Oncolytic Newcastle disease virus induces autophagy-dependent immunogenic cell death in lung cancer cells
文献类型: 外文期刊
第一作者: Ye, Tian
作者: Ye, Tian;Wei, Liwen;Piao, Haozhe;Ye, Tian;Zhang, Guirong;Ye, Tian;Jiang, Ke;Meng, Songshu;Barr, Martin P.;Barr, Martin P.;Xu, Qing;Xu, Qing;Xu, Qing;Ding, Chan
作者机构:
关键词: Newcastle disease virus; immunogenic cell death; apoptosis; autophagy; lung cancer
期刊名称:AMERICAN JOURNAL OF CANCER RESEARCH ( 影响因子:6.166; 五年影响因子:5.863 )
ISSN: 2156-6976
年卷期: 2018 年 8 卷 8 期
页码:
收录情况: SCI
摘要: In addition to direct oncolysis, oncolytic viruses trigger immunogenic cell death (ICD) and primes antitumor immunity. We have previously shown that oncolytic Newcastle disease virus (NDV), strain FMW (NDV/FMW), induces apoptosis and/or autophagy in cancer cells. In this study, we investigated whether oncolytic NDV can induce ICD in lung cancer cells and whether apoptosis or autophagy plays a role in NDV-triggered ICD. To this end, we examined cell surface expression of calreticulin (CRT) on NDV-infected lung cancer cells and measured ICD determinants, high mobility group box 1 (HMGB1), heat shock protein 70/90 (HSP70/90) and ATP in supernatants following viral infection. Flow cytometric analysis using anti-CRT antibody and PI staining of NDV-infected lung cancer cells showed an increase in the number of viable (propidium iodide-negative) cells, suggesting the induction of CRT exposure upon NDV infection. In addition, confocal and immunoblot analysis using anti-CRT antibody showed that an enhanced accumulation of CRT on the cell surface of NDV-infected cells, indicating the translocation of CRT to the cell membrane upon NDV infection. We further demonstrated that NDV infection induced the release of secreted HMGB1 and HSP70/90 by examining the concentrated supernatants of NDV-infected cells. Furthermore, pre-treatment with either the pan-caspase inhibitor z-VAD-FMK or the necrosis inhibitor Necrostain-1, had no impact on NDV-induced release of ICD determinants in lung cancer cells. Rather, depletion of autophagy-related genes in lung cancer cells significantly inhibited the induction of ICD determinants by NDV. Of translational importance, in a lung cancer xenograft model, treatment of mice with supernatants from NDV-infected cells significantly inhibited tumour growth. Together, these results indicate that oncolytic NDV is a potent ICD-inducer and that autophagy contributes to NDV-mediated induction of ICD in lung cancer cells.
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