Depletion of Peripheral Macrophages and Brain Microglia Increases Brain Tumor Titers of Oncolytic Viruses

Fulci, Giulia; Dmitrieva, Nina; Gianni, Davide; Fontana, Elisabeth J.; Pan, Xiaogang; Lu, Yanhui; Kaufman, Claire; Kaur, Balveen; Lawler, Sean E.; Lee, Robert J.; Marsh, Clay B.; Brat, Daniel J.; Rooijen, Nico van; Rachamimov, Anat Stemmer; Hochberg, Fred H.; Weissleder, Ralph; Martuza, Robert L.; Chiocca, E. Antonio

doi:10.1158/0008-5472.can-07-1063

Cited by 145 publications

(167 citation statements)

References 46 publications

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“…48 In contrast, accumulation of CD68-positive cells within the tumor bed was only observed around viral plaques. Whether the inflammatory cells were present due to natural killer cell-induced interferon-g or were they recruited by other means to phagocytose virus-lysed cells is not clear.…”

Section: Infiltration By Cd68-positive Cells In Areas Of Active Viralmentioning

confidence: 91%

Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

et al. 2009

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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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Section: Infiltration By Cd68-positive Cells In Areas Of Active Viralmentioning

confidence: 91%

Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

et al. 2009

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“…These studies demonstrated that cyclophosphamide is able to inhibit neutralizing antibody induction, macrophages, regulatory T cells (Tregs) induction and intratumoral interferon (IFN)-g production. [2][3][4][5][6][7][8] It remains to be determined, however, how much this approach will benefit cancer patients who often have already various degrees of 'pre-existing' immunosuppression due to disease and chemotherapy.…”

Section: Suppression Of Innate Immune Response Enhances Efficacymentioning

confidence: 99%

Gene therapy progress and prospects cancer: oncolytic viruses

Liu¹,

2008

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“…10,18 In vivo, the absence of the E3B immuno-modulatory genes has also been suggested to prevent efficient spread of this mutant. 19,20 More recently, improved oncolytic viruses have been engineered with smaller specific gene deletions to retain viral potency. Several of these mutants target the pRb/p16 pathway by deletion of the small E1ACR2 domain, essential for pRb binding and inactivation, and S-phase entry to support viral replication and propagation.…”

Section: Introductionmentioning

confidence: 99%

The oncolytic adenovirus AdΔΔ enhances selective cancer cell killing in combination with DNA-damaging drugs in pancreatic cancer models

et al. 2011

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Pancreatic adenocarcinomas are aggressive and frequently develop resistance to all current therapies. Replication-selective adenoviruses can overcome resistance to chemotherapeutics through their sensitizing effects on drug-induced cell killing. We previously found that adenovirus deleted in the anti-apoptotic E1B19K gene enhanced gemcitabine-induced apoptotis. Here we demonstrate that our engineered double-deleted AdDD mutant (deleted in the pRb-binding E1ACR2 region and E1B19K) selectively replicates and enhances cell killing in combination with DNA-damaging cytotoxic drugs in pancreatic cancer cells. Combinations of AdDD with gemcitabine, irinotecan or cisplatin resulted in two-to fourfold decreases in EC 50 (half maximal effective concentration) values and was more efficent than similar combinations with wild-type virus, the dl1520 (ONYX-015) and dl922-947 mutants. AdDD replication was impaired in normal bronchial human epithelial cells and did not sensitize the cells to drugs. Gemcitabine-insensitive AsPC-1, BxPC-3 and PANC-1 cells were efficiently killed by irinotecan in combination with AdDD. Suboptimal doses of AdDD and gemcitabine significantly prolonged time to tumor progression in two human pancreatic tumor xenograft in vivo models, PT45 and SUIT-2. We conclude that AdDD has low toxicity to normal cells while potently sensitizing pancreatic cancer cells to DNA-damaging drugs, and holds promise as an improved therapeutic strategy for pancreatic cancer.

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Depletion of Peripheral Macrophages and Brain Microglia Increases Brain Tumor Titers of Oncolytic Viruses

Cited by 145 publications

References 46 publications

Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

Cellular effects of oncolytic viral therapy on the glioblastoma microenvironment

Gene therapy progress and prospects cancer: oncolytic viruses

The oncolytic adenovirus AdΔΔ enhances selective cancer cell killing in combination with DNA-damaging drugs in pancreatic cancer models

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