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利用免疫功能正常的小鼠模型比较分析两种登革热病毒 2 型血清型引起的肝脏损伤。

Comparative analysis of liver involvement caused by two DENV-2 lineages using an immunocompetent murine model.

机构信息

Laboratory of Viral Morphology and Morphogenesis, Instituto Oswaldo Cruz, Fiocruz, Avenida Brasil 4365, Rio de Janeiro, RJ, 21040-900, Brazil.

Laboratory of Viral Immunology, Instituto Oswaldo Cruz, Fiocruz, Avenida Brasil, 4365, Rio de Janeiro, RJ, 21040-900, Brazil.

出版信息

Sci Rep. 2021 May 6;11(1):9723. doi: 10.1038/s41598-021-88502-2.

Abstract

Dengue (DEN) is the most prevalent arbovirus among humans, and four billion people live at risk of infection. The clinical manifestations of DEN are variable, and the disease may present subclinically or asymptomatically. A quarter of patients develop classical dengue (CD) or severe dengue (SD), which is potentially lethal and involves vascular permeability changes, severe hemorrhage and organ damage. The involvement of the liver is a fairly common feature in DEN, and alterations range from asymptomatic elevation of transaminases to acute liver failure. Since its introduction in Brazil in 1990, two strains of Dengue virus (DENV) serotype 2 (DENV-2) have been detected: Lineage I, which is responsible for an outbreak in 1991, and Lineage II, which caused an epidemic greater than the previous one and had a different epidemiological profile. To date, studies on different strains of the same serotype/genotype and their association with disease severity are scarce. In addition, one of the greatest challenges regarding the study of DEN pathogenesis and the development of drug and vaccine therapies is the absence of an animal model that reproduces the disease as it occurs in humans. The main goals of this study were to assess BALB/c mouse susceptibility experimentally infected by two distinct DENV-2 strains and characterize possible differences in the clinical signs and alterations induced in the liver resulting from those infections. Mice infected by the two DENV-2 lineages gained less weight than uninfected mice; however, their livers were slightly heavier. Increased AST and AST levels were observed in infected mice, and the number of platelets increased in the first 72 h of infection and subsequently decreased. Mice infected with both lineages presented leukocytosis but at different times of infection. The histopathological changes induced by both lineages were similar and comparable to the changes observed in DEN fatal cases. The viral genome was detected in two liver samples. The results demonstrate the susceptibility of BALB/c mice to both DENV-2 lineages and suggest that the changes induced by those strains are similar, although for some parameters, they are manifested at different times of infection.

摘要

登革热(DEN)是人类中最常见的虫媒病毒,有 40 亿人面临感染风险。DEN 的临床表现多种多样,疾病可能亚临床或无症状出现。四分之一的患者会出现典型登革热(CD)或重症登革热(SD),后者可能致命,涉及血管通透性改变、严重出血和器官损伤。肝脏受累是 DEN 的一个相当常见的特征,改变范围从转氨酶无症状升高到急性肝衰竭。自 1990 年在巴西引入以来,已检测到两种登革热病毒(DENV)血清型 2(DENV-2)株:引起 1991 年暴发的 I 系,以及比前一次更大规模流行且具有不同流行病学特征的 II 系。迄今为止,关于同一血清型/基因型的不同毒株及其与疾病严重程度的关联的研究很少。此外,研究 DEN 发病机制和开发药物及疫苗疗法所面临的最大挑战之一是缺乏可复制人类疾病的动物模型。本研究的主要目的是评估两种不同 DENV-2 株在 BALB/c 小鼠体内的实验感染易感性,并对由此引起的临床症状和肝脏改变的可能差异进行特征描述。感染两种 DENV-2 谱系的小鼠体重增加低于未感染的小鼠,但肝脏稍重。感染小鼠的 AST 和 ALT 水平升高,感染后 72 小时内血小板数量增加,随后减少。两种谱系感染的小鼠均出现白细胞增多,但在感染的不同时间。两种谱系引起的组织病理学变化相似,与致命性 DEN 病例观察到的变化相当。两种肝组织样本中均检测到病毒基因组。结果表明 BALB/c 小鼠对两种 DENV-2 谱系均易感,并提示这些株系引起的变化相似,尽管对于某些参数,它们在感染的不同时间表现出来。

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