D F Barreto, C M Takiya, M V Paes, J Farias-Filho, A T Pinhão, A M B Alves, S M Costa, O M Barth
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引用次数: 0
Abstract
The difficulty in studying dengue virus (DENV) infection in humans and in developing a virus vaccine is the absence of a suitable animal model which develops the full spectra of the Dengue haemorrhagic fever (DHF) and Dengue shock syndrome (DSS). Despite the fact that viruses have been found in various animal tissues, we isolated DENV from tissues of adult BALB/c mice, inoculated with DENV serotype 2 (DENV-2) obtained from human serum. Viruses were ultrastructurally identified and immunolocalized by immunofluorescence techniques in C6/36 mosquito cell cultures, inoculated with tissues (liver, lung, kidney and cerebellum) macerate supernatant from mice, 48 h post-infection (p.i.). These organs, collected at the same stage of infection, were examined histologically. The histopathological analysis revealed focal alterations in all tissues examined. Liver contained focal ballooned hepatocytes, but without modifying the average diameter of the majority of hepatocytes. Sinusoidal lumen was significantly diminished at this stage but portal and centrolobular veins became congested. Lungs exhibited hemorrhagic foci in the alveolar space, vascular congestion and focal alveolitis. Cerebellar tissue showed rare foci of neuronal compactation (Purkinje cells) and perivascular oedema. In kidneys it was observed an increase in glomerular volume with augmented endocapillary and mesangial cellularity, with reactivity to anti-IgM in all glomeruli of infected mice. In conclusion, DENV-2 was found in all tissues examined early in the evolution of infection. Presence of viruses in tissues has mainly led to hemodynamic alterations with generalized vascular congestion and increased permeability, and mast cell recruitment in lungs. The latter could participate in the vascular modifications in tissues.
研究登革病毒(DENV)在人类中的感染和开发病毒疫苗的困难在于缺乏一种合适的动物模型来开发登革出血热(DHF)和登革休克综合征(DSS)的全谱。尽管在各种动物组织中发现了病毒,但我们从BALB/c成年小鼠组织中分离出DENV,接种了从人血清中获得的DENV血清2型(DENV-2)。在感染后48 h (p.i),用C6/36蚊子细胞培养物接种小鼠组织(肝、肺、肾和小脑)浸渍上清,用免疫荧光技术对病毒进行超微结构鉴定和免疫定位。在感染的同一阶段收集这些器官,进行组织学检查。组织病理学分析显示所有检查组织的局灶性改变。肝脏包含局灶性肝细胞,但没有改变大多数肝细胞的平均直径。窦腔明显缩小,门静脉和小叶中心静脉充血。肺泡间隙出血灶、血管充血和局灶性肺泡炎。小脑组织显示罕见的神经元压实灶(浦肯野细胞)和血管周围水肿。在肾脏中,观察到肾小球体积增加,毛细血管内和系膜细胞增多,所有感染小鼠肾小球对抗igm具有反应性。总之,DENV-2在感染演变早期检测的所有组织中均有发现。病毒在组织中的存在主要导致血流动力学改变,包括全身血管充血和通透性增加,以及肺部肥大细胞的聚集。后者可以参与组织的血管修饰。