JNK-deficiency enhanced oncolytic vaccinia virus replication and blocked activation of double-stranded RNA-dependent protein kinase

被引:24
作者
Hu, W. [1 ,2 ]
Hofstetter, W. [1 ]
Guo, W. [1 ]
Li, H. [1 ]
Pataer, A. [1 ]
Peng, H. H. [1 ]
Guo, Z. S. [3 ,4 ]
Bartlett, D. L. [3 ,4 ]
Lin, A. [5 ]
Swisher, S. G. [1 ]
Fang, B. [1 ]
机构
[1] Univ Texas Houston, MD Anderson Canc Ctr, Dept Thorac & Cardiovasc Surg, Houston, TX 77030 USA
[2] Zhejiang Univ, Sir Run Run Shaw Hosp, Dept Colorectal Surg, Hangzhou, Zhejiang, Peoples R China
[3] Univ Pittsburgh, Inst Canc, Div Surg Oncol, Dept Surg, Pittsburgh, PA USA
[4] Univ Pittsburgh, Sch Med, Pittsburgh, PA USA
[5] Univ Chicago, Ben May Inst Canc Res, Chicago, IL 60637 USA
来源
CANCER GENE THERAPY | 2008年 / 15卷 / 09期
关键词
JNK; PKR; virotherapy; cancer; virus replication; apoptosis;
D O I
10.1038/cgt.2008.32
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
Vaccinia virus has recently been used as an expression vector for gene delivery and an oncolytic agent for cancer therapy. Although it has been established that interferon-induced double-stranded RNA (dsRNA)-activated protein kinase (PKR) and RNase L interfere with viral replication, little else is known about the other host factors that might affect viral replication and virus-mediated host cell killing. In this study, we evaluated the roles of c-Jun NH2-terminal kinase (JNK) in oncolytic vaccinia virus replication and vaccinia virus-mediated host cell killing. We found that JNK knockout mouse embryonic fibroblasts (MEFs) were more susceptible to oncolytic vaccinia virus infection than wild-type MEFs. Moreover, viral replication and the production of infectious viral progeny were up to 100-fold greater in JNK-deficient MEFs than in wild-type MEFs. A similar result was observed for wild-type vaccinia virus. The increased killing of infected cells and the production of viral progeny was also observed in wild-type MEFs that had been treated with JNK inhibitors and in human colon cancer cells that had been transfected with dominant-negative JNK constructs. Moreover, testing on several human lung cancer cell lines and HeLa cells showed an inverse correlation between levels of JNK expression and susceptibility to oncolytic vaccinia virus. Our study also revealed that oncolytic virus infection-mediated PKR activation was blocked or diminished in JNK-deficient MEFs. The adenovirus-mediated ectopic expression of human PKR in JNK-deficient MEFs reduced vaccinia virus replication to the levels observed in wild-type MEFs, indicating that JNK is required for vaccinia virus to efficiently activate PKR. Our results demonstrated that the cellular status of JNK function can dramatically affect oncolytic vaccinia virus replication and vaccinia virus-mediated host cell killing. This finding may enable further improvements in oncolytic virotherapy using vaccinia virus.
引用
收藏
页码:616 / 624
页数:9
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