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A nonpolio enterovirus with respiratory tropism causes poliomyelitis in intercellular adhesion molecule 1 transgenic mice

机译:具有呼吸嗜性的非脊髓灰质炎性肠病毒在细胞间粘附分子1转基因小鼠中引起脊髓灰质炎

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摘要

Coxsackievirus A21 (CAV21) is classified within the species Human enterovirus C (HEV-C) of the Enterovirus genus of picornaviruses. HEV-C share striking homology with the polioviruses (PV), their closest kin among the enteroviruses. Despite a high level of sequence identity, CAV21 and PV cause distinct clinical disease typically attributed to their differential use of host receptors. PV cause poliomyelitis, whereas CAV21 shares a receptor and a propensity to cause upper respiratory tract infections with the major group rhinoviruses. As a model for CAV21 infection, we have developed transgenic mice that express human intercellular adhesion molecule 1, the cell-surface receptor for CAV21. Surprisingly, CAV21 administered to these mice via the intramuscular route causes a paralytic condition consistent with poliomyelitis. The virus appears to invade the CNS by retrograde axonal transport, as has been demonstrated to occur in analogous PV infections. We detected human intercellular adhesion molecule 1 expression on both transgenic mouse and human spinal cord anterior horn motor neurons, indicating that members of HEV-C may share PV's potential to elicit poliomyelitis in humans.
机译:柯萨奇病毒A21(CAV21)被归类于小核糖核酸病毒肠病毒属的人类肠病毒C(HEV-C)。 HEV-C与脊髓灰质炎病毒(PV)具有惊人的同源性,脊髓灰质炎病毒是它们在肠病毒中最接近的亲属。尽管序列同一性水平很高,但CAV21和PV会引起明显的临床疾病,通常是由于宿主受体的差异使用所致。 PV引起脊髓灰质炎,而CAV21具有受体和倾向,可引起主要人群鼻病毒感染上呼吸道感染。作为CAV21感染的模型,我们开发了表达人细胞间粘附分子1(CAV21的细胞表面受体)的转基因小鼠。出人意料的是,通过肌内途径向这些小鼠施用的CAV21引起与脊髓灰质炎一致的麻痹状态。该病毒似乎是通过逆行轴突运输而侵入中枢神经系统的,这已在类似的PV感染中得到证实。我们在转基因小鼠和脊髓前角运动神经元上均检测到人细胞间粘附分子1的表达,这表明HEV-C成员可能共享PV引发人类脊髓灰质炎的潜力。

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