Systemic Therapy of Spontaneous Prostate Cancer in Transgenic Mice with Oncolytic Herpes Simplex Viruses

Varghese, Susan; Rabkin, Samuel D.; Nielsen, G. Petur; MacGarvey, Usha; Liu, Renbin; Martuza, Robert L.

doi:10.1158/0008-5472.can-07-0674

Cited by 47 publications

(42 citation statements)

References 48 publications

(62 reference statements)

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“…We propose that upon differentiation, DNMT activation leads to CpG island methylation, which in turn causes loss of repressor protein binding. This is consistent with results showing that following dense DNA hypermethylation of promoters, EZH2 is no longer required to maintain DNA methylation and therefore is released (44). A combination of activating transcription factors that begin to be expressed in CXCR4ϩ cells, including transcription factors that activate the FoxA2 enhancer (22), together with alterations in chromatin modifications such as H3K27 trimethylation (repressive) and H3 acetylation or H3K4 dimethylation (activating) may then lead to activation of FoxA2 gene expression (Fig.…”

Section: Discussionsupporting

confidence: 90%

Paradoxical Role of DNA Methylation in Activation of FoxA2 Gene Expression during Endoderm Development

Halpern

Vana

Walker

2014

Journal of Biological Chemistry

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Section: Discussionsupporting

confidence: 90%

Paradoxical Role of DNA Methylation in Activation of FoxA2 Gene Expression during Endoderm Development

Halpern

Vana

Walker

2014

Journal of Biological Chemistry

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“…Preclinical and clinical studies argue that prior immunity to HSV does not represent an obstacle. Thus, intravenously administered ␥ 1 34.5-deleted HSV was effective in prostate and pulmonary tumor models, irrespective of whether mice were previously immunized with HSV (35,36). In phase I clinical trials, ␥ 1 34.5-deleted HSV was administered i.t.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of human tumor growth in mice by an oncolytic herpes simplex virus designed to target solely HER-2-positive cells

Menotti

Nicoletti

Gatta

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

126

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Oncolytic virotherapy exploits the ability of viruses to infect, replicate into, and kill tumor cells. Among the viruses that entered clinical trials are HSVs. HSVs can be engineered to become tumorspecific by deletion of selected genes or retargeting to tumorspecific receptors. A clinically relevant surface molecule is HER-2, hyperexpressed in one fourth of mammary and ovary carcinomas, and associated with high metastatic ability. As a previously undescribed strategy to generate HSV recombinants retargeted to HER-2 and detargeted from natural receptors, we replaced the Ig-folded core in the receptor-binding virion glycoprotein gD with anti-HER-2 single-chain antibody. The recombinant entered cells solely via HER-2 and lysed HER-2-positive cancer cells. Because of the high specificity, its safety profile in i.p. injected mice was very high, with a LD 50 >5 ؋ 10 8 pfu, a figure at least 10,000-fold higher than that of corresponding WT-gD carrying virus (LD 50 Ϸ 5 ؋ 10 4 pfu). When administered intratumorally to nude mice bearing HER-2-hyperexpressing human tumors, it strongly inhibited progressive tumor growth. The results provide a generally applicable strategy to engineer HSV recombinants retargeted to a wide range of receptors for which a single-chain antibody is available, and show the potential for retargeted HSV to exert target-specific inhibition of human tumor growth. Therapy with HER-2-retargeted oncolytic HSV could be effective in combined or sequential protocols with monoclonal antibodies and small inhibitors, particularly in patients resistant to HER-2-targeted therapy because of alterations in HER-2 signaling pathway, or against brain metastases inaccessible to anti-HER-2 antibodies. mammary carcinoma ͉ ovary carcinoma ͉ retarget ͉ tropism

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“…To date, this is the first efficacious treatment for TRAMP mice at an advanced stage of disease (29,30,(33)(34)(35) and the only report of the cure of spontaneous tumors with unmanipulated, unselected donor T lymphocytes. These findings are of particular relevance in the TRAMP model in which the genetic pressure for cancer recurrence is particularly strong (11) and able to induce unresponsiveness of high-affinity tumor-specific T cells (36,37).…”

Section: Discussionmentioning

confidence: 99%

Concomitant Tumor and Minor Histocompatibility Antigen–Specific Immunity Initiate Rejection and Maintain Remission from Established Spontaneous Solid Tumors

et al. 2010

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Nonmyeloablative hematopoietic cell transplantation can cure patients with hematologic malignancies but has reported limited success against solid tumors. This is possibly because of profound peripheral tolerance mechanisms and/or suboptimal tumor recognition by effector T lymphocytes. We report that in mice developing spontaneous prostate cancer, nonmyeloablative minor histocompatibility mismatched hematopoietic stem cell transplantation, and donor lymphocyte infusion of unmanipulated lymphocytes combined with posttransplant tumor-specific vaccination circumvents tumor-specific tolerance, allowing acute tumor rejection and the establishment of protective immunosurveillance. Although donor-derived tumor-specific T cells readily differentiated into effector cells and infiltrated the tumor soon after infusion, they were alone insufficient for tumor eradication, which instead required the concomitance of minor histocompatibiltiy antigen-specific CD8 + T-cell responses. The establishment of protective immunosurveillance was best induced by posttransplant tumor-specific vaccination. Hence, these results provide the proof of principle that tumor-specific T-cell responses have to be harnessed together with minor histocompatibility responses and sustained by posttransplant tumor-specific vaccination to improve the efficacy of allotransplantion for the cure of solid tumors.

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Systemic Therapy of Spontaneous Prostate Cancer in Transgenic Mice with Oncolytic Herpes Simplex Viruses

Cited by 47 publications

References 48 publications

Paradoxical Role of DNA Methylation in Activation of FoxA2 Gene Expression during Endoderm Development

Paradoxical Role of DNA Methylation in Activation of FoxA2 Gene Expression during Endoderm Development

Inhibition of human tumor growth in mice by an oncolytic herpes simplex virus designed to target solely HER-2-positive cells

Concomitant Tumor and Minor Histocompatibility Antigen–Specific Immunity Initiate Rejection and Maintain Remission from Established Spontaneous Solid Tumors

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