Your search keyword '"Hezel M"' showing total 5 results

1. Molecular network pathways and functional analysis of tumor signatures associated with development of resistance to viral gene therapy

Author

Song, T-J, Haddad, D, Adusumilli, P, Kim, T, Stiles, B, Hezel, M, Socci, N D, Gönen, M, and Fong, Y

Published

2012

2. Virally-directed fluorescent imaging (VFI) can facilitate endoscopic staging

Author

Adusumilli, P. S., Eisenberg, D. P., Stiles, B. M., Hendershott, K. J., Stanziale, S. F., Chan, M.-K., Hezel, M., Huq, R., Rusch, V. W., and Fong, Y.

Published

2006

3. Cytokine-secreting herpes viral mutants effectively treat tumor in a murine metastatic colorectal liver model by oncolytic and T-cell-dependent mechanisms.

Author

DeRubertis, B. G., Stiles, B. M., Bhargava, A., Gusani, N. J., Hezel, M., D'Angelica, M., and Fong, Y.

Subjects

HERPES simplex virus, GENE therapy, COLON tumors, TUMOR treatment, T cells, CELLULAR mechanics, CELL proliferation, GENETIC mutation

Abstract

In this model of hepatic micrometastases, the antitumor efficacy and role of the T-cell and natural killer (NK) cell populations were studied for oncolytic herpes simplex virus type-1 (HSV-1) viral mutants containing the granulocyte-monocyte colony stimulating factor (GM-CSF (NV1034)) or interluken-12 (IL-12 (NV1042)) cytokine genes. These were compared to saline and control virus (NV1023) in vitro and in vivo. HSV-1 mutants were assessed for cytotoxicity, replication and cytokine expression in CT-26 cells. A syngeneic micrometastatic liver model was then established in naive and immune cell-depleted animals to assess the antitumor efficacy of these viruses. In vitro cytotoxicity and viral replication were similar for each virus, resulting in greater than 80 and 98% cytotoxicity at multiplicity of infection of 1 and 10, respectively. Peak viral titers were 25- to 50-fold higher than initial titer and were not significantly different between viruses. In vivo, all three viruses reduced metastases relative to control, but cytokine-secreting viruses did so with greater efficacy compared to NV1023. This effect was abrogated by T-cell depletion, but not NK-cell depletion. Single-agent therapy with oncolytic viral agents containing GM-CSF or IL-12 is effective in a murine model of liver metastases and likely involves direct viral oncolysis and actions of specific immune effector cells.Cancer Gene Therapy (2007) 14, 590–597. doi:10.1038/sj.cgt.7701053; published online 13 April 2007 [ABSTRACT FROM AUTHOR]

Published

2007

4. Treatment of cholangiocarcinoma with oncolytic herpes simplex virus combined with external beam radiation therapy.

Author

Jarnagin, W. R., Zager, J. S., Hezel, M, Stanziale, S. F., Adusumilli, P. S., Gonen, M, Ebright, M. I., Culliford, A, Gusani, N. J., and Fong, Y

Subjects

CHOLANGIOCARCINOMA, CANCER treatment, GENE therapy, HERPES simplex virus, RADIOTHERAPY, CELL-mediated cytotoxicity, VIRAL replication, CELL lines, COMBINATION drug therapy

Abstract

Replication-competent oncolytic herpes simplex viruses (HSV), modified by deletion of certain viral growth genes, can selectively target malignant cells. The viral growth gene γ134.5 has significant homology to GADD34 (growth arrest and DNA damage protein 34), which promotes cell cycle arrest and DNA repair in response to stressors such as radiation (XRT). By upregulating GADD34, XRT may result in greater oncolytic activity of HSV strains deficient in the γ134.5 gene. The human cholangiocarcinoma cell lines KMBC, SK-ChA-1 and YoMi were treated with NV1023, an oncolytic HSV lacking one copy of γ134.5. Viral proliferation assays were performed at a multiplicity of infection (MOI, number of viral particles per tumor cell) equal to 1, either alone or after XRT at 250 or 500 cGy. Viral replication was assessed by plaque assay. In vitro cytotoxicity assays were performed using virus at MOIs of 0.01 and 0.1, with or without XRT at 250 cGy and cell survival determined with lactate dehydrogenase assay. Established flank tumors in athymic mice were treated with a single intratumoral injection of virus (103 or 104 plaque forming units), either alone or after a single dose of XRT at 500 cGy, and tumor volumes measured. RT-PCR was used to measure GADD34 mRNA levels in all cell lines after a single dose of XRT at 250 or 500 cGy. NV1023 was tumoricidal in all three cell lines, but sensitivity to the virus varied. XRT enhanced viral replication in vitro in all cell lines. Combination treatment with low-dose XRT and virus was highly tumoricidal, both in vitro and in vivo. The greatest tumor volume reduction with combination therapy was seen with YoMi cells, the only cell line with increased GADD34 expression after XRT and the only cell line in which a synergistic treatment effect was suggested. In KMBC and SK-ChA-1 cells, neither of which showed increased GADD34 expression after XRT, tumor volume reduction was less pronounced and there was no suggestion of a synergistic effect in either case. Oncolytic HSV are effective in treating human cholangiocarcinoma cell lines, although sensitivity to virus varies. XRT-enhanced viral replication occurs through a mechanism that is not necessarily dependent on GADD34 upregulation. However, XRT-induced upregulation of GADD34 further promotes tumoricidal activity in viral strains deficient in the γ134.5 gene, resulting in treatment synergy; this effect is cell type dependent. Combined XRT and oncolytic viral therapy is a potentially important treatment strategy that may enhance the therapeutic ratios of both individual therapies.Cancer Gene Therapy (2006) 13, 326–334. doi:10.1038/sj.cgt.7700890; published online 2 September 2005 [ABSTRACT FROM AUTHOR]

Published

2006

5. Neoadjuvant treatment of hepatic malignancy: an oncolytic herpes simplex virus expressing IL-12 effectively treats the parent tumor and protects against recurrence-after resection.

Author

Jarnagin, W R, Zager, J S, Klimstra, D, Delman, K A, Malhotra, S, Ebright, M, Little, S, DeRubertis, B, Stanziale, S F, Hezel, M, Federoff, H, and Fong, Y

Subjects

LIVER cancer, HERPES simplex virus, INTERLEUKIN-12

Abstract

The objective of the study was to evaluate the utility of NV1042, a replication competent, oncolytic herpes simplex virus (HSV) containing the interleukin-12 (IL-12) gene, as primary treatment for hepatic tumors and to further assess its ability to reduce tumor recurrence following resection. Resection is the most effective therapy for hepatic malignancies, but is not possible in the majority of the patients. Furthermore, recurrence is common after resection, most often in the remnant liver and likely because of microscopic residual disease in the setting of postoperative host cellular immune dysfunction. We hypothesize that, unlike other gene transfer approaches, direct injection of liver tumors with replication competent, oncolytic HSV expressing IL-12 will not only provide effective control of the parent tumor, but will also elicit an immune response directed at residual tumor cells, thus decreasing the risk of cancer recurrence after resection. Solitary Morris hepatomas, established in Buffalo rat livers, were injected directly with 10[SUP7] particles of NV1042, NV1023, an oncolytic HSV identical to NV1042 but without the IL-12 gene, or with saline. Following tumor injection, the parent tumors were resected and measured and the animals were challenged with an intraportal injection of 10[SUP5] tumor cells, recreating the clinical scenario of residual microscopic cancer. In vitro cytotoxicity against Morris hepatoma cells was similar for both viruses at a multiplicity of infection of 1 (MOI, ratio of viral particles to target cells), with ≥ 90% tumor cell kill by day 6. NV1042 induced high-level expression of IL-12 in vitro, peaking after 4 days in culture. Furthermore, a single intratumoral injection of NV1042, but not NV1023, induced marked IL-12 and interferon-γ (IFN-γ) expression. Both viruses induced a significant local immune response as evidenced by an increase in the number of intratumoral CD4(+) and CD8(+) lymphocytes, although the... [ABSTRACT FROM AUTHOR]

Published

2003