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Amino acid substitutions in VP2, VP1, and 2C attenuate a Coxsackievirus A16 in mice

Microb Pathog. 2020-11; 
Gaobo Zhang, Bing Hu, Yuqi Huo, Jia Lu, Jing Guo, Mi Deng, Pengfei Li, Weishan Wang, Li Li, Shengli Meng, Zejun Wang, Shuo Shen
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PCR Cloning and Subcloning … Nine pairs of primers were used to generate overlapping PCR fragments covering the whole genome for sequencing (Table 1). Sequencing was performed by GenScript (Nanjing) Co., Ltd, China. Table 1. Primers used for cloning and sequencing … Get A Quote

摘要

Coxsackievirus A16 (CVA16) is one of the major etiological agents of hand, foot and mouth disease (HFMD), a common acute infectious disease affecting infants and young children. Severe symptoms of the central nervous system may develop and even lead to death. Here, a plaque-purified CVA16 strain, L731-P1 (P1), was serially passaged in Vero cells for six times and passage 6 (P6) stock became highly attenuated in newborn mice. Genomic sequencing of the P1 and P6 revealed seven nucleotide substitutions at positions 1434 (C to U), 2744 (A to G), 2747 (A to G), 3161 (G to A), 3182 (A to G), 4968 (C to U), and 6064 (C to U). Six of these substitutions resulted in amino acid changes at VP2-T161 M, VP1-N102D, VP1-T103... More

关键词

Attenuating determinants, Coxsackievirus A16, Mutants