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Comparative pathogenesis of US porcine epidemic diarrhea virus (PEDV) strain PC21A in conventional 9-day-old nursing piglets vs. 26-day-old weaned pigs

机译:美国猪流行性腹泻病毒(PEDV)株PC21A在常规9日龄断奶仔猪和26日龄断奶仔猪中的比较发病机理

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Our study demonstrated potential mechanisms by which porcine epidemic diarrhea virus (PEDV) infection induces greater disease severity of nursing vs. weaned conventional pigs. Twenty-six-day-old weaned [PEDV-inoculated (n = 11); mock (n = 9)] and 9-day-old nursing pigs [PEDV-inoculated (n = 9); mock (n = 11)] were inoculated orally [8.9 log(10) genomic equivalents (GE)/pig] with PC21A strain or mock (MEM). Pigs were monitored for clinical signs and PEDV RNA titers in feces and serum. For pathology and immunofluorescence staining for Ki67 (marker for crypt proliferation) and LGR5 (marker for crypt stem cell), 3-4 pigs were euthanized at postinoculation days (PIDs) 1, 3 and 5. Severe watery diarrhea and atrophic enteritis with moderate to high PEDV RNA titers in feces (7.5-12.2 log(10) GE/ml) and low viral RNA titers in serum (5.6-8.6 log(10) GE/ml were observed in all inoculated nursing piglets at PIDs 1-5. In contrast, weaned pigs did not show evidence of PEDV infection at PID 1. Pigs exhibited high fecal shedding titers at PIDs 2-5 and mild to severe atrophic enteritis at PIDs 3-5, indicating a longer incubation for PEDV infection. While uninoculated or inoculated 27-31-day-old pigs showed large numbers of Ki67- or LGR5-positive cells in the intestinal crypts, there was a lack of LGR5-positive cells and low proliferation of crypts in jejunum of uninoculated 10-14-day-old piglets, possibly causing a slower turnover of enterocytes; however, the number of LGR5-positive cells and proliferation of intestinal crypts increased remarkably at 3-5 days after inoculation. Biologic mediators that promote crypt stem cell regeneration would be targets to improve the intestinal epithelium renewal during PEDV infection. (C) 2015 Elsevier B.V. All rights reserved.
机译:我们的研究表明,与断奶常规猪相比,猪流行性腹泻病毒(PEDV)感染可引起更大的病害严重程度。二十六天大的仔猪断奶[接种PEDV(n = 11);模拟(n = 9)]和9天大的仔猪[接种PEDV(n = 9);模拟(n = 11)]口服PC21A株或模拟(MEM)接种[8.9 log(10)基因组当量(GE)/猪]。监测猪的粪便和血清中的临床体征和PEDV RNA滴度。对于Ki67(隐窝增生标记)和LGR5(隐窝干细胞标记)的病理学和免疫荧光染色,在接种后第1、3和5天对3-4头猪实施安乐死。严重的水样腹泻和萎缩性肠炎,中等至在PID 1-5处所有接种的哺乳仔猪中,粪便中PEDV RNA滴度较高(7.5-12.2 log(10)GE / ml)和血清中病毒RNA滴度较低(5.6-8.6 log(10)GE / ml)。相比之下,断奶的猪在PID 1时没有显示PEDV感染的迹象。猪在PID 2-5时表现出高的粪便脱落滴度,在PID 3-5时表现出轻度至重度萎缩性肠炎,表明PEDV感染的孵育时间更长。 27-31日龄的猪在肠道隐窝中显示大量Ki67或LGR5阳性细胞,未接种10-14天龄的仔猪空肠中LGR5阳性细胞缺乏且隐窝增殖低,可能会导致肠上皮细胞的更新较慢;但是,LGR5-阳性接种后3-5天,ve细胞和肠道隐窝的增殖显着增加。促进隐窝干细胞再生的生物介质将成为改善PEDV感染期间肠上皮更新的靶标。 (C)2015 Elsevier B.V.保留所有权利。

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