Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

被引:0
|
作者
P C Huszthy
H Immervoll
J Wang
D Goplen
H Miletic
G E Eide
R Bjerkvig
机构
[1] NorLux Neuro-oncology Laboratory,Department of Biomedicine
[2] University of Bergen,Department of Pathology
[3] Helse-Vest,Department of Oncology and Medical Physics
[4] Haukeland University Hospital,Department of Public Health and Primary Health Care
[5] Section for Pathology,undefined
[6] The Gade Institute,undefined
[7] University of Bergen,undefined
[8] Haukeland University Hospital,undefined
[9] Haukeland University Hospital,undefined
[10] Centre for Clinical Research,undefined
[11] Haukeland,undefined
[12] University Hospital,undefined
[13] Epiforsk Research Group,undefined
[14] University of Bergen,undefined
[15] NorLux Neuro-oncology,undefined
[16] Centre Recherché de Public Santé,undefined
来源
Gene Therapy | 2010年 / 17卷
关键词
G207; oncolytic herpes viral vector; glioblastoma xenograft; proliferation index; apoptotic index; microvessel density;
D O I
暂无
中图分类号
学科分类号
摘要
The objective of the present study was to evaluate the cellular effects of the oncolytic HSV-1 based vector, G207, on the tumor microenvironment. We established progressively growing intracerebral xenografts in athymic nude rats generated from three different human GBM surgical specimens. The lesions were identified by MRI and subsequently injected with a concentrated vector stock. The animals were killed 10 or 30 days after G207 injection and the tumors were quantitatively evaluated for virus-induced changes in proliferation, apoptosis and vascularity. Moreover, we assessed vector spread as well as the infiltration pattern of CD68-positive inflammatory cells. In all G207-injected lesions, immunostaining identified widespread regions of viral infection and replication (plaques). Proliferation indices were significantly lower, whereas apoptotic counts were significantly elevated in plaques as compared with that in non-infected areas of the same lesions, as well as in corresponding control xenografts. Furthermore, there was a significant decline in the number of blood vessels in the plaques and the vascular area fractions were reduced. CD68-positive inflammatory cells accumulated in the plaques. The present study highlights the favorable cellular responses to G207 treatment seen from a clinical viewpoint, such as reduced tumor cell proliferation, more frequent events of tumor cell death and a strongly attenuated tumor vascular compartment. However, our results suggest that transduction of a significant volume of tumor tissue is essential, as these beneficial changes were only observed in areas of active viral replication, leaving non-transduced tumor tissues unaffected.
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页码:202 / 216
页数:14
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