Chimeric HCMV/HSV-1 and Δγ134.5 oncolytic herpes simplex virus elicit immune mediated antigliomal effect and antitumor memory

被引:24
|
作者
Ghonime, Mohammed G. [1 ]
Jackson, Josh [2 ]
Shah, Amish [2 ]
Roth, Justin [2 ]
Li, Mao [2 ]
Saunders, Ute [2 ]
Coleman, Jennifer [3 ]
Gillespie, G. Yancey [3 ]
Markert, James M. [2 ,3 ]
Cassady, Kevin A. [1 ,4 ,5 ]
机构
[1] Nationwide Childrens Hosp, Ctr Childhood Canc & Blood Disorders, Res Inst, Columbus, OH USA
[2] Univ Alabama Birmingham, Sch Med, Birmingham, AL USA
[3] Univ Alabama Birmingham, Dept Neurosurg, Birmingham, AL USA
[4] Nationwide Childrens Hosp, Dept Pediat Infect Dis, Columbus, OH USA
[5] Ohio State Univ, Coll Med, Columbus, OH 43210 USA
来源
TRANSLATIONAL ONCOLOGY | 2018年 / 11卷 / 01期
关键词
HUMAN CYTOMEGALOVIRUS IRS1; NEUROVIRULENCE; REPLICATION; GLIOMA; INFECTION; RESECTION; MUTANTS; PROTEIN; GROWTH; CELLS;
D O I
10.1016/j.tranon.2017.10.005
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Malignant gliomas are the most common primary brain tumor and are characterized by rapid and highly invasive growth. Because of their poor prognosis, new therapeutic strategies are needed. Oncolytic virotherapy (OV) is a promising strategy for treating cancer that incorporates both direct viral replication mediated and immune mediated mechanisms to kill tumor cells. C134 is a next generation Delta gamma(1)34.5 oHSV-1 with improved intratumoral viral replication. It remains safe in the CNS environment by inducing early IFN signaling which restricts its replication in non-malignant cells. We sought to identify how C134 performed in an immunocompetent tumor model that restricts its replication advantage over first generation viruses. To achieve this we identified tumors that have intact IFN signaling responses that restrict C134 and first generation virus replication similarly. Our results show that both viruses elicit a T cell mediated anti-tumor effect and improved animal survival but that subtle difference exist between the viruses effect on median survival despite equivalent in vivo viral replication. To further investigate this we examined the anti-tumor activity in immunodeficient mice and in syngeneic models with re-challenge. These studies show that the T cell response is integral to C134 replication independent anti-tumor response and that OV therapy elicits a durable and circulating anti-tumor memory. The studies also show that repeated intratumoral administration can extend both OV anti-tumor effects and induce durable anti-tumor memory that is superior to tumor antigen exposure alone.
引用
收藏
页码:86 / 93
页数:8
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