Your search keyword '"Marcia Meseck"' showing total 23 results

1. Safety and Immunogenicity of an Inactivated Recombinant Newcastle Disease Virus Vaccine Expressing SARS-CoV-2 Spike: Interim Results of a Randomised, Placebo-Controlled, Phase 1/2 Trial

Author

Punnee Pitisuttithum, Viravarn Luvira, Saranath Lawpoolsri, Sant Muangnoicharoen, Supitcha Kamolratanakul, Chaisith Sivakorn, Piengthong Narakorn, Somchaiya Surichan, Sumalee Prangpratanporn, Suttida Puksuriwong, Steven Lamola, Laina D. Mercer, Rama Raghunandan, Weina Sun, Yonghong Liu, Juan Manuel Carreño, Rami Scharf, Weerapong Phumratanaprapin, Fatima Amanat, Luc Gagnon, Ching-Lin Hsieh, Ruangchai Kaweepornpoj, Sarwat Khan, Manjari Lal, Stephen McCroskery, Jason McLellan, Ignacio Mena, Marcia Meseck, Benjaluck Phonrat, Yupa Sabmee, Ratsamikorn Singchareon, Stefan Slamanig, Nava Suthepakul, Johnstone Tcheou, Narumon Thantamnu, Sompone Theerasurakarn, Steven Tran, Thanakrit Vilasmongkolchai, Jessica A White, Nina Bhardwaj, Adolfo Garcia-Sastre, Peter Palese, Florian Krammer, Kittisak Poopipatpol, Ponthip Wirachwong, Richard Hjorth, and Bruce L Innis

Subjects

medicine.medical_specialty, biology, business.industry, Immunogenicity, Vaccine trial, General Medicine, Placebo, biology.organism_classification, Interim analysis, Newcastle disease, Article, Vaccination, Internal medicine, medicine, Adverse effect, business, Intramuscular injection

Abstract

SummaryBackgroundProduction of affordable coronavirus disease 2019 (COVID-19) vaccines in low- and middle-income countries is needed. NDV-HXP-S is an inactivated egg-based Newcastle disease virus vaccine expressing the spike protein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). It’s being developed in Thailand, Vietnam, and Brazil; herein are initial results from Thailand.MethodsThis phase 1 stage of a randomised, dose-escalation, observer-blind, placebo-controlled, phase 1/2 trial was conducted at the Vaccine Trial Centre, Mahidol University (Bangkok). Healthy adults aged 18-59 years, non-pregnant and negative for SARS-CoV-2 antibodies were eligible. Participants were block randomised to receive one of six treatments by intramuscular injection twice, 28 days apart: 1 µg±CpG1018 (a toll-like receptor 9 agonist), 3 µg±CpG1018, 10 µg, or placebo. Participants and personnel assessing outcomes were masked to treatment. The primary outcomes were solicited and spontaneously reported adverse events (AEs) during 7 and 28 days after each vaccination, respectively. Secondary outcomes were immunogenicity measures (anti-S IgG and pseudotyped virus neutralisation). An interim analysis assessed safety at day 57 in treatment-exposed individuals and immunogenicity through day 43 per protocol. ClinicalTrials.gov (NCT04764422).FindingsBetween March 20 and April 23, 2021, 377 individuals were screened and 210 were enrolled (35 per group); all received dose one; five missed dose two. The most common solicited AEs among vaccinees, all predominantly mild, were injection site pain (InterpretationNDV-HXP-S had an acceptable safety profile and potent immunogenicity. The 3 µg and 3 µg+CpG1018 formulations advanced to phase 2.FundingNational Vaccine Institute (Thailand), National Research Council (Thailand), Bill & Melinda Gates Foundation, National Institutes of Health (USA)

Published

2021

2. Abstract CT173: PGV-001: A phase I trial of a multipeptide personalized neoantigen vaccine in the adjuvant setting

Author

Julia Kodysh, John P. Finnigan, Timothy O'Donnell, Thomas U. Marron, Marcia Meseck, Alex Rubinsteyn, Philip Friedlander, Ana Belen Blazquez, Nina Bhardwaj, and Mansi Saxena

Subjects

Oncology, Cancer Research, medicine.medical_specialty, biology, business.industry, medicine.medical_treatment, Immunogenicity, Cancer, Human leukocyte antigen, medicine.disease, Vaccination, Antigen, Internal medicine, MHC class I, biology.protein, Medicine, business, Adjuvant, CD8

Abstract

Background: Mutation-derived tumor antigens (MTAs) arise as a result of somatic mutations, such as nucleotide substitutions and small insertions/deletions. MTAs can serve as specific targets for antitumor therapy, including neoantigen vaccines. The goal of neoantigen vaccination is to help prime T cells to recognize such tumor-specific mutations. Here we describe a phase I trial testing a personalized genomic vaccine (PGV-001) in multiple histologies in the adjuvant setting (NCT02721043). Methods: This trial included patients with histologic diagnosis of solid malignancies or multiple myeloma with a >30% risk of recurrence but no measurable disease at the time of first vaccination. For each patient, HLA typing was performed, and the patient's tumor and germline DNA and tumor RNA were sequenced. Mutated peptides containing predicted neoantigens were selected using the OpenVax computational pipeline, which prioritizes somatic mutations by expression of the mutant allele in the tumor RNA and predicted MHC class I epitope binding for the patient's HLA type. A maximum of 10 peptides was included in each patient's personalized vaccine. The vaccine was administered over the course of 6 months, given in combination with poly-ICLC as the adjuvant. The primary objectives were to determine safety and tolerability, feasibility, and immunogenicity of the PGV-001 neoantigen vaccine. Results: The neoantigen vaccine was successfully administered to 13 patients, spanning 5 different tumor types. For each patient, an average of 1730 somatic mutations were identified (range 521-5106), of which 349 were coding variants (range 68-1493), 88 were coding and expressed in the tumor RNA (range 9-233), and 71 were coding, expressed and resulted in predicted MHC class I ligands (range 8-193). The urothelial, head & neck, and lung tumors resulted in larger numbers of predicted neoantigens than in the cases of multiple myeloma or breast tumors. Despite this difference, each of the 13 patient tumor samples showed enough of a neoantigen load to enable vaccination. We have also initiated analysis of immunogenicity, and early reports demonstrate neoantigen-specific CD4 and CD8 T-cell responses. Conclusions: The PGV-001 personalized neoantigen vaccine was successfully administered to 13 patients, where each patient's neoantigen load was adequate for vaccine synthesis. While we have demonstrated the computational feasibility of identification of neoantigens for inclusion in the PGV-001 genomic vaccine, clinical outcomes will be reported separately. Citation Format: Julia Kodysh, Thomas Marron, Alex Rubinsteyn, Tim O'Donnell, John Finnigan, Ana Blazquez, Mansi Saxena, Marcia Meseck, Philip Friedlander, Nina Bhardwaj. PGV-001: A phase I trial of a multipeptide personalized neoantigen vaccine in the adjuvant setting [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr CT173.

Published

2020

3. Abstract A005: A phase I study of the safety and immunogenicity of a multipeptide personalized genomic vaccine in the adjuvant treatment of solid cancers

Author

Eric M. Genden, Sacha Gnjatic, Brett A. Milles, Marcia Meseck, Julia Kodysh, Samir Parekh, Nina Bhardwaj, John Mandeli, Elisa Port, Krysztof Misiukiewicz, Amy Tiersten, Ashutosh K. Tewari, Hern J. Cho, Hooman Khorasani, Timothy O'Donnell, Jeff Hammerbacher, Milind Mahajan, Matthew D. Galsky, Hanna Irie, Ana Belen Blazquez, Eric E. Schadt, Andrea S. Wolf, John Holt, Thomas U. Marron, Sujit S. Nair, Michael J. Donovan, Rachel Lubong Sabado, William Oh, John P. Finnigan, Alex Rubinsteyn, Peter Dottino, and Phillip A. Friedlander

Subjects

Cancer Research, medicine.medical_treatment, ELISPOT, Immunogenicity, Immunology, Biology, Virology, Epitope, Vaccination, Cancer immunotherapy, Antigen, medicine, Adjuvant, Ex vivo

Abstract

Introduction: Mutation-derived tumor antigens (MTAs) arise as a direct result of somatic variations, including nucleotide substitutions, insertions, and deletions that occur during carcinogenesis. These somatic variations can be characterized via genetic sequencing and used to identify MTAs. We developed a platform for a fully-personalized MTA-based vaccine in the adjuvant treatment of solid and hematologic malignanicies. Methods: This is a single-arm, open label, proof-of-concept phase I study designed to test the safety and immunogenicity of Personalized Genomic Vaccine 001 (PGV001) that targets up to 10 predicted personal tumor neoantigens. The single-center study will enroll 20 eligible subjects with histologic diagnosis of solid and hematologic malignancies. Subjects must have no measurable disease at time of first vaccine administration, and 5-year disease recurrence risk of > 30%. Toxicity will be defined by CTCAE v5.0. Blood samples will be collected at various time points for immune response monitoring. Each patient’s vaccine peptides are selected by identifying somatic mutations from comparison of tumor and normal exome sequencing data, phasing somatic variants with co-occurring germline variants using tumor RNA sequencing data, and ranking mutated peptide sequences ”Openvax pipeline.” The process for determining somatic variants hews closely to the Broad Institute’s “Best Practices” for cancer SNVs and indels. The phasing of somatic and germline variants is implemented in a custom bioinformatics tool called Isovar. Mutated protein sequences containing phased variants are ranked according to two criteria: expression of the mutant allele in tumor RNA and aggregated predicted affinity to the patient’s Class I MHCs. Both quantities are normalized and multiplied together to create single ranked ordering of the candidate mutant sequences. Results: PGV001_002 (head and neck squamous cell cancer), who has completed vaccination, received 10 doses of vaccine comprising 10 long peptides (25 amino acid length) combined with poly-ICLC (toll-like receptor-3 agonist) intradermally. Vaccine-induced blood T-cell responses were determined, at weeks 0 (before-treatment) and 27 (after-treatment), ex vivo by interferon (IFN)-g enzyme-linked immunospot (ELISPOT) assay and after in vitro expansion by intracellular cytokine staining (ICS). Overlapping 15-16-mer assays peptides (OLPs) spanning the entirety of each ILP and 9-10-mer peptides corresponding to each predicted class I epitope (Min) were pooled and used to monitor immunogenicity. Ex vivo responses to these peptide pools were undetectable at week 0 but were evident at week 27 against 2 OLPs out of 10 (20%) and in 5 Min out of 10 (50%). After in vitro expansion, neoantigen-specific CD4+ and CD8+ T-cell responses were found in 5 out of 10 pooled peptides (50%). 7 out of 10 (70%) epitopes elicited polyfunctional T-cell responses (secretion of INF-α, TNF-α, and/or IL-2) from either CD4+ or CD8+ T-cells. Conclusion: To identify which predicted epitopes within the peptides pools stimulated the T-cell responses, we deconvoluted all the pools by either ex vivo and in vitro expansion. Ex vivo IFN-α production was detected in 1 (15-mer) peptide out of 15 (6.7%) and in 4 (9-10-mer) peptides out of 22 (18.2%). After expansion with single peptides, of 22 (9-10-mer) peptides tested, CD8+ T-cells were reactive against 13 peptides (59%), while CD4+ responses were seen in response to 11 of 15 (15-16-mer) peptides tested. Both CD4+ and CD8+ T-cell responses were polyfunctional. The PGV001 vaccine in our first patient showed both safety and immunogenicity, eliciting both CD4+ and CD8+ responses to the vaccine peptides. As we are enrolling additional patients, the information learned from this clinical trial will instruct the next generation of MTA-based vaccines, future development of immunotherapeutic approaches and rational combinations. Citation Format: Ana B. Blazquez, Alex Rubinsteyn, Julia Kodysh, John P. Finnigan, Thomas Marron, Rachel L. Sabado, Marcia Meseck, Timothy J. O'Donnell, Jeffrey Hammerbacher, Michael Donovan, John Holt, Milind Mahajan, John Mandeli, Krysztof Misiukiewicz, Eric M. Genden, Brett A. Milles, Hooman Khorasani, Peter R. Dottino, Hanna Irie, Amy B. Tiersten, Elisa R. Port, Andrea S. Wolf, Hern J. Cho, Ashutosh Tewari, Samir S. Parekh, Sujit Nair, Matthew D. Galsky, William K. Oh, Sacha Gnjatic, Eric E. Schadt, Phillip A. Friedlander, Nina Bhardwaj. A phase I study of the safety and immunogenicity of a multipeptide personalized genomic vaccine in the adjuvant treatment of solid cancers [abstract]. In: Proceedings of the Fourth CRI-CIMT-EATI-AACR International Cancer Immunotherapy Conference: Translating Science into Survival; Sept 30-Oct 3, 2018; New York, NY. Philadelphia (PA): AACR; Cancer Immunol Res 2019;7(2 Suppl):Abstract nr A005.

Published

2019

4. The potential of recombinant vesicular stomatitis virus-mediated virotherapy against metastatic colon cancer

Author

Minoru Yamaki, Takemasa Sakaguchi, Katsunori Shinozaki, Oliver Ebert, Hideki Ohdan, Marcia Meseck, and Savio L. C. Woo

Subjects

Male, Oncology, medicine.medical_specialty, Lung Neoplasms, Bevacizumab, Colon, Colorectal cancer, Recombinant Fusion Proteins, Genetic Vectors, Newcastle disease virus, Biology, Metastasis, Viral Proteins, Hepatic arterial infusion, Cell Line, Tumor, Internal medicine, Genetics, medicine, Animals, Humans, Lung, Oncolytic Virotherapy, Cetuximab, Liver Neoplasms, Cancer, Vesiculovirus, General Medicine, medicine.disease, Rats, Inbred F344, Rats, Oxaliplatin, Oncolytic virus, Colonic Neoplasms, Cancer research, medicine.drug

Abstract

Colorectal cancer (CRC) is the fourth most frequently diagnosed cancer and the second leading cause of cancer-related mortality in the United States. The liver and lung are the most common sites of distant metastasis of CRC. The approval of newer chemotherapeutic agents such as oxaliplatin, irinotecan, bevacizumab, cetuximab and panitumumab has significantly improved survival, yet the majority of patients still succumb to the disease in less than 2 years. Novel therapeutic agents that can provide significant clinical benefit for metastatic CRC patients are needed. Oncolytic vesicular stomatitis virus (VSV) is a promising tool as a cancer therapeutic agent. In this study, we examined the feasibility of repeated intravenous infusions of rVSV in multiple CRC lung metastases, compared with repeated hepatic arterial administration in multifocal CRC liver metastasis in immune competent rats. We established a multifocal liver metastases model or the multiple lung metastases model using a CRC cell line, RCN-H4, implanted into syngeneic F344/DuCrj rats. 4.0x10(6) plaque-forming units (pfu) of recombinant VSV vectors expressing mutant (L289A) Newcastle disease virus fusion protein [rVSV-NDV/F(L289A)] were administered 3 times for 3 consecutive days locally via the hepatic artery for liver metastases or systemically via the penial vein for lung metastases. In the liver metastasis model, significantly enhanced survival was observed with rVSV-NDV/F(L289A)-treated rats (P=0.0196). Median survival was 110 and 25 days, respectively. In addition, 4 out of 7 of the rVSV-NDV/F(L289A)-treated rats demonstrated long-term survival exceeding 100 days. The long-term surviving rats were sacrificed to evaluate for residual malignancy. Liver tumors were not detected. In the lung metastasis model, median survival was 10 [VSV-NDV/F(L289A)-treated rats] and 7 days (control). Although survival was significantly prolonged (P

Published

2012

5. Dendritic Cell Vaccines

Author

Rachel Lubong Sabado, Nina Bhardwaj, and Marcia Meseck

Subjects

0301 basic medicine, biology, business.industry, medicine.medical_treatment, Immunotherapy, Disease, Dendritic cell, Major histocompatibility complex, Clinical trial, 03 medical and health sciences, Therapeutic approach, 030104 developmental biology, 0302 clinical medicine, Immune system, Antigen, 030220 oncology & carcinogenesis, Immunology, medicine, biology.protein, business

Abstract

Exploitation of the patient's own immune system to induce antitumor immune responses using dendritic cell (DC) immunotherapy has been established in early clinical trials as a safe and promising therapeutic approach for cancer. However, their limited success in larger clinical trials highlights the need to optimize DC vaccine preparations. This chapter describes the methodologies utilized for the preparation of the DC vaccine most commonly used in clinical trials. Optional variations at different stages in DC vaccine preparation, based on the nature of antigen, delivery of antigen, maturation stimuli, and mode of administration for DC vaccines, are also presented for consideration as these are often dependent on the disease setting, desired immune response, and/or resources available.

Published

2016

6. The Novel Role of Tyrosine Kinase Inhibitor in the Reversal of Immune Suppression and Modulation of Tumor Microenvironment for Immune-Based Cancer Therapies

Author

Ping-Ying Pan, Celia M. Divino, Ge Ma, Junko Ozao-Choy, Shu Hsia Chen, Max Sung, Johnny Kao, Marcia Meseck, George X. Wang, and Myron Schwartz

Subjects

Cancer Research, Indoles, medicine.drug_class, Molecular Sequence Data, Mice, Transgenic, chemical and pharmacologic phenomena, Biology, Lymphocyte Activation, T-Lymphocytes, Regulatory, Article, Tyrosine-kinase inhibitor, Carcinoma, Lewis Lung, Mice, Immune system, Sunitinib, medicine, Animals, Cytotoxic T cell, Myeloid Cells, Pyrroles, Amino Acid Sequence, Protein Kinase Inhibitors, Mice, Inbred BALB C, Tumor microenvironment, FOXP3, Interleukin, Sunitinib malate, Mice, Inbred C57BL, Oncology, Colonic Neoplasms, Immunology, Cancer research, medicine.drug

Abstract

In tumor-bearing hosts, myeloid-derived suppressor cells (MDSC) and T regulatory cells (Treg) play important roles in immune suppression, the reversal of which is vitally important for the success of immune therapy. We have shown that ckit ligand is required for MDSC accumulation and Treg development. We hypothesized that sunitinib malate, a receptor tyrosine kinase inhibitor, could reverse MDSC-mediated immune suppression and modulate the tumor microenvironment, thereby improving the efficacy of immune-based therapies. Treatment with sunitinib decreased the number of MDSC and Treg in advanced tumor-bearing animals. Furthermore, it not only reduced the suppressive function of MDSCs but also prevented tumor-specific T-cell anergy and Treg development. Interestingly, sunitinib treatment resulted in reduced expression of interleukin (IL)-10, transforming growth factor-β, and Foxp3 but enhanced expression of Th1 cytokine IFN-γ and increased CTL responses in isolated tumor-infiltrating leukocytes. A significantly higher percentage and infiltration of CD8 and CD4 cells was detected in tumors of sunitinib-treated mice when compared with control-treated mice. More importantly, the expression of negative costimulatory molecules CTLA4 and PD-1 in both CD4 and CD8 T cells, and PDL-1 expression on MDSC and plasmacytoid dendritic cells, was also significantly decreased by sunitinib treatment. Finally, sunitinib in combination with our immune therapy protocol (IL-12 and 4-1BB activation) significantly improves the long-term survival rate of large tumor-bearing mice. These data suggest that sunitinib can be used to reverse immune suppression and as a potentially useful adjunct for enhancing the efficacy of immune-based cancer therapy for advanced malignancies. [Cancer Res 2009;69(6):2514–22]

Published

2009

7. rVSV(MΔ51)-M3 Is an Effective and Safe Oncolytic Virus for Cancer Therapy

Author

Adolfo García-Sastre, John Mandeli, John T. Fallon, Lan Wu, Marcia Meseck, Katsunori Shinozaki, Savio L. C. Woo, Jennifer Altomonte, Oliver Ebert, and Tian-Gui Huang

Subjects

Male, Carcinoma, Hepatocellular, Cell Survival, Neutrophils, viruses, Genetic enhancement, Genetic Vectors, Heterologous, Lymphocyte Depletion, Virus, Viral Proteins, Cell Line, Tumor, Scientific Papers, Genetics, medicine, Animals, Potency, Vector (molecular biology), Rats, Inbred BUF, Molecular Biology, Sequence Deletion, Oncolytic Virotherapy, biology, Liver Neoplasms, Cancer, Vesiculovirus, biology.organism_classification, medicine.disease, Virology, Rats, Oncolytic virus, Killer Cells, Natural, Oncolytic Viruses, Vesicular stomatitis virus, Cytokines, Molecular Medicine, Leukocyte Reduction Procedures

Abstract

Oncolytic vesicular stomatitis virus (VSV) is being developed as a novel therapeutic agent for cancer treatment, although it is toxic in animals when administered systemically at high doses. Its safety can be substantively improved by an M Delta 51 deletion in the viral genome, and yet VSV(M Delta 51) induces a much greater, robust cellular inflammatory response in the host than wild-type VSV, which severely attenuates its oncolytic potency. We have reported that the oncolytic potency of wild-type VSV can be enhanced by vector-mediated expression of a heterologous viral gene that suppresses cellular inflammatory responses in the lesions. To develop an effective and safe VSV vector for cancer treatment, we tested the hypothesis that the oncolytic potency of VSV(M Delta 51) can be substantively elevated by vector-mediated expression of M3, a broad-spectrum and high-affinity chemokine-binding protein from murine gammaherpesvirus-68. The recombinant vector rVSV(M Delta 51)-M3 was used to treat rats bearing multifocal lesions (1-10 mm in diameter) of hepatocellular carcinoma (HCC) in their liver by hepatic artery infusion. Treatment led to a significant reduction of neutrophil and natural killer cell accumulation in the lesions, a 2-log elevation of intratumoral viral titer, substantively enhanced tumor necrosis, and prolonged animal survival with a 50% cure rate. Importantly, there were no apparent systemic and organ toxicities in the treated animals. These results indicate that the robust cellular inflammatory responses induced by VSV(M Delta 51) in HCC lesions can be overcome by vector-mediated intratumoral M3 expression, and that rVSV(M Delta 51)-M3 can be developed as an effective and safe oncolytic agent to treat advanced HCC patients in the future.

Published

2008

8. 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

9. The systemic administration of Ig-4-1BB ligand in combination with IL-12 gene transfer eradicates hepatic colon carcinoma

Author

D. P. Xu, Shu Hsia Chen, Savio L. C. Woo, Marcia Meseck, Tian-Gui Huang, and Bernhard Sauter

Subjects

Recombinant Fusion Proteins, Genetic enhancement, Genetic Vectors, Gene delivery, Lymphocyte Activation, Antibodies, Adenoviridae, Mice, chemistry.chemical_compound, Transduction, Genetic, Cell Line, Tumor, Genetics, Animals, Molecular Biology, Cells, Cultured, Mice, Inbred BALB C, biology, Liver Neoplasms, Genetic transfer, Dendritic Cells, Genetic Therapy, Neoplasms, Experimental, Ligand (biochemistry), Interleukin-12, Killer Cells, Natural, 4-1BB Ligand, 4-1BB ligand, chemistry, Immunoglobulin G, Colonic Neoplasms, Tumor Necrosis Factors, Immunology, biology.protein, Systemic administration, Cancer research, Interleukin 12, Molecular Medicine, Immunotherapy, Antibody, Spleen, T-Lymphocytes, Cytotoxic

Abstract

We have previously shown that the local-membrane bound 4-1BB ligand and IL-12 gene transfer induced a significant antitumor response in a mouse colon carcinoma model. However, a high viral dose was required in order to achieve the best efficacy. In this study, we hypothesize that the systemic administration of soluble Ig-4-1BB ligand can give rise to better T-cell immune activation than local gene delivery. With potential clinical applications in mind, we further compare whether the natural 4-1BB ligand fused to mouse IgG2a (Ig-4-1BBL) would be as effective as the agonistic anti-4-1BB antibody. The dimeric form of Ig-4-1BBL was purified from HeLa cells transduced with a recombinant adenovirus (ADV/Ig-4-1BBL) expressing Ig-4-1BBL. Functional activity was confirmed by the ligand's ability to bind to activated splenic T cells or bone marrow (BM)-derived dendritic cells (DCs) that express 4-1BB receptor. The soluble Ig-4-1BBL efficiently costimulated CD3-activated T-cell proliferation in vitro. More importantly, it induced tumor-specific CTLs as effectively as the agonistic anti-4-1BB antibody. When combined with IL-12 gene transfer, systemic administration of the Ig-4-1BBL proved to be more potent than local gene delivery. In addition, the Ig-4-1BBL is as potent as the agonistic anti-4-1BB antibody for the treatment of hepatic MCA26 colon carcinoma, resulting in 50% complete tumor regression and long-term survival. In long-term surviving mice, both treatment modalities induced persistent tumor-specific CTL activity. In summary, these results suggest that the systemic delivery of Ig-4-1BBL can generate a better antitumor response than local gene delivery. Ig-4-1BBL had equivalent biological functions when compared to the agonistic anti-4-1BB antibody. Thus, soluble 4-1BBL dimmer can be developed as a promising agent for cancer therapy in humans.

Published

2005

10. Functional Genomic Analysis of Type II IL-1β Decoy Receptor: Potential for Gene Therapy in Human Arthritis and Inflammation

Author

Savio L. C. Woo, Mukundan Attur, Marcia Meseck, Mary Y. Leung, Mandar Dave, Christine Cipolletta, and Ashok R. Amin

Subjects

Cell type, Genetic enhancement, Genetic Vectors, Immunology, Inflammation, Biology, Adenoviridae, Cell Line, Mice, Paracrine signalling, Chondrocytes, Organ Culture Techniques, Transduction, Genetic, Osteoarthritis, medicine, Animals, Humans, Immunology and Allergy, Receptors, Interleukin-1 Type II, Autocrine signalling, Cells, Cultured, Aged, Cartilage, Synovial Membrane, Receptors, Interleukin-1, Epithelial Cells, Genetic Therapy, Genomics, Fibroblasts, Middle Aged, Molecular biology, In vitro, medicine.anatomical_structure, Synovial Cell, Cattle, Proteoglycans, Rabbits, Inflammation Mediators, medicine.symptom, Interleukin-1

Abstract

Gene expression arrays show that human epithelial cells and human arthritis-affected cartilage lack detectable amounts of mRNA for IL-1 antagonizing molecules: IL-1Ra and IL-1RII, but constitutively express IL-1. Functional genomic analysis was performed by reconstituting human IL-1RII expression in various IL-1RII-deficient cell types to examine its antagonist role using gene therapy approaches. Adenovirus-expressing IL-1RII when transduced into human and bovine chondrocytes, human and rabbit synovial cells, human epithelial cells, and rodent fibroblasts expressed membrane IL-1RII and spontaneously released functional soluble IL-1RII. The IL-1RII+ (but not IL-1RII−) cells were resistant to IL-1β-induced, NO, PGE2, IL-6, and IL-8 production or decreased proteoglycan synthesis. IL-1RII inhibited the function of IL-1 in chondrocytes and IL-1- and TNF-α-induced inflammatory mediators in human synovial and epithelial cells. IL-1RII+ chondrocytes were more resistant to induction of NO and PGE2 by IL-1β compared with IL-1RII− cells incubated with a 10-fold (weight) excess of soluble type II IL-1R (sIL-1RII) protein. In cocultures, IL-1RII+ synovial cells released sIL-1RII, which in a paracrine fashion protected chondrocytes from the effects of IL-1β. Furthermore, IL-1RII+ (but not IL-1RII−) chondrocytes when transplanted onto human osteoarthritis-affected cartilage in vitro, which showed spontaneous release of sIL-1RII for 20 days, inhibited the spontaneous production of NO and PGE2 in cartilage in ex vivo. In summary, reconstitution of IL-1RII in IL-1RII− cells using gene therapy approaches significantly protects cells against the autocrine and paracrine effects of IL-1 at the signaling and transcriptional levels.

Published

2002

11. 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

12. Glucose-stimulated and self-limiting insulin production by glucose 6-phosphatase promoter driven insulin expression in hepatoma cells

Author

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

Subjects

medicine.medical_specialty, medicine.medical_treatment, Genetic Vectors, Transfection, Adenoviridae, Liver Neoplasms, Experimental, Insulin receptor substrate, Internal medicine, Gene expression, Genetics, medicine, Animals, Insulin, Promoter Regions, Genetic, Molecular Biology, Type 1 diabetes, Reporter gene, biology, Genetic Therapy, medicine.disease, Stimulation, Chemical, IRS2, Rats, Insulin receptor, Diabetes Mellitus, Type 1, Glucose, Endocrinology, Gene Expression Regulation, Glucose-6-Phosphatase, Hepatocytes, biology.protein, Molecular Medicine, Glucose 6-phosphatase

Abstract

The liver is an attractive target organ for insulin gene expression in type 1 diabetes as it contains appropriate cellular mechanisms of regulated gene expression in response to blood glucose and insulin. We hypothesize that insulin production regulated by both glucose and insulin may be achieved using the promoter of the glucose 6-phosphatase gene (G6Pase), the expression of which in the liver is induced by glucose and suppressed by insulin. Recombinant adenoviral vectors expressing the reporter gene CAT or insulin under transcriptional direction of the G6Pase promoter were constructed. Glucose-stimulated as well as self-limiting insulin production was achieved in vector-transduced hepatoma cells in which expression of the insulin gene was controlled by the G6Pase promoter. While insulin strongly inhibited the G6Pase promoter activity under low glucose conditions, its inhibitory capacity was attenuated when glucose levels were elevated. At the physiologic glucose level of 5.5 mM glucose, vector-transduced hepatoma cells produced a self-limited level of insulin at approximately 0.2-0.3 ng/ml, which is within the range of fasting levels of insulin in normal animals. These results indicate that the G6Pase promoter possesses desirable features and may be developed for regulated hepatic insulin gene expression in type 1 diabetes.

Published

2000

13. Myeloid-derived suppressor cells as a vehicle for tumor-specific oncolytic viral therapy

Author

Brian A. Coakley, Ge Ma, Savio L. C. Woo, Ping-Ying Pan, Hui-Ming Chen, Shu Hsia Chen, Marcia Meseck, Samuel Eisenstein, Celia M. Divino, Karen C. Briley-Saebo, and Stephen C. Ward

Subjects

Cancer Research, Virus, Vesicular stomatitis Indiana virus, Article, Mice, Random Allocation, Immune system, Cell Movement, medicine, Animals, Myeloid Cells, Tissue Distribution, Oncolytic Virotherapy, Mice, Inbred BALB C, biology, Cancer, Cell Differentiation, biology.organism_classification, medicine.disease, Oncolytic virus, Mice, Inbred C57BL, Oncolytic Viruses, Viral Tropism, Oncology, Vesicular stomatitis virus, Immunology, Colonic Neoplasms, Myeloid-derived Suppressor Cell, Systemic administration, Oncolytic Virus Therapy

Abstract

One of the several impediments to effective oncolytic virus therapy of cancer remains a lack of tumor-specific targeting. Myeloid-derived suppressor cells (MDSC) are immature myeloid cells induced by tumor factors in tumor-bearing hosts. The biodistribution kinetics of MDSC and other immune cell types in a murine hepatic colon cancer model was investigated through the use of tracking markers and MRI. MDSCs were superior to other immune cell types in preferential migration to tumors in comparison with other tissues. On the basis of this observation, we engineered a strain of vesicular stomatitis virus (VSV), an oncolytic rhabdovirus that bound MDSCs and used them as a delivery vehicle. Improving VSV-binding efficiency to MDSCs extended the long-term survival of mice bearing metastatic colon tumors compared with systemic administration of wild-type VSV alone. Survival was further extended by multiple injections of the engineered virus without significant toxicity. Notably, direct tumor killing was accentuated by promoting MDSC differentiation towards the classically activated M1-like phenotype. Our results offer a preclinical proof-of-concept for using MDSCs to facilitate and enhance the tumor-killing activity of tumor-targeted oncolytic therapeutics. Cancer Res; 73(16); 5003–15. ©2013 AACR.

Published

2013

14. A functional recombinant human 4-1BB ligand for immune costimulatory therapy of cancer

Author

Savio L. C. Woo, Tian-Gui Huang, Marcia Meseck, Ge Ma, George X. Wang, and Shu Hsia Chen

Subjects

Cancer Research, Recombinant Fusion Proteins, T-Lymphocytes, Immunology, Molecular Sequence Data, CHO Cells, Lymphocyte Activation, Article, chemistry.chemical_compound, Mice, Immune system, Cricetulus, Western blot, Adjuvants, Immunologic, Glutamate-Ammonia Ligase, Cricetinae, Neoplasms, Gene Order, medicine, Immunology and Allergy, Animals, Humans, Amino Acid Sequence, Cell Proliferation, Pharmacology, biology, medicine.diagnostic_test, Base Sequence, Chinese hamster ovary cell, Haplorhini, Ligand (biochemistry), Fusion protein, Molecular biology, Rats, 4-1BB ligand, 4-1BB Ligand, chemistry, biology.protein, Leukocytes, Mononuclear, Immunotherapy, Protein A, Clone (B-cell biology)

Abstract

Costimulatory factors hold great promise for development into novel anticancer biotherapeutics. An agonist to 4-1BB is ranked number 8 by National Cancer Institute on the list of 20 agents with high potential for use in treating cancer. We earlier reported on a recombinant murine 4-1BB ligand fusion protein that binds 4-1BB receptor on murine T cells and stimulates their proliferation in tumor-bearing mice. To facilitate clinical translation,we constructed a corresponding recombinant human 4-1BB ligand fusion protein (hIg-h4-1BBLs) and showed its ability to activate human T cells in vitro. Using Chinese hamster ovary cells transformed with a plasmid coexpressing hIg-h4-1BBLs and rat glutamine synthetase, we generated a high-producing clone by sequential selection with methionine sulfoximine. The hIg-h4-1BBLs was partially purified by protein A column chromatography and characterized biochemically and functionally, using human 4-1BB binding and human T-cell proliferation assays, in vitro.Sodium dodecyl sulfate-polyacrylamide gel electrophoresis and Western Blot confirmed that the hIg-h4-1BBLs is expressed predominantly as a functionally active multimeric protein with the ability to specifically bind to cells expressing human 4-1BB receptor and induce significant T-cell proliferation in vitro using both human and monkey peripheral blood mononuclear cells. The hIg-h4-1BBLs can be produced in large quantities from the high producer clone and developed as a novel immune costimulatory biotherapeutic to treat, alone and in combination with other modalities, various malignant diseases in patients through T-cell activation. Process development of this clinical agent has been discussed with the Food and Drug Administration in a pre-Investigational New Drug meeting and presented to the Office of Biotechnology Activities in a public hearing.

Published

2011

15. Enhanced oncolytic potency of vesicular stomatitis virus through vector-mediated inhibition of NK and NKT cells

Author

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

Subjects

Male, Cancer Research, Genetic enhancement, Genetic Vectors, Newcastle disease virus, Cytomegalovirus, Recombinant virus, Virus Replication, Article, Necrosis, Liver Neoplasms, Experimental, Lymphocytes, Tumor-Infiltrating, Cytopathogenic Effect, Viral, Animals, Vector (molecular biology), Rats, Inbred BUF, Molecular Biology, Inflammation, Oncolytic Virotherapy, biology, Vesiculovirus, biology.organism_classification, Natural killer T cell, Virology, Oncolytic virus, Rats, Specific Pathogen-Free Organisms, Killer Cells, Natural, Chemotaxis, Leukocyte, Viral replication, Vesicular stomatitis virus, Molecular Medicine, Natural Killer T-Cells, Tumor necrosis factor alpha, Immunocompetence

Abstract

Recombinant oncolytic viruses represent a promising alternative option for the treatment of malignant cancers. We have reported earlier the safety and efficacy of recombinant vesicular stomatitis virus (VSV) vectors in a rat model of hepatocellular carcinoma (HCC). However, the full potential of VSV therapy is limited by a sudden decline in intratumoral virus replication observed early after viral administration, a phenomenon that coincides with an accumulation of inflammatory cells within infected lesions. To overcome the antiviral function of these cells, we present a recombinant virus, rVSV-UL141, which expresses a protein from human cytomegalovirus known to downregulate the natural killer (NK) cell-activating ligand CD155. The modified vector resulted in an inhibition of NK cell recruitment in vitro, as well as decreased intratumoral accumulations of NK and NKT cells in vivo. Administration of rVSV-UL141 through hepatic artery infusion in immune-competent Buffalo rats harboring orthotopic, multi-focal HCC lesions resulted in a one-log elevation of intratumoral virus replication over a control rVSV vector, which translated to enhance tumor necrosis and substantial prolongation of survival. Moreover, these results were achieved in the absence of apparent toxicities. The present study suggests the applicability of this strategy for the development of effective and safe oncolytic agents to treat multi-focal HCC, and potentially a multitude of other cancers, in the future.

Published

2008

16. FoxO1 mediates insulin-dependent regulation of hepatic VLDL production in mice

Author

Germán Perdomo, Dongming Su, Adama Kamagate, Sandra Slusher, H. Henry Dong, Shen Qu, Dae Hyun Kim, Marcia Meseck, and American Diabetes Association

Subjects

endocrine system, Very low-density lipoprotein, medicine.medical_specialty, Transgene, medicine.medical_treatment, FOXO1, Biology, Lipoproteins, VLDL, digestive system, Models, Biological, Microsomal triglyceride transfer protein, Mice, Internal medicine, medicine, Animals, Humans, Insulin, Transcription factor, Triglycerides, Forkhead Box Protein O1, Hypertriglyceridemia, nutritional and metabolic diseases, Forkhead Transcription Factors, General Medicine, medicine.disease, Mice, Inbred C57BL, Insulin receptor, Endocrinology, Glucose, Gene Expression Regulation, Liver, biology.protein, Commentary, lipids (amino acids, peptides, and proteins), RNA Interference, Carrier Proteins, hormones, hormone substitutes, and hormone antagonists, Signal Transduction

Abstract

Excessive production of triglyceride-rich VLDL is attributable to hypertriglyceridemia. VLDL production is facilitated by microsomal triglyceride transfer protein (MTP) in a rate-limiting step that is regulated by insulin. To characterize the underlying mechanism, we studied hepatic MTP regulation by forkhead box O1 (FoxO1), a transcription factor that plays a key role in hepatic insulin signaling. In HepG2 cells, MTP expression was induced by FoxO1 and inhibited by exposure to insulin. This effect correlated with the ability of FoxO1 to bind and stimulate MTP promoter activity. Deletion or mutation of the FoxO1 target site within the MTP promoter disabled FoxO1 binding and resulted in abolition of insulin-dependent regulation of MTP expression. We generated mice that expressed a constitutively active FoxO1 transgene and found that increased FoxO1 activity was associated with enhanced MTP expression, augmented VLDL production, and elevated plasma triglyceride levels. In contrast, RNAi-mediated silencing of hepatic FoxO1 was associated with reduced MTP and VLDL production in adult mice. Furthermore, we found that hepatic FoxO1 abundance and MTP production were increased in mice with abnormal triglyceride metabolism. These data suggest that FoxO1 mediates insulin regulation of MTP production and that augmented MTP levels may be a causative factor for VLDL overproduction and hypertriglyceridemia in diabetes., This study was supported in part by the American Diabetes Association and NIH grant DK066301.

Published

2007

17. Aberrant Forkhead Box O1 Function Is Associated with Impaired Hepatic Metabolism

Author

Germán Perdomo, Marcia Meseck, H. Henry Dong, Shen Qu, Jennifer Altomonte, Yong Fan, Jing He, Adama Kamagate, and National Institutes of Health (US)

Subjects

medicine.medical_specialty, endocrine system, medicine.medical_treatment, Mice, Obese, FOXO1, Mice, Transgenic, Receptors, Cell Surface, Biology, Carbohydrate metabolism, Article, Impaired glucose tolerance, chemistry.chemical_compound, Mice, Endocrinology, Diabetes mellitus, Internal medicine, medicine, Animals, Humans, Tissue Distribution, Cells, Cultured, Glycogen, Forkhead Box Protein O1, Insulin, Fatty Acids, Forkhead Transcription Factors, Fasting, medicine.disease, Liver Glycogen, Mice, Inbred C57BL, Fatty acid synthase, Glucose, chemistry, Liver, biology.protein, Diet, Atherogenic, Receptors, Leptin, Steatosis

Abstract

FoxO1 plays an important role in mediating the effect of insulin on hepatic metabolism. Increased FoxO1 activity is associated with reduced ability of insulin to regulate hepatic glucose production. However, the underlying mechanism and physiology remain unknown. We studied the effect of FoxO1 on the ability of insulin to regulate hepatic metabolism in normal vs. insulin-resistant liver under fed and fasting conditions. FoxO1 gain of function, as a result of adenovirus-mediated or transgenic expression, augmented hepatic gluconeogenesis, accompanied by decreased glycogen content and increased fat deposition in liver. Mice with excessive FoxO1 activity exhibited impaired glucose tolerance. Conversely, FoxO1 loss of function, caused by hepatic production of its dominant-negative variant, suppressed hepatic gluconeogenesis, resulting in enhanced glucose disposal and improved insulin sensitivity in db/db mice. FoxO1 expression becomes deregulated, culminating in increased nuclear localization and accounting for its increased transcription activity in livers of both high fat-induced obese mice and diabetic db/db mice. Increased FoxO1 activity resulted in up-regulation of hepatic peroxisome proliferator-activated receptor-γ coactivator-1β, fatty acid synthase, and acetyl CoA carboxylase expression, accounting for increased hepatic fat infiltration. These data indicate that hepatic FoxO1 deregulation impairs the ability of insulin to regulate hepatic metabolism, contributing to the development of hepatic steatosis and abnormal metabolism in diabetes., This work was supported by National Institutes of Health Grant DK066301.

Published

2006

18. Inhibition of Foxo1 function is associated with improved fasting glycemia in diabetic mice

Author

Jenny Suriawinata, Jun Nakae, Domenico Accili, Sonal Harbaran, Jennifer Altomonte, Marcia Meseck, Swan N. Thung, Anja Richter, and H. Henry Dong

Subjects

Blood Glucose, endocrine system, medicine.medical_specialty, Carcinoma, Hepatocellular, Physiology, Ratón, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Recombinant Fusion Proteins, FOXO1, Type 2 diabetes, Biology, Transfection, digestive system, Mice, Physiology (medical), Diabetes mellitus, Internal medicine, medicine, Tumor Cells, Cultured, Animals, Forkhead Box Protein O1, Insulin, Gluconeogenesis, food and beverages, nutritional and metabolic diseases, Diabetic mouse, Forkhead Transcription Factors, Fasting, medicine.disease, Endocrinology, Glucose, Diabetes Mellitus, Type 2, Gene Expression Regulation, Liver, Mutagenesis, Site-Directed, hormones, hormone substitutes, and hormone antagonists, Function (biology), Transcription Factors

Abstract

Excessive hepatic glucose production is a contributing factor to fasting hyperglycemia in diabetes. Insulin suppresses hepatic glucose production by inhibiting the expression of two gluconeogenic enzymes, phosphoenolpyruvate carboxykinase (PEPCK) and glucose-6-phosphatase (G-6-Pase). The forkhead transcription factor Foxo1 has been implicated as a mediator of insulin action in regulating hepatic gluconeogenesis, and a Foxo1 mutant (Foxo1-Delta256), devoid of its carboxyl domain, has been shown to interfere with Foxo1 function and inhibit gluconeogenic gene expression in cultured cells. To study the effect of Foxo1-Delta256 on glucose metabolism in animals, the Foxo1-Delta256 cDNA was delivered to the livers of mice by adenovirus-mediated gene transfer. Hepatic Foxo1-Delta256 production resulted in inhibition of gluconeogenic activity, as evidenced by reduced PEPCK and G-6-Pase expression in the liver. Mice treated with the Foxo1-Delta256 vector exhibited significantly reduced blood glucose levels. In contrast, blood glucose levels in control vector-treated animals remained unchanged, which coincided with the lack of alterations in the expression levels of PEPCK and G-6-Pase. When tested in diabetic db/db mice, hepatic production of Foxo1-Delta256 was shown to reduce fasting hyperglycemia. Furthermore, we showed that hepatic Foxo1 expression was deregulated as a result of insulin resistance in diabetic mice and that Foxo1-Delta256 interfered with Foxo1 function via competitive binding to target promoters. These results demonstrated that functional inhibition of Foxo1, caused by hepatic expression of its mutant, is associated with reduced hepatic gluconeogenic activity and improved fasting glycemia in diabetic mice.

Published

2003

19. IFN-gamma sensitization of prostate cancer cells to Fas-mediated death: a gene therapy approach

Author

Steven E. Canfield, Shu Hsia Chen, Waleed A. Hassen, William Selleck, Randy C. Eisensmith, Marcia Meseck, Simon J. Hall, and Alexei I. Kuzmin

Subjects

Male, Transcriptional Activation, Programmed cell death, Fas Ligand Protein, Time Factors, Cell Survival, Genetic enhancement, Genetic Vectors, Apoptosis, Biology, Fas ligand, Adenoviridae, Prostate cancer, Interferon-gamma, Mice, LNCaP, Drug Discovery, medicine, Genetics, In Situ Nick-End Labeling, Tumor Cells, Cultured, Animals, Humans, fas Receptor, Molecular Biology, Pharmacology, Membrane Glycoproteins, Prostatic Neoplasms, Genetic Therapy, medicine.disease, Interleukin-12, Mice, Inbred C57BL, Cell culture, Immunology, Interleukin 12, Cancer research, Molecular Medicine

Abstract

While human prostate cancers and cell lines express Fas, most of these cell lines are resistant to Fas-mediated death. In the present studies we addressed the ability of IFN-gamma to influence Fas-mediated cell death in prostate cancer cells. In vitro exposure of the human cell lines LNCaP and PC3 and the mouse cell line RM-1 to agonist anti-Fas antibody and/or soluble Fas ligand resulted in killing of only PC3 cells. However, preincubation with IFN-gamma resulted in synergistic killing in all three cell lines. In vitro treatment of RM-1 with a replication-incompetent adenovirus expressing mouse FasL (Ad.FasL) resulted in maximal cell kill near 40%, which correlated with baseline Fas expression. The addition of IFN-gamma enhanced cell kill to a degree consistent with the resulting higher levels of Fas and maintained synergistic killing at very low doses of vector. Co-inoculation of orthotopic RM-1 primary tumors with Ad.mFasL and an adenovirus expressing mouse IL-12 (Ad.mIL-12) to drive host production of IFN-gamma negated the survival advantage of Ad.mIL-12 alone. However, the staggered injection of Ad.mIL-12 and Ad.FasL achieved almost threefold higher levels of apoptosis in primary tumor tissue and doubled median survival. Therefore, IFN-gamma is capable of bestowing increased sensitivity to Fas-mediated cell death in prostate cancer cells and, in a gene therapy approach, may define a powerful tool to treat prostate cancers.

Published

2003

20. Myeloid derived suppressor cells (MDSCs) assume an M1 phenotype when exposed to vesicular stomatitis virus, synergistically treating tumors

Author

Brian A. Coakley, Ping-Ying Pan, Samuel Eisenstein, Savio L. C. Woo, Shu Hsia Chen, Marcia Meseck, Ge Ma, and Celia M. Divino

Subjects

biology, Vesicular stomatitis virus, business.industry, Myeloid-derived Suppressor Cell, Medicine, Surgery, biology.organism_classification, business, Phenotype, Virology

Published

2012

21. Adenovirus-mediated expression of glucokinase in the liver as an adjuvant treatment for type 1 diabetes

Author

Jennifer Altomonte, Savio L. C. Woo, Robert C McEvoy, Marcia Meseck, H. Henry Dong, Núria Morral, and Swan N. Thung

Subjects

medicine.medical_specialty, medicine.medical_treatment, Genetic enhancement, Genetic Vectors, Biology, Adenoviridae, Diabetes mellitus, Internal medicine, Glucokinase, Genetics, medicine, Glucose homeostasis, Hypoglycemic Agents, Insulin, Molecular Biology, Triglycerides, Type 1 diabetes, Genetic transfer, Genetic Therapy, medicine.disease, Streptozotocin, Lipid Metabolism, Endocrinology, Diabetes Mellitus, Type 1, Glucose, Liver, Molecular Medicine, Glycogen, medicine.drug

Abstract

Glucokinase (GK) plays a crucial role in hepatic glucose disposal. Its activity is decreased in patients with maturity-onset diabetes of the young and in some animal models of diabetes. We investigated the feasibility of manipulating GK expression as an adjuvant treatment for type 1 diabetes, using an E1/E3-deleted adenoviral vector (Ad.EF1(alpha)GK) delivered to the liver of streptozotocin-induced type 1 diabetic rats. First, we studied the metabolic impact of constitutive glucokinase expression in the absence of insulin. Normal blood glucose levels were observed after gene transfer, and glucose tolerance was substantially enhanced compared with diabetic control animals, suggesting that hepatic GK expression is a feasible mechanism to enhance glucose disposal. In a second study we administered Ad.EF1(alpha)GK together with subcutaneous insulin injections to determine whether the combined action of insulin plus GK activity would provide better glucose homeostasis than insulin treatment alone. This combination approach resulted in constant, near-normal glucose values under fed conditions. Furthermore, the animals stayed in the normoglycemic range after an overnight fast, indicating that the risk to develop hypoglycemia is not increased by expression of GK. Alterations of other metabolic routes were observed, suggesting that insulin-regulated expression of GK may be necessary to use the strategy as a treatment of type 1 diabetes.

Published

2002

22. 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

23. Employing Myeloid Derived Suppressor Cells As A Novel Vector For Tumor Specific Treatment Delivery

Author

Savio L. C. Woo, Brian A. Coakley, Ge Ma, K.B. Saebo, Celia M. Divino, Shu Hsia Chen, Marcia Meseck, and Samuel Eisenstein

Subjects

Treatment delivery, Tumor specific, Myeloid-derived Suppressor Cell, Cancer research, Surgery, Vector (molecular biology), Biology

Published

2011