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脊髓内接种脊髓灰质炎病毒受体转基因小鼠中的脊髓灰质炎

Poliomyelitis in intraspinally inoculated poliovirus receptor transgenic mice.

作者信息

Deatly A M, Coleman J W, McMullen G, McAuliffe J M, Jayarama V, Cupo A, Crowley J C, McWilliams T, Taffs R E

机构信息

Viral Vaccine Research, Wyeth-Lederle Vaccines and Pediatrics, 401 North Middletown Road, Pearl River, New York, 10965, USA.

出版信息

Virology. 1999 Mar 15;255(2):221-7. doi: 10.1006/viro.1998.9574.

Abstract

Mice transgenic with the human poliovirus receptor gene develop clinical signs and neuropathology similar to those of human poliomyelitis when neurovirulent polioviruses are inoculated into the central nervous system (CNS). Factors contributing to disease severity and the frequencies of paralysis and mortality include the poliovirus strain, dose, and gender of the mouse inoculated. The more neurovirulent the virus, as defined by monkey challenge results, the higher the rate of paralysis, mortality, and severity of disease. Also, the time to disease onset is shorter for more neurovirulent viruses. Male mice are more susceptible to polioviruses than females. TGM-PRG-3 mice have a 10-fold higher transgene copy number and produce 3-fold more receptor RNA and protein levels in the CNS than TGM-PRG-1 mice. CNS inoculations with type III polioviruses differing in relative neurovirulence show that these mouse lines are similar in disease frequency and severity, demonstrating that differences in receptor gene dosage and concomitant receptor abundance do not affect susceptibility to infection. However, there is a difference in the rate of accumulation of clinical signs. The time to onset of disease is shorter for TGM-PRG-3 than TGM-PRG-1 mice. Thus, receptor dosage affects the rate of appearance of poliomyelitis in these mice.

摘要

当将神经毒力强的脊髓灰质炎病毒接种到中枢神经系统(CNS)时,转染了人脊髓灰质炎病毒受体基因的小鼠会出现与人类脊髓灰质炎相似的临床症状和神经病理学表现。影响疾病严重程度、瘫痪频率和死亡率的因素包括脊髓灰质炎病毒株、剂量以及接种小鼠的性别。根据猴体攻击试验结果定义,病毒的神经毒力越强,瘫痪率、死亡率和疾病严重程度就越高。此外,神经毒力越强的病毒,发病时间越短。雄性小鼠比雌性小鼠对脊髓灰质炎病毒更易感。与TGM-PRG-1小鼠相比,TGM-PRG-3小鼠的转基因拷贝数高10倍,在中枢神经系统中产生的受体RNA和蛋白质水平多3倍。用相对神经毒力不同的III型脊髓灰质炎病毒进行中枢神经系统接种表明,这些小鼠品系在疾病发生率和严重程度方面相似,这表明受体基因剂量和相应的受体丰度差异并不影响感染易感性。然而,临床症状的累积速度存在差异。TGM-PRG-3小鼠的发病时间比TGM-PRG-1小鼠短。因此,受体剂量影响这些小鼠中脊髓灰质炎的出现速度。

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