Graduate Institute of Biomedical Science, Chang Gung University, Guishan, Taoyuan, Taiwan.
Novo Nordisk Research Centre, Department of Animal Facility, Discovery Biology, Beijing, China.
J Virol. 2019 May 15;93(11). doi: 10.1128/JVI.00183-19. Print 2019 Jun 1.
Enterovirus 71 (EV71) infection is generally associated with hand-foot-and-mouth disease (HFMD) and may cause severe neurological disorders and even death. An effective murine oral infection model for studying the pathogenesis of various clinical EV71 isolates is lacking. We developed a transgenic (Tg) mouse that expresses an EV71 receptor, that is, human scavenger receptor class B member 2 (hSCARB2), in a pattern highly similar to that of endogenous murine SCARB2 (mSCARB2) protein. A FLAG-tagged cDNA fragment composed of exons 3 to 12 was inserted into a murine gene-containing bacterial artificial chromosome (BAC) clone, and the resulting transgene was used for establishment of chimeric receptor-expressing Tg mice. Tg mice intragastrically (i.g.) infected with clinical isolates of EV71 showed neurological symptoms, such as ataxia and paralysis, and fatality. There was an age-dependent decrease in susceptibility to viral infection. Pathological characteristics of the infected Tg mice resembled those of encephalomyelitis in human patients. Viral infection was accompanied by microglial activation. Clodronate treatment of the brain slices from Tg mice enhanced viral replication, while lipopolysaccharide treatment significantly inhibited it, suggesting an antiviral role for microglia during EV71 infection. Taken together, this Tg mouse provides a model that closely mimics natural infection for studying EV71 pathogenesis and for evaluating the efficacy of vaccines or other antiviral drugs. The availability of a murine model of EV71 infection is beneficial for the understanding of pathogenic mechanisms and the development and assessment of vaccines and antiviral drugs. However, the lack of a murine oral infection model thwarted the study of pathogenesis induced by clinically relevant EV71 strains that are transmitted via the oral-oral or oral-fecal route. Our Tg mice could be intragastrically infected with clinically relevant EV71 strains in an efficient way and developed neurological symptoms and pathological changes strikingly resembling those of human infection. Moreover, these mice showed an age-dependent change in susceptibility that is similar to the human case. This Tg mouse, when combined with the use of other genetically modified mice, potentially contributes to studying the relationship between developmental changes in immunity and susceptibility to virus.
肠道病毒 71 型(EV71)感染通常与手足口病(HFMD)有关,可能导致严重的神经障碍甚至死亡。目前缺乏用于研究各种临床 EV71 分离株发病机制的有效小鼠口服感染模型。我们开发了一种转基因(Tg)小鼠,该小鼠在与人源性清道夫受体 B 类成员 2(hSCARB2)非常相似的模式下表达 EV71 受体,即内源性鼠源 SCARB2(mSCARB2)蛋白。一个由外显子 3 到 12 组成的 FLAG 标记的 cDNA 片段被插入到一个含有鼠源性基因的细菌人工染色体(BAC)克隆中,所得的转基因被用于建立表达嵌合受体的 Tg 小鼠。经口(i.g.)感染临床分离 EV71 的 Tg 小鼠表现出神经症状,如共济失调和瘫痪,并导致死亡。病毒感染的易感性随年龄的增长而降低。感染 Tg 小鼠的病理特征类似于人类患者的脑脊髓炎。病毒感染伴随着小胶质细胞的激活。用 clodronate 处理 Tg 小鼠的脑切片可增强病毒复制,而用脂多糖处理则显著抑制病毒复制,提示小胶质细胞在 EV71 感染过程中发挥抗病毒作用。总之,这种 Tg 小鼠为研究 EV71 发病机制和评估疫苗或其他抗病毒药物的疗效提供了一种模拟天然感染的模型。EV71 感染的小鼠模型的出现有利于理解致病机制,以及疫苗和抗病毒药物的开发和评估。然而,由于缺乏小鼠口服感染模型,阻碍了对通过口口或粪口途径传播的临床相关 EV71 株引起的发病机制的研究。我们的 Tg 小鼠可以有效地经口感染临床相关的 EV71 株,并表现出与人类感染非常相似的神经症状和病理变化。此外,这些小鼠的易感性随年龄的变化与人类病例相似。这种 Tg 小鼠与其他基因修饰小鼠结合使用,可能有助于研究免疫发育变化与病毒易感性之间的关系。
