Your search keyword '"Marcia Meseck"' showing total 5 results

1. Exponential Enhancement of Oncolytic Vesicular Stomatitis Virus Potency by Vector-mediated Suppression of Inflammatory Responses In Vivo

Author

Marcia Meseck, Oliver Ebert, John T. Fallon, Li Chen, Jennifer Altomonte, Adolfo García-Sastre, Lan Wu, and Savio L. C. Woo

Subjects

Pharmacology, Biology, Natural killer T cell, medicine.disease, biology.organism_classification, Virology, Oncolytic virus, Chemokine binding, In vivo, Vesicular stomatitis virus, Hepatocellular carcinoma, Drug Discovery, medicine, Genetics, Potency, Molecular Medicine, Tumor necrosis factor alpha, Molecular Biology

Abstract

Oncolytic virotherapy is a promising strategy for treatment of malignancy, although its effectiveness is hampered by host antiviral inflammatory responses. The efficacy of treatment of oncolytic vesicular stomatitis virus (VSV) in rats bearing multifocal hepatocellular carcinoma (HCC) can be substantially elevated by antibody-mediated depletion of natural killer (NK) cells. In order to test the hypothesis that the oncotyic potency of VSV can be exponentially elevated by evasion of inflammatory responses in vivo, we constructed a recombinant VSV vector expressing equine herpes virus-1 glycoprotein G, which is a broad-spectrum viral chemokine binding protein (rVSV-gG). Infusion of rVSV-gG via the hepatic artery into immune-competent rats bearing syngeneic and multifocal HCC in their livers, resulted in a reduction of NK and NKT cells in the tumors and a 1-log enhancement in intratumoral virus titer in comparison with a reference rVSV vector. The treatment led to increased tumor necrosis and substantially prolonged animal survival without toxicities. These results indicate that rVSV-gG has the potential to be developed as an effective and safe oncolytic agent to treat patients with advanced HCC. Furthermore, the novel concept that oncolytic potency can be substantially enhanced by vector-mediated suppression of host antiviral inflammatory responses could have general applicability in the field of oncolytic virotherapy for cancer.

Published

2008

2. Rejection of Metastatic 4T1 Breast Cancer by Attenuation of Treg Cells in Combination With Immune Stimulation

Author

Tian-Gui Huang, Savio L. C. Woo, John T. Fallon, John Mandeli, Li Chen, and Marcia Meseck

Subjects

Breast Neoplasms, Enzyme-Linked Immunosorbent Assay, Injections, Intralesional, T-Lymphocytes, Regulatory, Adenoviridae, Mice, Breast cancer, Immune system, Immunity, Interferon, Cell Line, Tumor, Drug Discovery, medicine, Genetics, Animals, IL-2 receptor, Neoplasm Metastasis, Molecular Biology, DNA Primers, Pharmacology, Mice, Inbred BALB C, Base Sequence, business.industry, Cancer, Granulocyte-Macrophage Colony-Stimulating Factor, medicine.disease, Metastatic breast cancer, Interleukin-12, Granulocyte macrophage colony-stimulating factor, Immunology, Molecular Medicine, business, medicine.drug

Abstract

4T1 breast carcinoma is a highly malignant and poorly immunogenic murine tumor model that resembles advanced breast cancer in humans, and is refractory to most immune stimulation-based treatments. We hypothesize that the ineffectiveness of immune stimulatory treatment is mediated by the suppressive effects of CD4(+)CD25(+) regulatory T (Treg) cells, which can be attenuated by engaging the glucocorticoid-induced tumor necrosis factor receptor family-related protein with its natural ligand (GITRL); further, combination treatment with existing immune stimulation regimens will augment anti-tumor immunity and eradicate metastatic 4T1 tumors in mice.A soluble homodimeric form of mouse GITRL (mIg-mGITRLs) was molecularly constructed and used to treat orthotopic 4T1 tumors established in immune-competent, syngeneic Balb/c mice. When applied in combination with adenovirus-mediated intratumoral murine granulocyte macrophage colony stimulating factor (GM-CSF) and interleukin-12 (IL-12) gene delivery plus systemic 4-1BB activation, mIg-mGITRLs attenuated the immune-suppressive function of splenic Treg cells, which led to elevated interferon-gamma (IFN-gamma) production, tumor-specific cytolytic T-cell activities, tumor rejection and long-term survival in 65% of the animals without apparent toxicities. The results demonstrate that addition of mIg-mGITRLs to an immune-stimulatory treatment regimen significantly improved long-term survival without apparent toxicity, and could potentially be clinically translated into an effective and safe treatment modality for metastatic breast cancer in patients.

Published

2007

3. OX40 Ligation Enhances Primary and Memory Cytotoxic T Lymphocyte Responses in an Immunotherapy for Hepatic Colon Metastases

Author

Yunjuan Zang, Kaare J. Weber, Shu Hsia Chen, Marcia Meseck, and Ping-Ying Pan

Subjects

Combination therapy, medicine.medical_treatment, Antibodies, Mice, Immune system, Antigen, Drug Discovery, Genetics, Cytotoxic T cell, Medicine, Animals, Neoplasm Metastasis, Molecular Biology, Pharmacology, business.industry, Liver Neoplasms, Immunotherapy, Antigens, Differentiation, Interleukin-12, CTL, Immunology, Colonic Neoplasms, Cancer research, Interleukin 12, Molecular Medicine, business, Immunologic Memory, CD8, T-Lymphocytes, Cytotoxic

Abstract

Previously, we showed that the eradication of murine hepatic metastatic colon carcinomas was achieved by using a combination therapy with adenovirus-mediated gene delivery of interleukin 12 (IL-12) and anti-4-1BB agonistic antibody. However, the therapeutic efficacy was compromised severely when mice with tumors larger than 8 x 8 mm(2) were treated. In this report, we studied the effect of OX40 costimulation through agonistic anti-OX40 in combination with the IL-12 + anti-4-1BB immunotherapy on primary and memory anti-tumor cytotoxic T lymphocyte responses in a large-tumor setting (8 x 8 to 12 x 12 mm(2)). Tumor-infiltrating leukocytes (TILs) isolated from mice treated with the combination therapy of IL-12, anti-4-1BB, and anti-OX40 showed a significantly higher ex vivo direct cytotoxic T lymphocyte (CTL) activity against parental tumors, as compared with those from mice treated with IL-12 and anti-4-1BB. In vivo depletion of CD4(+)T cells during combination therapy significantly decreased the number of tumor-infiltrating CD8(+)T cells and their cytotoxic activity in mice treated with IL-12 + anti-4-1BB + anti-OX40 combination therapy but not in the group treated with IL-12 + anti-4-1BB, which indicated that in vivo OX40 engagement on CD4(+) T cells led to the higher CTL responses observed in animals treated with IL-12 + anti-4-BB + anti-OX40 combination therapy. Furthermore, the combination therapy of IL-12, anti-4-1BB, and anti-OX40 resulted in a significantly higher survival rate in treated mice, as compared with treatment with IL-12 and anti-4-1BB. More importantly, long-term surviving mice from the combination therapy with IL-12, anti-4-1BB, and anti-OX40 exhibited higher memory CTL responses against parental tumor cells. The results demonstrated that OX40 ligation of CD4(+) T cells facilitated the development of primary and memory CTL responses against tumorcells and that coordinated immune activation by IL-12, anti-4-1BB, and anti-OX40 resulted in a significantly higher survival rate in mice with large tumor burdens. Thus, the combination therapy with the adenovirus encoding IL-12 (Adv.mIL-12) + anti-4-1BB + anti-OX40 antibodies may provide a better treatment modality for patients with advanced cancers, often associated with a state of immune suppression or tolerance.

Published

2002

4. Auto-regulated Hepatic Insulin Gene Expression in Type 1 Diabetic Rats

Author

Marcia Meseck, Savio L. C. Woo, and Ruihuan Chen

Subjects

Chloramphenicol O-Acetyltransferase, medicine.medical_specialty, Time Factors, Fasting Hypoglycemia, medicine.medical_treatment, Biology, Hypoglycemia, Transfection, Adenoviridae, Cell Line, Diabetes Mellitus, Experimental, Rats, Nude, Transduction, Genetic, Fructose-Bisphosphate Aldolase, Internal medicine, Drug Discovery, medicine, Genetics, Animals, Humans, Insulin, Promoter Regions, Genetic, Molecular Biology, Pharmacology, Type 1 diabetes, Dose-Response Relationship, Drug, Glucokinase, Aldolase B, Glucose Tolerance Test, medicine.disease, Rats, Insulin oscillation, Diabetes Mellitus, Type 1, Endocrinology, Postprandial, Liver, Glucose-6-Phosphatase, biology.protein, Molecular Medicine, Female

Abstract

Paradigms of insulin gene therapy for type 1 diabetes should incorporate vigorous control for insulin gene expression to be effective in correcting postprandial hyperglycemia and to be safe in preventing fasting hypoglycemia. We hypothesize that hepatic insulin gene expression auto-regulated positively by glucose and negatively by insulin might be both effective and safe in the treatment of type 1 diabetes. Expression of the glucose 6-phosphatase (G6Pase) gene in the liver is both stimulated by glucose and suppressed by insulin. The G6Pase promoter incorporated with intronic enhancers of the aldolase B gene was used to direct insulin gene expression in the liver of streptozotocin-induced diabetic nude rats. In the treated animals, blood insulin levels were elevated after feeding, and nonfasting hyperglycemia was significantly reduced. Glucose tolerance testing also illustrated that the treated animals exhibited accelerated glucose utilization rates. Upon fasting, blood glucose was reduced to normoglycemic range within 4 h and maintained at that level during the prolonged fasting of 16 h. No hypoglycemia was observed in any treated animals at any time throughout the fasting period, as blood insulin gradually declined to the normal range. These results suggest that auto-regulated hepatic insulin expression can potentially be developed as an effective and safe treatment modality for type 1 diabetes.

Published

2001

5. 764. Attenuation of Treg Cells by GITR Ligand Led to Synergistic Enhancement of Treatment Efficacy with Immune-Stimulatory Therapies in Mice Bearing Metastatic 4T1 Breast Carcinoma

Author

Savio L. C. Woo, Li Chen, Tian-Gui Huang, and Marcia Meseck

Subjects

Pharmacology, education.field_of_study, biology, business.industry, T cell, Population, chemical and pharmacologic phenomena, Immune system, medicine.anatomical_structure, Immunology, Drug Discovery, Interleukin 12, biology.protein, Genetics, Medicine, Molecular Medicine, IL-2 receptor, Antibody, business, Antigen-presenting cell, education, Molecular Biology, CD8

Abstract

CD25+CD4+ regulatory T cells (Treg) are capable of suppressing cytolytic activity of CD8+ T cells which may hamper the development of effective immune therapies against cancer. The glucocorticoid-induced TNF receptor family-related gene (GITR) is a membrane receptor is predominantly expressed on these Treg cells, and the immune-suppressive activity of Treg can be inhibited by its interaction with GITR Ligand (GITRL) expressed on antigen presenting cells. Depletion of Treg using anti-CD25 or blocking GITR signaling by GITRL alone, however, was not capable of eradicating pre-established tumors in laboratory animals. Implantation of poorly immunogenic but highly tumorigenic 4T1 breast carcinoma cells in the mammary glands of syngeneic Balb/c mice led to the development of orthotopic lesions that are spontaneously metastatic. We showed that an immune enhancement therapy by intratumoral delivery of a recombinant adenovirus vector expressing murine GMCSF and IL12 (Ad.mGMCSF-IRES-mIL12), in combination with intraperitoneal administration of a fusion protein of murine immunoglobulin with the ecto-domain of murine 4-1BB ligand (mIg-m4-1BBLs), in mice bearing 4T1 breast carcinoma led to significantly prolonged survival, although the treated animals eventually succumbed to tumor relapse. The Treg population was significantly elevated in the splenocytes of the treated animals and depletion of CD4+CD25+ cell population led to a significant increase in splenic T cell proliferation activity in vitro. We hypothesized that addition of a fusion protein made of murine immunoglobulin and the ecto-domain of GITR ligand (mIg-mGITRLs) to the treatment regimen would have a synergistic effect on anti-tumor immune responses through attenuation of Treg cell-mediated immune suppression, which would lead to much enhanced treatment efficacy. The data presented here show that mIg-mGITRLs has the ability to attenuate the immune suppressive activity of CD4+CD25+ Treg cells in vitro. Intraperitoneal administration of mIg-mGITRLs with Ad.mGMCSF-IRES-mIL12 + mIg-m4-1BBLs treatment in 4T1-bearing mice resulted in tumor-free and long-term survival in >60% of the animals. Furthermore, this combination therapy induced robust tumor-specific CTL activities and the long-term surviving animals were able to reject a challenge of live parental tumor cells. There were no apparent toxic effects and taken together, the results suggest this novel combination therapy induced a systemic and effective anti-tumor immunity that is persistent, which may be translated into an effective and safe treatment modality for metastatic breast cancer in humans.

Published

2006