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Human SCARB2 transgenic mice as an infectious animal model for Enterovirus 71

机译:人类SCARB2转基因小鼠作为肠道病毒71的感染动物模型

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摘要

[[abstract]]Enterovirus 71 (EV71) and coxsackievirus (CVA) are the most common causative factors for hand, foot, and mouth disease (HFMD) and neurological disorders in children. Lack of a reliable animal model is an issue in investigating EV71-induced disease manifestation in humans, and the current clinical therapies are symptomatic. We generated a novel EV71-infectious model with hSCARB2-transgenic mice expressing the discovered receptor human SCARB2 (hSCARB2). The challenge of hSCARB2-transgenic mice with clinical isolates of EV71 and CVA16 resulted in HFMD-like and neurological syndromes caused by E59 (B4) and N2838 (B5) strains, and lethal paralysis caused by 5746 (C2), N3340 (C4), and CVA16. EV71 viral loads were evident in the tissues and CNS accompanied the upregulated pro-inflammatory mediators (CXCL10, CCL3, TNF-a, and IL-6), correlating to recruitment of the infiltrated T lymphocytes that result in severe diseases. Transgenic mice preimmunized with live E59 or the FI-E59 vaccine was able to resist the subsequent lethal challenge with EV71. These results indicate that hSCARB2-transgenic mice are a useful model for assessing anti-EV71 medications and for studying the pathogenesis induced by EV71.
机译:[[摘要]]肠病毒71(EV71)和柯萨奇病毒(CVA)是儿童手足口病(HFMD)和神经系统疾病的最常见致病因素。缺乏可靠的动物模型是研究EV71诱导的人类疾病表现的一个问题,目前的临床治疗是有症状的。我们用表达已发现的受体人类SCARB2(hSCARB2)的hSCARB2转基因小鼠产生了新型EV71感染模型。用临床分离株EV71和CVA16攻击hSCARB2转基因小鼠会导致E59(B4)和N2838(B5)菌株引起的HFMD样和神经系统综合症,以及5746(C2),N3340(C4)引起的致死性麻痹,和CVA16。 EV71病毒载量在组织中很明显,中枢神经系统伴随着上调的促炎性介质(CXCL10,CCL3,TNF-α和IL-6),这与导致严重疾病的浸润性T淋巴细胞的募集有关。用活E59或FI-E59疫苗预免疫的转基因小鼠能够抵抗随后的EV71致死性攻击。这些结果表明,hSCARB2转基因小鼠是评估抗EV71药物和研究EV71致病机理的有用模型。

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    Ho, W;

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