Shih Shin-Ru, Weng Kuo-Feng, Stollar Victor, Li Mei-Ling
Department of Medical Biotechnology and Laboratory Science, Chang Gung University, Tao-Yuan, Taiwan.
J Neurovirol. 2008 Jan;14(1):53-61. doi: 10.1080/13550280701798980.
Human glioblastoma cells (SF268) develop apoptosis, as characterized by DNA fragmentation and caspase activation, upon infection with Enterovirus 71 (EV71). To determine the step in virus replication that triggers apoptosis, the authors used ultraviolet (UV)-inactivated virus, inhibitors of protein and viral RNA synthesis, and chloroquine to block virus uncoating. Activation of caspase-3 was detected 24 h after infection with EV71 but not with UV-inactivated EV71. Apoptosis was inhibited when EV71-infected cells were treated with chloroquine, guanidine HCl, or cycloheximide. In summary, the authors studied the event(s) required to induce apoptosis in EV71-infected human glioblastoma cells, a subject much less studied than the possible role of viral proapoptotic genes, concluding that EV71 induces apoptosis in the infected SF268 cell in the presence of viral protein synthesis and virus replication, whereas virus adsorption, internalization, entry, uncoating, and viral RNA replication are all not required to trigger the apoptosis.
人胶质母细胞瘤细胞(SF268)在感染肠道病毒71型(EV71)后会发生凋亡,其特征为DNA片段化和半胱天冬酶激活。为了确定触发凋亡的病毒复制步骤,作者使用了紫外线(UV)灭活病毒、蛋白质和病毒RNA合成抑制剂以及氯喹来阻断病毒脱壳。感染EV71后24小时检测到半胱天冬酶-3激活,但感染UV灭活的EV71后未检测到。当用氯喹、盐酸胍或环己酰亚胺处理EV71感染的细胞时,凋亡受到抑制。总之,作者研究了在EV71感染的人胶质母细胞瘤细胞中诱导凋亡所需的事件,这一主题的研究远少于病毒促凋亡基因可能发挥的作用,得出结论:在存在病毒蛋白质合成和病毒复制的情况下,EV71在感染的SF268细胞中诱导凋亡,而病毒吸附、内化、进入、脱壳和病毒RNA复制均不是触发凋亡所必需的。
