症是通过口服培养肌肉幼虫诱导的。上皮细胞每次隐藏细胞位置(CP)的上皮抑制是在免疫组化后进行研究,并使用得分和Wincrypts计划。与未感染的对照相比,T.Spiraiis感染的小肠中H2B-GFP保持干细胞的数量显着降低。 H2B-GFP保持干细胞在CP 4周围达到的对照部分,但在发炎的小肠的部分中观察到更高细胞位置(> 10)的较小峰。在后者中,PANETH细胞总数显着增加,具有显着降低的H2B-GFP保持群细胞,但未标记的(H2B-GFP-阴性)碱细胞的显着增加。总之,随后螺旋螺旋蛋白排出,降低了推定的缓慢循环干细胞数。在Crypt碱基的新产生的群集细胞的显着增加导致剩余慢循环干细胞的更高细胞位置。

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