Your search keyword '"David A. Zaharoff"' showing total 20 results

1. Safety and Pharmacokinetics of Intravesical Chitosan/Interleukin-12 Immunotherapy in Murine Bladders

Author

Maura R. Vrabel, Khue G. Nguyen, Siena M. Mantooth, Ethan S. Wagner, David A. Zaharoff, and Danielle M. Meritet

Subjects

Chitosan, chemistry.chemical_compound, Oncology, chemistry, Pharmacokinetics, business.industry, Urology, medicine.medical_treatment, Interleukin 12, medicine, Immunotherapy, Pharmacology, business

Abstract

BACKGROUND: Intravesical administration of interleukin 12 (IL-12) co-formulated with the biopolymer, chitosan (CS/IL-12), has demonstrated remarkable antitumor activity against preclinical models of bladder cancer. However, given historical concerns regarding severe toxicities associated with systemic IL-12 administration in clinical trials, it is important to evaluate the safety of intravesical CS/IL-12 prior to clinical translation. OBJECTIVE: To evaluate the pharmacokinetics as well as the local and systemic toxicities of intravesical CS/IL-12 immunotherapy in laboratory mice. METHODS: Local inflammatory responses in mouse bladders treated with intravesical IL-12 or CS/IL-12 were assessed via histopathology. Serum cytokine levels following intravesical and subcutaneous (s.c.) administrations of IL-12 or CS/IL-12 in laboratory mice were compared. Systemic toxicities were evaluated via body weight and liver enzyme levels. RESULTS: Intravesical IL-12 and CS/IL-12 treatments did not induce significant local or systemic toxicity. IL-12 dissemination and exposure from intravesical administration was significantly lower compared to s.c. injections. Weekly intravesical CS/IL-12 treatments were well-tolerated and did not result in blunted immune responses. CONCLUSIONS: Intravesical CS/IL-12 is safe and well-tolerated in mice. In particular, the lack of cystitis and acute inflammation justifies continued investigation of intravesical CS/IL-12 immunotherapy in larger animals and patients with bladder cancer.

Published

2021

2. Construction of heparan sulfate microarray for investigating the binding of specific saccharide sequences to proteins

Author

Lin Yi, David A. Zaharoff, Robert J. Linhardt, Maurice Horton, Vijayakanth Pagadala, Yongmei Xu, Fuming Zhang, Jian Liu, Zhangjie Wang, Ken H. Pearce, and Guowei Su

Subjects

Glycan, Microarray, Antithrombin III, 010402 general chemistry, 01 natural sciences, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Sulfation, Carbohydrate Conformation, medicine, Extracellular, Humans, Fibroblast, 030304 developmental biology, 0303 health sciences, Binding Sites, biology, Chemistry, Heparan sulfate, Microarray Analysis, 0104 chemical sciences, medicine.anatomical_structure, Carbohydrate Sequence, Analytical Glycobiology, biology.protein, Fibroblast Growth Factor 2, Heparitin Sulfate, DNA microarray, Function (biology)

Abstract

Heparan sulfate (HS) is a heterogeneous, extracellular glycan that interacts with proteins and other molecules affecting many biological processes. The specific binding motifs of HS interactions are of interest, but have not been extensively characterized. Glycan microarrays are valuable tools that can be used to probe the interactions between glycans and their ligands while relying on relatively small amounts of samples. Recently, chemoenzymatic synthesis of HS has been employed to produce specific HS structures that can otherwise be difficult to produce. In this study, a microarray of diverse chemoenzymatically synthesized HS structures was developed and HS interactions were characterized. Fluorescently labeled antithrombin III (AT) and fibroblast growth factor-2 (FGF2) were screened against 95 different HS structures under three different printing concentrations to confirm the utility of this microarray. Specific sulfation patterns were found to be important for binding to these proteins and results are consistent with previous specificity studies. Furthermore, the binding affinities (KD,surf) of AT and FGF2 to multiple HS structures were determined using a microarray technique and is consistent with previous reports. Lastly, the 95-compound HS microarray was used to determine the distinct binding profiles for interleukin 12 and platelet factor 4. This technique is ideal for rapid expansion and will be pivotal to the high-throughput characterization of biologically important structure/function relationships.

Published

2020

3. Molecular mechanisms of heparin-induced modulation of human interleukin 12 bioactivity

Author

Francis B. Gillam, Jared J. Hopkins, David A. Zaharoff, Suresh Kumar Thallapuranam, Rashmi Jalah, Barbara K. Felber, Jian Liu, Ravi Kumar Gundampati, Guy R. Pilkington, Khue G. Nguyen, Srinivas Jayanthi, Guowei Su, and Jenifer Bear

Subjects

0301 basic medicine, endocrine system, T-Lymphocytes, medicine.medical_treatment, Immunology, Calorimetry, Biochemistry, Biophysical Phenomena, Flow cytometry, Glycosaminoglycan, Mice, 03 medical and health sciences, chemistry.chemical_compound, Sulfation, medicine, Animals, Humans, Receptor, Molecular Biology, Dose-Response Relationship, Drug, 030102 biochemistry & molecular biology, medicine.diagnostic_test, Heparin, Receptors, Interleukin-2, Cell Biology, Heparan sulfate, Flow Cytometry, Interleukin-12, Recombinant Proteins, Mice, Inbred C57BL, HEK293 Cells, 030104 developmental biology, Cytokine, chemistry, Interleukin 12, Cytokines, Female, Heparitin Sulfate, Protein Binding, Signal Transduction, medicine.drug

Abstract

Human interleukin-12 (hIL-12) is a heparin-binding cytokine whose activity was previously shown to be enhanced by heparin and other sulfated glycosaminoglycans. The current study investigated the mechanisms by which heparin increases hIL-12 activity. Using multiple human cell types, including natural killer cells, an IL-12 indicator cell line, and primary peripheral blood mononuclear and T cells, along with bioactivity, flow cytometry, and isothermal titration calorimetry assays, we found that heparin-dependent modulation of hIL-12 function correlates with several of heparin's biophysical characteristics, including chain length, sulfation level, and concentration. Specifically, only heparin molecules longer than eight saccharide units enhanced hIL-12 activity. Furthermore, heparin molecules with three sulfate groups per disaccharide unit outperformed heparin molecules with one or two sulfate groups per disaccharide unit in terms of enhanced hIL-12 binding and activity. Heparin also significantly reduced the EC(50) value of hIL-12 by up to 11.8-fold, depending on the responding cell type. Cytokine-profiling analyses revealed that heparin affected the level, but not the type, of cytokines produced by lymphocytes in response to hIL-12. Interestingly, although murine IL-12 also binds heparin, heparin did not enhance its activity. Using the gathered data, we propose a model of hIL-12 stabilization in which heparin serves as a co-receptor enhancing the interaction between heterodimeric hIL-12 and its receptor subunits. The results of this study provide a foundation for further investigation of heparin's interactions with IL-12 family cytokines and for the use of heparin as an immunomodulatory agent.

Published

2019

4. Modulation of Interleukin-12 activity in the presence of heparin

Author

Srinivas Jayanthi, Sean G. Smith, David A. Zaharoff, Khue G. Nguyen, Barbara K. Felber, Thallapuranam Krishnaswamy Suresh Kumar, and Bhanu prasanth Koppolu

Subjects

0301 basic medicine, endocrine system, Protein Conformation, Science, Plasma protein binding, Biophysical Phenomena, Interleukin-12 Subunit p35, Article, Cell Line, Flow cytometry, Glycosaminoglycan, 03 medical and health sciences, chemistry.chemical_compound, Scattering, Small Angle, medicine, Humans, Immunologic Factors, Receptor, Multidisciplinary, 030102 biochemistry & molecular biology, medicine.diagnostic_test, Heparin, Chemistry, Biological activity, Heparan sulfate, Flow Cytometry, Interleukin-12, In vitro, 3. Good health, 030104 developmental biology, Biochemistry, Chromatography, Gel, Medicine, Heparitin Sulfate, Protein Multimerization, Protein Binding, medicine.drug

Abstract

Glycosaminoglycans (GAGs), especially heparin and heparan sulfate (HS), modulate the functions of numerous cytokines. The aims of this multidisciplinary research were to characterize heparin binding to interleukin-12 (IL-12) and determine the mechanism(s) by which heparin influences IL-12 bioactivity. Heparin and HS were found to bind human IL-12 (hIL-12) with low micromolar affinity and increase hIL-12 bioactivity by more than 6-fold. Conversely, other GAGs did not demonstrate significant binding, nor did their addition affect hIL-12 bioactivity. Biophysical studies demonstrated that heparin induced only minor conformational changes while size-exclusion chromatography and small angle X-ray scattering studies indicated that heparin induced dimerization of hIL-12. Heparin modestly protected hIL-12 from proteolytic degradation, however, this was not a likely mechanism for increased cytokine activity in vitro. Flow cytometry studies revealed that heparin increased the amount of hIL-12 bound to cell surfaces. Heparin also facilitated hIL-12 binding and signaling in cells in which both hIL-12 receptor subunits were functionally deleted. Results of this study demonstrate a new role for heparin in modulating the biological activity of IL-12.

Published

2017

5. Effect of Chitosan Properties on Immunoreactivity

Author

Sruthi Ravindranathan, Sean G. Smith, David A. Zaharoff, and Bhanu prasanth Koppolu

Subjects

0301 basic medicine, endotoxin, Polymers, Surface Properties, Antigen-Presenting Cells, Pharmaceutical Science, Biocompatible Materials, 02 engineering and technology, macromolecular substances, Gene delivery, Article, immune response, Cell Line, Microbiology, Chitosan, Mice, 03 medical and health sciences, chemistry.chemical_compound, Immune system, Tissue engineering, Drug Discovery, Animals, Humans, Particle Size, Antigen-presenting cell, lcsh:QH301-705.5, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Tissue Engineering, Tumor Necrosis Factor-alpha, Viscosity, Chemistry, Macrophages, Gene Transfer Techniques, technology, industry, and agriculture, Biomaterial, Dendritic Cells, 021001 nanoscience & nanotechnology, Mice, Inbred C57BL, carbohydrates (lipids), 030104 developmental biology, lcsh:Biology (General), Biochemistry, Cell culture, chitosan, immunoreactivity, Female, Tumor necrosis factor alpha, 0210 nano-technology

Abstract

Chitosan is a widely investigated biopolymer in drug and gene delivery, tissue engineering and vaccine development. However, the immune response to chitosan is not clearly understood due to contradicting results in literature regarding its immunoreactivity. Thus, in this study, we analyzed effects of various biochemical properties, namely degree of deacetylation (DDA), viscosity/polymer length and endotoxin levels, on immune responses by antigen presenting cells (APCs). Chitosan solutions from various sources were treated with mouse and human APCs (macrophages and/or dendritic cells) and the amount of tumor necrosis factor-α (TNF-α) released by the cells was used as an indicator of immunoreactivity. Our results indicate that only endotoxin content and not DDA or viscosity influenced chitosan-induced immune responses. Our data also indicate that low endotoxin chitosan (

Published

2016

6. Preclinical and Clinical Use of Chitosan and Derivatives for Biopharmaceuticals: From Preclinical Research to the Bedside

Author

David A. Zaharoff, Michael J. Heffernan, Jonathan K. Fallon, and John W. Greiner

Subjects

Chitosan, chemistry.chemical_compound, Preclinical research, chemistry, business.industry, Medicine, Pharmacology, business

Published

2012

7. Chitosan solution enhances the immunoadjuvant properties of GM-CSF

Author

John W. Greiner, Kenneth W. Hance, Connie J. Rogers, David A. Zaharoff, and Jeffrey Schlom

Subjects

CD4-Positive T-Lymphocytes, Injections, Subcutaneous, T cell, Antigen presentation, Gene Expression, CD8-Positive T-Lymphocytes, Pharmacology, Biology, Immunoadjuvant, Article, Chitosan, Mice, chemistry.chemical_compound, Adjuvants, Immunologic, Antigen, medicine, Animals, Cytotoxic T cell, Cell Proliferation, Antigen Presentation, General Veterinary, General Immunology and Microbiology, Histocompatibility Antigens Class II, Public Health, Environmental and Occupational Health, Granulocyte-Macrophage Colony-Stimulating Factor, Dendritic Cells, Dendritic cell, Cytotoxicity Tests, Immunologic, Lymphocyte Subsets, Infectious Diseases, medicine.anatomical_structure, chemistry, Delayed-Action Preparations, Immunology, Molecular Medicine, Female, Lymph Nodes, CD8, T-Lymphocytes, Cytotoxic

Abstract

Sustained, local delivery of immunomodulatory cytokines is under investigation for its ability to enhance vaccine and anti-tumor responses both clinically and preclinically. This study evaluates the ability of chitosan, a biocompatible polysaccharide, to (1) control the dissemination of a cytokine, GM-CSF, and (2) enhance the immunoadjuvant properties of GM-CSF. While cytokines have previously been delivered in lipid-based adjuvants and other vehicles, these do not have the clinical safety profile or unique properties of chitosan. We found that chitosan solution maintained a measurable depot of recombinant GM-CSF (rGM-CSF) at a subcutaneous injection site for up to 9 days. In contrast, when delivered in a saline vehicle, rGM-CSF was undetectable in 12-24h. Furthermore, a single s.c. injection of 20 microg rGM-CSF in chitosan solution (chitosan/rGM-CSF(20 microg)) transiently expanded lymph nodes up to 4.6-fold and increased the number of MHC class II expressing cells and dendritic cells by 7.4-fold and 6.8-fold, respectively. These increases were significantly greater than those measured when rGM-CSF was administered in saline at the standard preclinical dose and schedule, i.e. 4 daily s.c. injections of 20 microg. Furthermore, lymph node cells from mice injected with chitosan/rGM-CSF(20 microg) induced greater allogeneic T cell proliferation, indicating enhanced antigen presenting capability, than lymph node cells from mice injected with rGM-CSF alone. Finally, in vaccination experiments, chitosan/rGM-CSF was superior to either chitosan or rGM-CSF alone in enhancing the induction of antigen-specific CD4(+) proliferation, peptide-specific CD8(+) pentamer staining and cytotoxic T cell lysis. Altogether, chitosan/rGM-CSF outperformed standard rGM-CSF administrations in dendritic cell recruitment, antigen presentation and vaccine enhancement. We conclude that chitosan solution is a promising delivery platform for the sustained, local delivery of rGM-CSF.

Published

2007

8. Chitosan solution enhances both humoral and cell-mediated immune responses to subcutaneous vaccination

Author

Connie J. Rogers, John W. Greiner, Jeffrey Schlom, David A. Zaharoff, and Kenneth W. Hance

Subjects

CD4-Positive T-Lymphocytes, Injections, Subcutaneous, medicine.medical_treatment, Freund's Adjuvant, Aluminum Hydroxide, Enzyme-Linked Immunosorbent Assay, macromolecular substances, Immunopotentiator, Biology, Pharmacology, Lymphocyte Activation, Antibodies, Article, Chitosan, Mice, chemistry.chemical_compound, Immune system, Adjuvants, Immunologic, Antigen, medicine, Animals, Hypersensitivity, Delayed, Skin, Vaccines, General Veterinary, General Immunology and Microbiology, Histocytochemistry, Vaccination, technology, industry, and agriculture, Public Health, Environmental and Occupational Health, beta-Galactosidase, equipment and supplies, Lipids, Mice, Inbred C57BL, carbohydrates (lipids), Infectious Diseases, chemistry, Freund's adjuvant, Models, Animal, Humoral immunity, Immunology, biology.protein, Molecular Medicine, Female, Lymph Nodes, Antibody, Adjuvant

Abstract

The development of safe, novel adjuvants is necessary to maximize the efficacy of new and/or available vaccines. Chitosan is a non-toxic, biocompatible, biodegradable, natural polysaccharide derived from the exoskeletons of crustaceans and insects. Chitosan's biodegradability, immunological activity and high viscosity make it an excellent candidate as a depot/adjuvant for parenteral vaccination. To this end, we explored chitosan solution as an adjuvant for subcutaneous vaccination of mice with a model protein antigen. We found that chitosan enhanced antigen-specific antibody titers over five-fold and antigen-specific splenic CD4+ proliferation over six-fold. Strong increases in antibody titers together with robust delayed-type hypersensitivity (DTH) responses revealed that chitosan induced both humoral and cell-mediated immune responses. When compared with traditional vaccine adjuvants, chitosan was equipotent to incomplete Freund's adjuvant (IFA) and superior to aluminum hydroxide. Mechanistic studies revealed that chitosan exhibited at least two characteristics that may allow it to function as an immune adjuvant. First, the viscous chitosan solution created an antigen depot. More specifically, less than 9% of a protein antigen, when delivered in saline, remained at the injection site after 8 h. However, more than 60% of a protein antigen delivered in chitosan remained at the injection site for 7 days. Second, chitosan induced a transient 67% cellular expansion in draining lymph nodes. The expansion peaked between 14 and 21 days after chitosan injection and diminished as the polysaccharide was degraded. These mechanistic studies, taken together with the enhancement of a vaccine response, demonstrate that chitosan is a promising and safe platform for parenteral vaccine delivery.

Published

2007

9. Effects of pulse strength and pulse duration on in vitro DNA electromobility

Author

Fan Yuan and David A. Zaharoff

Subjects

Ions, Pulse (signal processing), Gene Transfer Techniques, Biophysics, Pulse duration, DNA, General Medicine, In Vitro Techniques, Gene delivery, Biology, Molecular biology, Fluorescence, Electrophoresis, Gel, Pulsed-Field, chemistry.chemical_compound, Electrophoresis, Plasmid, chemistry, Electric field, Electrochemistry, Agarose, Physical and Theoretical Chemistry, Gels, Plasmids

Abstract

Interstitial transport of DNA is a rate-limiting step in electric field-mediated gene delivery in vivo. Interstitial transport of macromolecules, such as plasmid DNA, over a distance of several cell layers, is inefficient due to small diffusion coefficient and inadequate convection. Therefore, we explored electric field as a novel driving force for interstitial transport of plasmid DNA. In this study, agarose gels were used to mimic the interstitium in tissues as they had been well characterized and could be prepared reproducibly. We measured the electrophoretic movements of fluorescently labeled plasmid DNA in agarose gels with three different concentrations (1.0%, 2.0% and 3.0%) subjected to electric pulses at three different field strengths (100, 200 and 400 V/cm) and four different pulse durations (10, 50, 75, 99 ms). We observed that: (1) shorter pulses (10 ms) were not as efficient as longer pulses in facilitating plasmid transport through agarose gels; (2) plasmid electromobility reached a plateau at longer pulse durations; and (3) plasmid electromobility increased with applied electric energy, up to a threshold, in all three gels. These data suggested that both pulse strength and duration needed to be adequately high for efficient plasmid transport through extracellular matrix. We also found that electric field was better than concentration gradient of DNA as a driving force for interstitial transport of plasmid DNA.

Published

2004

10. Intravesical chitosan/interleukin-12 immunotherapy induces tumor-specific systemic immunity against murine bladder cancer

Author

Matthew D. Katz, Sean G. Smith, David A. Zaharoff, Lirong Yang, Sruthi Ravindranathan, Bhanu prasanth Koppolu, and Samantha L. Kurtz

Subjects

Cancer Research, medicine.medical_treatment, Immunology, Dose-Response Relationship, Immunologic, Article, Chitosan, chemistry.chemical_compound, Mice, Random Allocation, Immunity, Cell Line, Tumor, medicine, Splenocyte, Immunology and Allergy, Animals, Mice, Inbred C3H, Bladder cancer, business.industry, Immunotherapy, medicine.disease, Acquired immune system, Interleukin-12, In vitro, Mice, Inbred C57BL, Administration, Intravesical, Oncology, chemistry, Urinary Bladder Neoplasms, Interleukin 12, Female, business

Abstract

Bladder cancer is a highly recurrent disease in need of novel, durable treatment strategies. This study assessed the ability of an intravesical immunotherapy composed of a coformulation of the biopolymer chitosan with interleukin-12 (CS/IL-12) to induce systemic adaptive tumor-specific immunity. Intravesical CS/IL-12 immunotherapy was used to treat established orthotopic MB49 and MBT-2 bladder tumors. All mice receiving intravesical CS/IL-12 immunotherapy experienced high cure rates of orthotopic disease. To investigate the durability and extent of the resultant adaptive immune response, cured mice were rechallenged both locally (intravesically) and distally. Cured mice rejected 100 % of intravesical tumor rechallenges and 50–100 % of distant subcutaneous rechallenges in a tumor-specific manner. The ability of splenocytes from cured mice to lyse targets in a tumor-specific manner was assessed in vitro, revealing that lytic activity of splenocytes from cured mice was robust and tumor specific. Protective immunity was durable, lasting for at least 18 months after immunotherapy. In an advanced bladder cancer model, intravesical CS/IL-12 immunotherapy controlled simultaneous orthotopic and subcutaneous tumors in 70 % of treated mice. Intravesical CS/IL-12 immunotherapy creates a robust and durable tumor-specific adaptive immune response against bladder cancer. The specificity, durability, and potential of this therapy to treat both superficial and advanced disease are deserving of consideration for clinical translation.

Published

2014

11. Controlling chitosan-based encapsulation for protein and vaccine delivery

Author

Bhanu prasanth Koppolu, Srinivas Jayanthi, Thallapuranam Krishnaswamy Suresh Kumar, Sruthi Ravindranathan, Sean G. Smith, and David A. Zaharoff

Subjects

Materials science, Hofmeister series, Sonication, Dispersity, Kinetics, Biophysics, Bioengineering, Calorimetry, macromolecular substances, Article, Biomaterials, Chitosan, chemistry.chemical_compound, Drug Delivery Systems, Nano, Chemical Precipitation, Particle Size, Vaccines, Chromatography, Sulfates, Osmolar Concentration, technology, industry, and agriculture, Water, Serum Albumin, Bovine, Molecular Weight, Solutions, Immobilized Proteins, chemistry, Chemical engineering, Mechanics of Materials, Ceramics and Composites, Thermodynamics, Particle size, Fluorescein-5-isothiocyanate, Protein Binding

Abstract

Chitosan-based nano/microencapsulation is under increasing investigation for the delivery of drugs, biologics and vaccines. Despite widespread interest, the literature lacks a defined methodology to control chitosan particle size and drug/protein release kinetics. In this study, the effects of precipitation–coacervation formulation parameters on chitosan particle size, protein encapsulation efficiency and protein release were investigated. Chitosan particle sizes, which ranged from 300 nm to 3 μm, were influenced by chitosan concentration, chitosan molecular weight and addition rate of precipitant salt. The composition of precipitant salt played a significant role in particle formation with upper Hofmeister series salts containing strongly hydrated anions yielding particles with a low polydispersity index (PDI) while weaker anions resulted in aggregated particles with high PDIs. Sonication power had minimal effect on mean particle size, however, it significantly reduced polydispersity. Protein loading efficiencies in chitosan nano/microparticles, which ranged from 14.3% to 99.2%, were inversely related to the hydration strength of precipitant salts, protein molecular weight and directly related to the concentration and molecular weight of chitosan. Protein release rates increased with particle size and were generally inversely related to protein molecular weight. This study demonstrates that chitosan nano/microparticles with high protein loading efficiencies can be engineered with well-defined sizes and controllable release kinetics through manipulation of specific formulation parameters.

Published

2013

12. 583 INTRAVESICAL IMMUNOTHERAPY WITH CHITOSAN AND INTERLEUKIN-12 INDUCES SYSTEMIC TUMOR-SPECIFIC IMMUNITY

Author

Lirong Yang, Jimmy Loc Nhu Vo, Sean G. Smith, and David A. Zaharoff

Subjects

Chitosan, chemistry.chemical_compound, chemistry, business.industry, Immunity, Urology, Tumor specific, Cancer research, Interleukin 12, Medicine, business, Intravesical chemotherapy

Published

2013

13. The effect of antigen encapsulation in chitosan particles on uptake, activation and presentation by antigen presenting cells

Author

David A. Zaharoff and Bhanu prasanth Koppolu

Subjects

Antigenicity, Materials science, Ovalbumin, Antigen presentation, Biophysics, Serum albumin, Antigen-Presenting Cells, Bioengineering, Biocompatible Materials, Article, Cell Line, Biomaterials, Chitosan, chemistry.chemical_compound, Mice, Co-stimulation, Antigen, Animals, Bovine serum albumin, Antigens, Particle Size, Antigen-presenting cell, Serum Albumin, Cell Proliferation, Antigen Presentation, biology, Macrophages, Dendritic Cells, Molecular biology, chemistry, Mechanics of Materials, Ceramics and Composites, biology.protein

Abstract

Particle-based vaccine delivery systems are under exploration to enhance antigen-specific immunity against safe but poorly immunogenic polypeptide antigens. Chitosan is a promising biomaterial for antigen encapsulation and delivery due to its ability to form nano- and microparticles in mild aqueous conditions thus preserving the antigenicity of loaded polypeptides. In this study, the influence of chitosan encapsulation on antigen uptake, activation and presentation by antigen presenting cells (APCs) is explored. Fluorescein isothiocyanate-labeled bovine serum albumin (FITC-BSA) and ovalbumin (OVA) were used as model protein antigens and encapsulated in chitosan particles via precipitation-coacervation at loading efficiencies >89%. Formulation conditions were manipulated to create antigen-encapsulated chitosan particles (AgCPs) with discrete nominal sizes (300 nm, 1 μm, and 3 μm). Uptake of AgCPs by dendritic cells and macrophages was found to be dependent on particle size, antigen concentration and exposure time. Flow cytometry analysis revealed that uptake of AgCPs enhanced upregulation of surface activation markers on APCs and increased the release of pro-inflammatory cytokines. Lastly, antigen-specific T cells exhibited higher proliferative responses when stimulated with APCs activated with AgCPs versus soluble antigen. These data suggest that encapsulation of antigens in chitosan particles enhances uptake, activation and presentation by APCs.

Published

2012

14. In vivo efficacy of a chitosan/IL-12 adjuvant system for protein-based vaccines

Author

David A. Zaharoff, John W. Greiner, Jeffrey Schlom, Jonathan K. Fallon, and Michael J. Heffernan

Subjects

CD4-Positive T-Lymphocytes, medicine.medical_treatment, Biophysics, Bioengineering, Enzyme-Linked Immunosorbent Assay, macromolecular substances, Biology, Pharmacology, Article, Biomaterials, Chitosan, chemistry.chemical_compound, Interferon-gamma, Mice, Immune system, Antigen, Adjuvants, Immunologic, Interferon, medicine, Splenocyte, Animals, Interferon gamma, Vaccines, technology, industry, and agriculture, Proteins, Molecular biology, Interleukin-12, Mice, Inbred C57BL, Ovalbumin, chemistry, Mechanics of Materials, Ceramics and Composites, biology.protein, Adjuvant, medicine.drug

Abstract

Vaccines based on recombinant proteins require adjuvant systems in order to generate Th1-type immune responses. We have developed a vaccine adjuvant system using a viscous chitosan solution and interleukin (IL)-12, a Th1-inducing cytokine. The chitosan solution is designed to create a depot of antigen and IL-12 at a subcutaneous injection site. We measured the in vivo immune response of a vaccine containing 0.25, 1, or 4 μg murine IL-12 and 75 μg ovalbumin (OVA), formulated in a 1.5% chitosan glutamate solution. The chitosan/IL-12/OVA vaccine, in comparison to chitosan/OVA, IL-12/OVA, or OVA alone, elicited greater antigen-specific CD4(+) and CD8(+) T-cell responses, as determined by CD4(+) splenocyte proliferation, Th1 cytokine release, CD8(+) T-cell interferon-γ release, and MHC class I peptide pentamer staining. The combination of chitosan and IL-12 also enhanced IgG2a and IgG2b antibody responses to OVA. Co-formulation of chitosan and IL-12 thus promoted the generation of a Th1 immune response to a model protein vaccine.

Published

2010

15. The antitumor and immunoadjuvant effects of IFN-alpha in combination with recombinant poxvirus vaccines

Author

Daniel Canter, Connie J. Rogers, David A. Zaharoff, Kenneth W. Hance, John W. Greiner, and Jeffrey Schlom

Subjects

Cancer Research, medicine.medical_treatment, Antigen presentation, DNA, Recombinant, Antineoplastic Agents, Mice, Transgenic, Vaccinia virus, Adenocarcinoma, Immunoadjuvant, Cancer Vaccines, Article, chemistry.chemical_compound, Mice, Carcinoembryonic antigen, Immune system, Adjuvants, Immunologic, Cell Line, Tumor, medicine, Animals, Fowlpox virus, biology, Histocompatibility Antigens Class I, Interferon-alpha, Combined Modality Therapy, Carcinoembryonic Antigen, Vaccination, Mice, Inbred C57BL, CTL, Cytokine, Phenotype, Oncology, chemistry, Immunology, biology.protein, Female, Lymph Nodes, Vaccinia

Abstract

Purpose: IFN-α is a pleiotropic cytokine possessing immunomodulatory properties that may improve the efficacy of therapeutic cancer vaccines. The aim of this study was to evaluate the effectiveness and compatibility of combining recombinant IFN-α with poxvirus vaccines targeting the human carcinoembryonic antigen (CEA) in murine models of colorectal and pancreatic adenocarcinomas, where CEA is a self-antigen.Experimental Design: The phenotypic and functional effects of IFN-α were evaluated in the draining inguinal lymph nodes of tumor-free mice. We studied the effect of the site of IFN-α administration (local versus distal) on antigen-specific immune responses to poxvirus vaccination. Mechanistic studies were conducted to assess the efficacy of IFN-α and CEA-directed poxvirus vaccines in tumor-bearing CEA transgenic mice.Results: We identified a dose and schedule of IFN-α that induced a locoregional expansion of the draining inguinal lymph nodes and improved cellular cytotoxicity (natural killer and CD8+) and antigen presentation. Suppression of the vaccinia virus was avoided by administering IFN-α distal to the site of vaccination. The combination of IFN-α and vaccine inhibited tumor growth, improved survival, and elicited CEA-specific CTL responses in mice with CEA+ adenocarcinomas. In mice with pancreatic tumors, IFN-α slowed tumor growth, induced CTL activity, and increased CD8+ tumor-infiltrating lymphocytes.Conclusions: These data suggest that IFN-α can be used as a biological response modifier with antigen-directed poxvirus vaccines to yield significant therapeutic antitumor immune responses. This study provides the rationale and mechanistic insights to support a clinical trial of this immunotherapeutic strategy in patients with CEA-expressing carcinomas.

Published

2009

16. Corrigendum to ‘Controlling chitosan-based encapsulation for protein and vaccine delivery’ [Biomaterials 35 (2014) 4382–4389]

Author

Thallapuranam Krishnaswamy Suresh Kumar, Bhanu prasanth Koppolu, Sean G. Smith, David A. Zaharoff, Srinivas Jayanthi, and Sruthi Ravindranathan

Subjects

Biomaterials, Chitosan, chemistry.chemical_compound, Mechanics of Materials, Chemistry, Biophysics, Ceramics and Composites, Bioengineering, Nanotechnology, Vaccine delivery, Encapsulation (networking)

Published

2015

17. Abstract 4404: A novel chitosan-based hydrogel for intratumoral release of immunotherapeutic cytokines

Author

Sean G. Smith, Bhanu prasanth Koppolu, David A. Zaharoff, Ethan D. Lowry, and Christopher Wallace

Subjects

Cancer Research, biology, business.industry, medicine.medical_treatment, Pharmacology, In vitro, Chitosan, chemistry.chemical_compound, Immune system, Cytokine, Oncology, chemistry, Cell culture, Immunology, medicine, biology.protein, Interferon gamma, Bovine serum albumin, Fluorescein isothiocyanate, business, medicine.drug

Abstract

Controlled delivery of IL-12 has been shown to stimulate the immune system to eliminate primary tumors and elicit tumor-specific, protective immunity. Recently, we have developed a novel in situ gelling chitosan-based hydrogel that appears capable of further improving cytokine delivery within the tumor microenvironment while preventing systemic dissemination of potentially toxic, pro-inflammatory cytokines. Change in viscosity during gelation was measured using a Brookfield DV-III Ultra Rheometer, revealing a 300-fold increase in viscosity. Manipulation of chitosan's chemical properties such as molecular weight, concentration, and degree of acetylation was found to control the time of gelation, which ranged from ten seconds to one minute. A protein release study was conducted using fluorescein isothiocyanate labeled bovine serum albumin (FITC-BSA) as a surrogate for IL-12. Dialysis tubes (with a molecular weight cutoff of 100kDa) were loaded with FITC-BSA co-formulated with hydrogel and FITC-BSA in PBS alone. The tubes were placed in a PBS bath and samples were taken at 48, 96, and 168 hours. The degree of release from the tubes was determined by measuring the fluorescence of protein in samples using a spectrofluorimeter. In vitro drug release studies demonstrated zero-order release of FITC-BSA from the hydrogel over a one-week period. Comparison to FITC-BSA in PBS indicates that the hydrogel exhibits a controlled kinetics profile. Bioactivity of IL-12 when co-formulated with the hydrogel was determined by quantifying the production of interferon gamma (IFNγ) by NK-92MI cells, a line of human Natural Killer immune cells. NK-92MI cells were grown in the presence of human IL-12 with and without the hydrogel, and IFNγ production was measured via ELISA. The bioactivity assay indicated that IL-12 bioactivity was not compromised when mixed with the hydrogel. Specifically, after a 24 hour incubation period, the amount of IFNγ produced by the NK-92MI cells was found to be similar between groups treated with IL-12 alone and IL-12/hydrogel co-formulation. After bioactivity was confirmed, mice (n = 3 per group) were subcutaneously injected with the mouse urothelial carcinoma cell line, MB49 (∼300,000 cells per mouse). After sufficient (approximately 50mm3) tumor growth, the mice were injected with either a hydrogel/IL-12 formulation or saline, which served as a control. Tumor volume was measured on days 7, 9, 14 and 19 after tumor implantation. In the anti-tumor study, mice treated with the IL-12/hydrogel co-formulation experience reduction in tumor size, while those treated with saline experience expected tumor growth. These studies demonstrate that a novel chitosan-based hydrogel allows for sustained delivery of antitumor cytokines without altering bioactivity. Citation Format: Ethan D. Lowry, Christopher Wallace, Bhanu prasanth Koppolu, Sean Smith, David Zaharoff. A novel chitosan-based hydrogel for intratumoral release of immunotherapeutic cytokines. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 4404. doi:10.1158/1538-7445.AM2015-4404

Published

2015

18. Effects of electric pulse strength and pulse duration on plasmid DNA electromobility

Author

David A. Zaharoff and Fan Yuan

Subjects

Electrophoresis, chemistry.chemical_compound, Materials science, Nuclear magnetic resonance, Plasmid, chemistry, Pulse (signal processing), Diffusion, Electric field, Analytical chemistry, Pulse duration, Agarose, Field strength

Abstract

Interstitial transport of DNA is a rate-limiting step in electric field-mediated gene delivery. Interstitial transport of macromolecules such as plasmid DNA is limited by small diffusion coefficient, large diffusion distance and inadequate convection. Here, we explore electric field as a novel interstitial driving force for plasmid DNA transport. We measured the electrophoretic movement, and hence, electromobility of fluorescently-labeled plasmid DNA in agarose gels of three concentrations (1, 2, and 3%), subjected to electric pulses at three levels of field strength (100, 200 and 400 V/cm) and four levels of pulse duration (10, 50, 75, 99 ms). In our experiments, electrophoresis is up to four orders of magnitude greater than diffusion for plasmid transport in agarose gel. In all gels, we found that shorter duration pulses (

Published

2003

19. Electromobility of plasmid DNA in tumor tissues during electric field-mediated gene delivery

Author

Roger C. Barr, Chuan-Yuan Li, Fan Yuan, and David A. Zaharoff

Subjects

Genetic enhancement, Genetic Vectors, Melanoma, Experimental, Gene delivery, Biology, chemistry.chemical_compound, Mice, Plasmid, Genetics, Animals, Molecular Biology, Mice, Inbred BALB C, Electroporation, Genetic transfer, Gene Transfer Techniques, Mammary Neoplasms, Experimental, Genetic Therapy, Molecular biology, Mice, Inbred C57BL, chemistry, Nucleic acid, Molecular Medicine, Feasibility Studies, Female, Collagen, Extracellular Space, Ex vivo, DNA, Plasmids

Abstract

Interstitial transport is a crucial step in plasmid DNA-based gene therapy. However, interstitial diffusion of large nucleic acids is prohibitively slow. Therefore, we proposed to facilitate interstitial transport of DNA via pulsed electric fields. To test the feasibility of this approach to gene delivery, we developed an ex vivo technique to quantify the magnitude of DNA movement due to pulsed electric fields in two tumor tissues: B16.F10 (a mouse melanoma) and 4T1 (a mouse mammary carcinoma). When the pulse duration and strength were 50 ms and 233 V/cm, respectively, we found that the average plasmid DNA movements per 10 pulses were 1.47 microm and 0.35 microm in B16.F10 and 4T1 tumors, respectively. The average plasmid DNA movements could be approximately tripled, ie to reach 3.69 microm and 1.01 microm, respectively, when the pulse strength was increased to 465 V/cm. The plasmid DNA mobility was correlated with the tumor collagen content, which was approximately eight times greater in 4T1 than in B16.F10 tumors. These data suggest that electric field can be a powerful driving force for improving interstitial transport of DNA during gene delivery.

Published

2001

20. Delivery of Plasmid DNA Through Intratumoral Infusion and Electroporation

Author

Frank Lohr, Xiao-Yu Zhang, Chuan-Yuan Li, Fan Yuan, Mark W. Dewhirst, and David A. Zaharoff

Subjects

chemistry.chemical_compound, Materials science, chemistry, Plasmid dna, Electroporation, Biophysics, Deformation (meteorology), DNA

Abstract

We investigated DNA transport in the interstitial space and across cell membrane facilitated by intratumoral infusion and in vivo electroporation, respectively. In the study, a rat fibrosarcoma was perfused ex vivo, and apparent hydraulic conductivity (Kapp) was quantified under different perfusion conditions. In addition, three plasmid DNA vectors were infused into solid tumors. Immediately after infusion, tumors were treated with or without electric pulses. Gene expression and tumor growth delay were determined at different time points after electroporation. We found that Kapp was very sensitive to the perfusion pressure, presumably due to perfusion-induced tissue deformation. Treatment of tumors with electric pulse facilitated gene expression in vivo. The growth of tumors treated with plasmid DNA encoding interleukin 12 (IL-12) and electric pulses was slower than those treated with IL-12 or electric pulses alone. These data suggest that gene delivery in solid tumors could be improved significantly through combination of intratumoral infusion and in vivo electroporation.

Published

2000