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作 者:杜江龙 薛宇佳 冶昡青 杨学才 曹欣[1] DU Jiang-long;XUE Yu-jia;YE Xuan-qing;YANG Xue-cai;CAO Xin(Life Science and Engineering College,Northivest University For Nationalities,Lanzhou,Gansu,730030,China)
机构地区:[1]西北民族大学生命科学与工程学院,甘肃兰州730030
出 处:《动物医学进展》2019年第4期112-115,共4页Progress In Veterinary Medicine
摘 要:对甲型肝炎病毒(HAV)发病机理和免疫调控的研究近年来重新受到关注。在发展中国家感染者的平均年龄增加,导致机制尚不明确的更严重的肝炎。而且,从HAV和丙型肝炎病毒(HCV)的免疫对比来看,这两种正链RNA病毒感染结果完全不同。HCV比HAV复制效率低,导致HCV蛋白表达量低,因此对IFN信号传导的拮抗作用较低。有研究发现循环的HAV病毒颗粒隐藏在膜里,导致先天免疫和抗体介导中和作用的激活。同时还考虑到CD4^+辅助T细胞对CD8^+细胞毒性T细胞对抗病毒免疫和肝损伤的作用,提出了一种非细胞毒性的HAV感染免疫控制模型。Despite the limited progress made in the past two to three decades,researches on the pathogenesis and immune regulation of Hepatitis A virus(HAV)have received renewed attention.From a public health point of view,the average age of infections in developing countries has increased,resulting in more severe hepatitis that mechanism is not clear.Furthermore,from the immunological comparison of HAV and hepatitis C virus(HCV),the results of these two positive-stranded RNA virus infections are quite different.HCV has a lower replication efficiency than HAV,resulting in low HCV protein expression and therefore low antagonism of IFN signaling.Studies have found that circulating HAV particles hidden in the membrane lead to innate immunity and antibody-mediated neutralization.The effect of CD4^+ helper cells on antiviral immunity and liver injury by CD8^+cytotoxic T cells were also considered,and a non-cytotoxic immune control model of HAV infection was also proposed.
分 类 号:S852.659.6[农业科学—基础兽医学]
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