柯萨奇病毒A组16型VP1-145位氨基酸变异影响对硫酸乙酰肝素结合能力的初步探究  

作　　者：宗彦君 孙甜甜 王蕊 刘莹 李冀琛 孙强[2,3] 刘志军[1] 张勇[2,3] ZONG Yanjun;SUN Tiantian;WANG Rui;LIU Ying;LI Jichen;SUN Qiang;LIU Zhijun;ZHANG Yong(Weifang Medical College,Weifang 261053,China;National Key Laboratory of Traceability and Intelligent Decision-making for Infectious Diseases(NITFID),National Institute for Viral Disease Control and Prevention,Chinese Center for Disease Control and Prevention,Beijing 102206,China;National Polio Laboratory,National Health Commission Key Laboratory for Laboratory Biosafety,National Institute for Viral Disease Control and Prevention,Chinese Center for Disease Control and Prevention,Beijing 102206,China)

机构地区：[1]潍坊医学院,潍坊261053 [2]传染病溯源预警和智能决策全国重点实验室,中国疾病预防控制中心病毒病预防控制所,北京102206 [3]国家脊髓灰质炎实验室,国家卫生健康委员会实验室生物安全重点实验室,中国疾病预防控制中心病毒病预防控制所,北京102206

出　　处：《病毒学报》2024年第2期346-356,共11页Chinese Journal of Virology

基　　金：国家重点研究发展计划项目(项目号:2021YFC2302003),题目:病毒监测网络数据标准及数据平台建设;山东省自然科学基金(项目号:ZR2019MC059),题目:巨细胞病毒基因UL138IE1和IE2诱导的动脉粥样硬化机制研究。

摘　　要：柯萨奇病毒A组16型(Coxsackievirus A16,CVA16)与肠道病毒A71型(Enterovirus A71,EV-A71)是国内导致手足口病的重要病原体,二者同源,来自共同祖先,基因组结构相同,并且均使用硫酸乙酰肝素(Heparan sulfate,HS)作为吸附受体。本研究基于EV-A71的VP1-145位氨基酸位点的相关研究结果,分析CVA16的VP1-145氨基酸差异,选取3株中国流行的,在该位点具有差异的CVA16,进行对HS结合能力影响的研究。使用不同浓度肝素酶Ⅰ处理人横纹肌肉瘤(Human rhabdomyosarcoma,RD)细胞,比较不同CVA16株对肝素酶Ⅰ处理前后的RD细胞的吸附能力,以及接种后12h,24h,48h后各毒株在RD细胞的复制情况。结果表明,在使用5mIU/mL和10mIU/mL浓度肝素酶Ⅰ水解RD细胞表面的HS后,VP1-145氨基酸位点为甘氨酸(Glycine,G)的CVA16对RD细胞的吸附能力下降,其下降程度与肝素酶Ⅰ的作用浓度呈正相关,且影响了后续12h,24h,48h病毒在RD细胞中的复制,其差异具有统计学意义(P<0.05)。而VP1-145氨基酸位点为谷氨酸(Glutamic acid,E)的两株CVA16均未观察到此种趋势。为了进一步探究该种结合能力的差异与病毒致病力之间的关系,对三株病毒进行2日龄ICR乳鼠感染实验。通过观察乳鼠生存率、临床评分、体重变化,来评估不同CVA16株在小鼠感染模型中的致病力差异。结果表明,CVA16(VP1-145E)的致病力明显强于CVA16(VP1-145G)。后对三株病毒进行全基因组测序,测序结果显示,除VP1-145位点外,三株CVA16还存在其他的差异位点,故后续我们又通过反向遗传学拯救病毒,对VP1-145位点的作用机制进行了进一步的探讨。本研究结果证实,VP1-145位点的氨基酸变异会影响CVA16与HS的结合能力,145位点为E的病毒,其与HS的结合能力较差,当145位点由E突变至G时,病毒与HS的结合能力增强,其与RD细胞的结合能力受到肝素酶Ⅰ的影响。本研究为CVA16毒力位点与致病机制的研究提供了一定的理论基础Coxsackievirus A16(CVA16)and enterovirus A71(EV-A71)are important pathogens causing hand,foot and mouth disease(HFMD)in China.They are homologous and from a common ancestor,with the same genome structure,and both use heparan sulfate(HS)as an adsorption receptor.Based on the research regarding of VP1-145 amino acid site of EV-A71,three strains of CVA16 with differences in VP1-145 amino acid site selected in this study that were prevalent in China to study the impact of VP1-145 amino acid site variation on HS binding ability.Human rhabdomyosarcoma(RD)cells were treated with different concentrations of heparinase I,and the adsorption ability of different CVA16 strains on RD cells before and after heparinase I treatment was compared,as well as the replication of each strain on RD cells 12h,24h and 48h after inoculation.The results showed that under the treatment of heparinase I at concentrations of 5 mIU/mL and 10 mIU/mL,the adsorption ability of CVA16 with the amino acid Glycine(G)at VP1-145 site to RD cells decreased,and the virus titer decreased at 12h,24h and 48h after inoculation.The degree of decrease was positively correlated with the concentration of heparinase I,and the difference was statistically significant(P<0.05).However,no such trend was observed in the two CVA16 strains with glutamic acid(E)at VP1-145 site.In order to further explore the relationship between the differences in binding ability and the virulence of the viruses,two-day-old ICR suckling mice infection experiment was conducted using three virus strains.To evaluate the differences in pathogenicity of different CVA16 strains in mouse infection models,the survival rate,clinical scores,and weight change of suckling mice were observed.The results showed that the pathogenicity of CVA16(VP1-145E)was significantly stronger than that of CVA16(VP1-145G).Then the whole genome sequencing of the three CVA16 strains showed that there were other different sites in addition to the VP1-145 site.Therefore,we rescued the virus by reverse genetics and further

关 键 词：柯萨奇病毒A组16型 VP1-145位点 硫酸乙酰肝素 致病力 

分 类 号：R373.2[医药卫生—病原生物学]