González L, Pitarch J L, Martin S, Thurston L, Moore J, Acín C, Jeffrey M
Animal Health and Veterinary Laboratories Agency (AHVLA), Penicuik, Midlothian EH26 0PZ, UK.
Facultad de Veterinaria, Universidad de Zaragoza, Zaragoza 50013, Spain.
J Comp Pathol. 2014 Jan;150(1):47-56. doi: 10.1016/j.jcpa.2013.06.006. Epub 2013 Sep 12.
The pathogenesis of scrapie in sheep after natural or oral exposure to the infectious agent generally involves the early accumulation of disease-associated prion protein (PrP(d)) in the lymphoreticular system (LRS). This phase is followed by neuroinvasion, for which two routes, ascending neural and haematogenous, have been postulated. The present study reports the use of immunohistochemistry to track the tissue progression of PrP(d) deposition in sheep of a single, highly scrapie-susceptible PrP genotype administered by the oral or conjunctival routes. Regardless of the route of infection, the earliest detection of PrP(d) was in gut- and pharynx-associated LRS tissues. Subsequently, the brain became PrP(d) positive simultaneously with other LRS tissues, but before the spinal cord and peripheral nervous tissues of the enteric, parasympathetic and sympathetic systems. The sites of initial PrP(d) accumulation in the brain were the dorsal motor nucleus of the vagus and the hypothalamus and their related circumventricular organs (the area postrema and the median eminence, respectively). These were the same for both routes of infection. Rapid progression to clinical disease was observed in sheep infected orally or conjunctivally, with definite signs of scrapie recorded at around 6 and 8 months after infection, respectively. Longer incubation periods in sheep infected by the conjunctival route were probably due to them receiving a lower dose than those infected orally. Irrespective of the route of infection, clinically affected sheep showed the same pathological phenotype (PrP(d) profile) and PrP(d) distribution throughout the brain. The identical peripheral and central pathogenesis observed in sheep of both groups suggests early dissemination of the infectious agent in the bloodstream and a common neuroinvasion pathway. The late involvement of the enteric and autonomic nervous system supports a haematogenous route of infection to the brain.
绵羊经自然感染或口服感染病原体后,羊瘙痒病的发病机制通常涉及疾病相关朊病毒蛋白(PrP(d))在淋巴网状系统(LRS)中的早期蓄积。此阶段之后是神经侵袭,对此已提出两种途径,即上行神经途径和血源性途径。本研究报告了利用免疫组织化学方法追踪PrP(d)沉积在单一、高度易感羊瘙痒病的PrP基因型绵羊体内的组织进展情况,这些绵羊通过口服或结膜途径给药。无论感染途径如何,最早检测到PrP(d)的部位是与肠道和咽部相关的LRS组织。随后,大脑与其他LRS组织同时变为PrP(d)阳性,但早于脊髓以及肠、副交感和交感神经系统的外周神经组织。大脑中PrP(d)最初蓄积的部位是迷走神经背运动核和下丘脑及其相关的室周器官(分别为最后区和正中隆起)。两种感染途径的情况均如此。经口服或结膜感染的绵羊均观察到迅速发展至临床疾病,分别在感染后约6个月和8个月记录到明确的瘙痒病体征。经结膜途径感染的绵羊潜伏期较长,可能是因为它们接受的剂量低于经口服感染的绵羊。无论感染途径如何,临床受影响的绵羊在整个大脑中均表现出相同的病理表型(PrP(d)谱)和PrP(d)分布。两组绵羊中观察到的相同的外周和中枢发病机制表明感染因子在血液中早期播散以及存在共同的神经侵袭途径。肠和自主神经系统的后期受累支持血源性感染至大脑的途径。
