Your search keyword '"Stephen J. Russell"' showing total 39 results

1. Neoadjuvant systemic oncolytic vesicular stomatitis virus is safe and may enhance long-term survivorship in dogs with naturally occurring osteosarcoma

Author

Kelly M. Makielski, Aaron L. Sarver, Michael S. Henson, Kathleen M. Stuebner, Antonella Borgatti, Lukkana Suksanpaisan, Caitlin Preusser, Alexandru-Flaviu Tabaran, Ingrid Cornax, M. Gerard O’Sullivan, Andrea Chehadeh, Donna Groschen, Kelly Bergsrud, Sara Pracht, Amber Winter, Lauren J. Mills, Marc D. Schwabenlander, Melissa Wolfe, Michael A. Farrar, Gary R. Cutter, Joseph S. Koopmeiners, Stephen J. Russell, Jaime F. Modiano, and Shruthi Naik

Subjects

oncolytic virus, osteosarcoma, neoadjuvant, immunotherapy, virotherapy, tumor microenvironment, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Osteosarcoma is a devastating bone cancer that disproportionally afflicts children, adolescents, and young adults. Standard therapy includes surgical tumor resection combined with multiagent chemotherapy, but many patients still suffer from metastatic disease progression. Neoadjuvant systemic oncolytic virus (OV) therapy has the potential to improve clinical outcomes by targeting primary and metastatic tumor sites and inducing durable antitumor immune responses. Here we describe the first evaluation of neoadjuvant systemic therapy with a clinical-stage recombinant oncolytic vesicular stomatitis virus (VSV), VSV-IFNβ-NIS, in naturally occurring cancer, specifically appendicular osteosarcoma in companion dogs. Canine osteosarcoma has a similar natural disease history as its human counterpart. VSV-IFNβ-NIS was administered prior to standard of care surgical resection, permitting microscopic and genomic analysis of tumors. Treatment was well-tolerated and a “tail” of long-term survivors (∼35%) was apparent in the VSV-treated group, a greater proportion than observed in two contemporary control cohorts. An increase in tumor inflammation was observed in VSV-treated tumors and RNA-seq analysis showed that all the long-term responders had increased expression of a T cell anchored immune gene cluster. We conclude that neoadjuvant VSV-IFNβ-NIS is safe and may increase long-term survivorship in dogs with naturally occurring osteosarcoma, particularly those that exhibit pre-existing antitumor immunity.

Published

2023

2. Polycytidine tract deletion from microRNA-detargeted oncolytic Mengovirus optimizes the therapeutic index in a murine multiple myeloma model

Author

Velia Penza, Justin W. Maroun, Rebecca A. Nace, Autumn J. Schulze, and Stephen J. Russell

Subjects

oncolytic virotherapy, oncolytic virus, picornavirus, Mengovirus, polyC tract, microRNA detargeting, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Mengovirus is an oncolytic picornavirus whose broad host range allows for testing in immunocompetent cancer models. Two pathogenicity-ablating approaches, polycytidine (polyC) tract truncation and microRNA (miRNA) targets insertion, eliminated the risk of encephalomyocarditis. To investigate whether a polyC truncated, miRNA-detargeted oncolytic Mengovirus might be boosted, we partially or fully rebuilt the polyC tract into the 5′ noncoding region (NCR) of polyC-deleted (MC0) oncolytic constructs (NC) carrying miRNA target (miRT) insertions to eliminate cardiac/muscular (miR-133b and miR-208a) and neuronal (miR-124) tropisms. PolyC-reconstituted viruses (MC24-NC and MC37-NC) replicated in vitro and showed the expected tropism restrictions, but reduced cytotoxicity and miRT deletions were frequently observed. In the MPC-11 immune competent mouse plasmacytoma model, both intratumoral and systemic administration of MC0-NC led to faster tumor responses than MC24-NC or MC37-NC, with combined durable complete response rates of 75%, 0.5%, and 30%, respectively. Secondary viremia was higher following MC0-NC versus MC24-NC or MC37-NC therapy. Sequence analysis of virus progeny from treated mice revealed a high prevalence of miRT sequences loss among MC24- and MC37- viral genomes, but not in MC0-NC. Overall, MC0-NC was capable of stably retaining miRT sites and provided a more effective treatment and is therefore our lead Mengovirus candidate for clinical translation.

Published

2023

3. MicroRNA-detargeting proves more effective than leader gene deletion for improving safety of oncolytic Mengovirus in a nude mouse model

Author

Yogesh R. Suryawanshi, Rebecca A. Nace, Stephen J. Russell, and Autumn J. Schulze

Subjects

microRNA, leader protein, oncolytic virus, Mengovirus, glioblastoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

A dual microRNA-detargeted oncolytic Mengovirus, vMC24NC, proved highly effective against a murine plasmacytoma in an immunocompetent syngeneic mouse model; however, there remains the concern of escape mutant development and the potential for toxicity in severely immunocompromised cancer patients when it is used as an oncolytic virus. Therefore, we sought to compare the safety and efficacy profiles of an attenuated Mengovirus containing a virulence gene deletion versus vMC24NC in an immunodeficient xenograft mouse model of human glioblastoma. A Mengovirus construct, vMC24ΔL, wherein the gene coding for the leader protein, a virulence factor, was deleted, was used for comparison. The vMC24ΔL induced significant levels of toxicity following treatment of subcutaneous human glioblastoma (U87-MG) xenografts as well as when injected intracranially in athymic nude mice, reducing the overall survival. The in vivo toxicity of vMC24ΔL was associated with viral replication in nervous and cardiac tissue. In contrast, microRNA-detargeted vMC24NC demonstrated excellent efficacy against U87-MG subcutaneous xenografts and improved overall survival significantly compared to that of control mice without toxicity. These results reinforce microRNA-detargeting as an effective strategy for ameliorating unwanted toxicities of oncolytic picornaviruses and substantiate vMC24NC as an ideal candidate for clinical development against certain cancers in both immunocompetent and immunodeficient hosts.

Published

2021

4. A brief review of reporter gene imaging in oncolytic virotherapy and gene therapy

Author

Susanna C. Concilio, Stephen J. Russell, and Kah-Whye Peng

Subjects

bioluminescence, Cerenkov luminescence, fluorescence, gene therapy, molecular imaging, magnetic resonance imaging, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Reporter gene imaging (RGI) can accelerate development timelines for gene and viral therapies by facilitating rapid and noninvasive in vivo studies to determine the biodistribution, magnitude, and durability of viral gene expression and/or virus infection. Functional molecular imaging systems used for this purpose can be divided broadly into deep-tissue and optical modalities. Deep-tissue modalities, which can be used in animals of any size as well as in human subjects, encompass single photon emission computed tomography (SPECT), positron emission tomography (PET), and functional/molecular magnetic resonance imaging (f/mMRI). Optical modalities encompass fluorescence, bioluminescence, Cerenkov luminescence, and photoacoustic imaging and are suitable only for small animal imaging. Here we discuss the mechanisms of action and relative merits of currently available reporter gene systems, highlighting the strengths and weaknesses of deep tissue versus optical imaging systems and the hardware/reagents that are used for data capture and processing. In light of recent technological advances, falling costs of imaging instruments, better availability of novel radioactive and optical tracers, and a growing realization that RGI can give invaluable insights across the entire in vivo translational spectrum, the approach is becoming increasingly essential to facilitate the competitive development of new virus- and gene-based drugs.

Published

2021

5. Collateral Lethal Effects of Complementary Oncolytic Viruses

Author

Justin W. Maroun, Velia Penza, Taylor M. Weiskittel, Autumn J. Schulze, and Stephen J. Russell

Subjects

Oncolytic virus, Vaccinia virus, Vesicular Stomatitis virus, Mengovirus, Antiviral Immunity, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Virus-infected cells release type 1 interferons, which induce an antiviral state in neighboring cells. Naturally occurring viruses are therefore equipped with stealth replication strategies to limit virus sensing and/or with combat strategies to prevent or reverse the antiviral state. Here we show that oncolytic viruses with simple RNA genomes whose spread was suppressed in tumor cells pretreated with interferon were able to replicate efficiently when the cells were coinfected with a poxvirus known to encode a diversity of innate immune combat proteins. In vivo the poxvirus was shown to reverse the intratumoral antiviral state, rescuing RNA virus replication in an otherwise restrictive syngeneic mouse tumor model leading to antitumor efficacy. Pairing of complementary oncolytic viruses is a promising strategy to enhance the antitumor activity of this novel class of anticancer drugs.

Published

2020

6. Oncolytic Virus with Attributes of Vesicular Stomatitis Virus and Measles Virus in Hepatobiliary and Pancreatic Cancers

Author

Bolni Marius Nagalo, Camilo Ayala Breton, Yumei Zhou, Mansi Arora, James M. Bogenberger, Oumar Barro, Michael B. Steele, Nathan J. Jenks, Alexander T. Baker, Dan G. Duda, Lewis Rowland Roberts, Stephen J. Russell, Kah Whye Peng, and Mitesh J. Borad

Subjects

hepatobiliary cancer, measles virus, oncolytic viral therapy, pancreatic cancer, vesicular stomatitis virus, hepatocellular carcinoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Recombinant vesicular stomatitis virus (VSV)-fusion and hemagglutinin (FH) was developed by substituting the promiscuous VSV-G glycoprotein (G) gene in the backbone of VSV with genes encoding for the measles virus envelope proteins F and H. Hybrid VSV-FH exhibited a multifaceted mechanism of cancer-cell killing and improved neurotolerability over parental VSV in preclinical studies. In this study, we evaluated VSV-FH in vitro and in vivo in models of hepatobiliary and pancreatic cancers. Our results indicate that high intrahepatic doses of VSV-FH did not result in any significant toxicity and were well tolerated by transgenic mice expressing the measles virus receptor CD46. Furthermore, a single intratumoral treatment with VSV-FH yielded improved survival and complete tumor regressions in a proportion of mice in the Hep3B hepatocellular carcinoma model but not in mice xenografted with BxPC-3 pancreatic cancer cells. Our preliminary findings indicate that VSV-FH can induce potent oncolysis in hepatocellular and pancreatic cancer cell lines with concordant results in vivo in hepatocellular cancer and discordant in pancreatic cancer without the VSV-mediated toxic effects previously observed in laboratory animals. Further study of VSV-FH as an oncolytic virotherapy is warranted in hepatocellular carcinoma and pancreatic cancer to understand broader applicability and mechanisms of sensitivity and resistance.

Published

2020

7. Oncolytic Activity of Targeted Picornaviruses Formulated as Synthetic Infectious RNA

Author

Noura B. Elsedawy, Rebecca A. Nace, Stephen J. Russell, and Autumn J. Schulze

Subjects

Oncolytic, Virotherapy, Virus, Coxsackievirus A21, Picornavirus, MicroRNA, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Infectious nucleic acid has been proposed as a superior formulation for oncolytic virus therapy. Oncolytic picornaviruses can be formulated as infectious RNA (iRNA), and their unwanted tropisms eliminated by microRNA (miRNA) detargeting. However, genomic insertion of miRNA target sequences into coxsackievirus A21 (CVA21) iRNA compromised its specific infectivity, negating further development as a novel oncolytic virus formulation. To address this limitation, we substituted a muscle-specific miRNA response element for the spacer region downstream of the internal ribosomal entry site in the 5′ non-coding region of CVA21 iRNA, thereby preserving genome length while avoiding the disruption of known surrounding RNA structural elements. This new iRNA (R-CVA21) retained high specific infectivity, rapidly generating replicating miRNA-detargeted viruses following transfection in H1-HeLa cells. Further, in contrast with alternatively configured iRNAs that were tested in parallel, intratumoral administration of R-CVA21 generated a spreading oncolytic infection that was curative in treated animals without associated myotoxicity. Moreover, R-CVA21 also exhibited superior miRNA response element stability in vivo. This novel formulation is a promising agent for clinical translation.

Published

2020

8. Generation of a Tumor-Specific Chemokine Gradient Using Oncolytic Vesicular Stomatitis Virus Encoding CXCL9

Author

Elizabeth C. Eckert, Rebecca A. Nace, Jason M. Tonne, Laura Evgin, Richard G. Vile, and Stephen J. Russell

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Genetically modified vesicular stomatitis virus (VSV) is an attractive agent for cancer treatment due to rapid intratumoral replication and observed clinical responses. Although VSV selectively kills malignant cells and can boost antitumor immunity, limited induction of intratumoral immune infiltration remains a barrier to efficacy in some cancer models. Here we engineered the oncolytic VSV platform to encode the T cell chemokine CXCL9, which is known to mediate the recruitment of activated CD8+ cytotoxic T cells and CD4+ T helper cells, and demonstrates conserved protein function between mice and humans. Chemotactic activity of the virally encoded chemokine was confirmed in vitro. Intratumoral concentration of CXCL9 was shown to increase after VSV therapy in three different cancer models, but to a much greater degree after VSV-CXCL9 therapy as compared with VSV control viruses. Despite a steep chemokine gradient from the tumor to the bloodstream, tumor trafficking of adoptively transferred and endogenous T cells was not measurably increased following VSV-CXCL9 therapy. Our results indicate that oncolytic VSV infection promotes release of CXCL9 in the tumor microenvironment, but further boosting of the functional chemokine gradient through virus engineering has little incremental impact on intratumoral immune cell infiltration in mouse and human tumor models. Keywords: oncolytic virotherapy, vesicular stomatitis virus, chemokine, chemokine gradient, CXCL9

Published

2020

9. Dual-Isotope SPECT Imaging with NIS Reporter Gene and Duramycin to Visualize Tumor Susceptibility to Oncolytic Virus Infection

Author

Lianwen Zhang, Lukkana Suksanpaisan, Huailei Jiang, Timothy R. DeGrado, Stephen J. Russell, Ming Zhao, and Kah-Whye Peng

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Noninvasive dual-imaging methods that provide an early readout on tumor permissiveness to virus infection and tumor cell death could be valuable in optimizing development of oncolytic virotherapies. Here, we have used the sodium iodide symporter (NIS) and 125I radiotracer to detect infection and replicative spread of an oncolytic vesicular stomatitis virus (VSV) in VSV-susceptible (MPC-11 tumor) versus VSV-resistant (CT26 tumor) tumors in BALB/c mice. In conjunction, tumor cell death was imaged simultaneously using technetium (99mTc)-duramycin that binds phosphatidylethanolamine in apoptotic and necrotic cells. Dual-isotope single-photon emission computed tomography/computed tomography (SPECT/CT) imaging showed areas of virus infection (NIS and 125I), which overlapped well with areas of tumor cell death (99mTc-duramycin imaging) in susceptible tumors. Multiple infectious foci arose early in MPC-11 tumors, which rapidly expanded throughout the tumor parenchyma over time. There was a dose-dependent increase in numbers of infectious centers and 99mTc-duramycin-positive areas with viral dose. In contrast, NIS or duramycin signals were minimal in VSV-resistant CT26 tumors. Combinatorial use of NIS and 99mTc-duramycin SPECT imaging for simultaneous monitoring of oncolytic virotherapy (OV) spread and the presence or absence of treatment-associated cell death could be useful to guide development of combination treatment strategies to enhance therapeutic outcome.

Published

2019

10. Impact of acquired del(17p) in multiple myeloma

Author

Arjun Lakshman, Utkarsh Painuly, S. Vincent Rajkumar, Rhett P. Ketterling, Prashant Kapoor, Patricia T. Greipp, Angela Dispenzieri, Morie A. Gertz, Francis K. Buadi, Martha Q. Lacy, David Dingli, Amie L. Fonder, Suzanne R. Hayman, Miriam A. Hobbs, Wilson I. Gonsalves, Yi Lisa Hwa, Nelson Leung, Ronald S. Go, Yi Lin, Taxiarchis V. Kourelis, Rahma Warsame, John A. Lust, Stephen J. Russell, Steven R. Zeldenrust, Robert A. Kyle, and Shaji K. Kumar

Subjects

Specialties of internal medicine, RC581-951

Abstract

Abstract: The high-risk abnormality del(17p) can be detected by fluorescence in situ hybridization on malignant plasma cells (PCs) and has an adverse prognostic impact in patients with multiple myeloma (MM). Patients with del(17p) have reduced overall survival (OS). Patients who acquire del(17p) later during the disease course are not well described. The disease characteristics at diagnosis predicting for acquired del(17p) and its overall impact on patient survival is not known. We compared 76 patients with MM who were negative for del(17p) at diagnosis and acquired it later with 152 control MM patients who did not acquire del(17p) at a comparable time point. Patients acquired del(17p) at a median of 35.6 months (range, 4.6-116.1 months) from diagnosis of MM after a median of 2 lines of therapy (range, 1-10 lines of therapy). When compared with controls, patients with acquired del(17p) had shorter median progression-free survival (PFS) (30.1 vs 23.0 months; P = .032) and OS (106.1 vs 68.2 months; P < .001) from diagnosis. After the detection of del(17p), the median PFS was 5.4 months and the median OS was 18.1 months. High lactate dehydrogenase level (odds ratio [OR], 3.69; 95% confidence interval [CI], 1.11-12.24) and presence of t(4;14) (OR, 2.66; 95% CI, 1.09-6.48) or any high-risk translocation (OR, 2.23; 95% CI, 1.00-4.95) at diagnosis predicted acquisition of del(17p). High PC proliferative rate predicted shorter OS from detection of del(17p) (hazard ratio, 2.28; 95% CI, 1.31-3.96; P = .004). Our study shows that acquisition of del(17p) is an important molecular event associated with reduction in OS in MM. Certain baseline factors may predict acquisition of del(17p). This needs validation in prospective data sets.

Published

2019

11. Serotypic evolution of measles virus is constrained by multiple co-dominant B cell epitopes on its surface glycoproteins

Author

Miguel Ángel Muñoz-Alía, Rebecca A. Nace, Lianwen Zhang, and Stephen J. Russell

Subjects

antigenic evolution, antibody escape, measles virus hemagglutinin, measles virus fusion, Medicine (General), R5-920

Abstract

Summary: After centuries of pestilence and decades of global vaccination, measles virus (MeV) genotypes capable of evading vaccine-induced immunity have not emerged. Here, by systematically building mutations into the hemagglutinin (H) glycoprotein of an attenuated measles virus strain and assaying for serum neutralization, we show that virus evolution is severely constrained by the existence of numerous co-dominant H glycoprotein antigenic sites, some critical for binding to the pathogenicity receptors SLAMF1 and nectin-4. We further demonstrate the existence in serum of protective neutralizing antibodies targeting co-dominant fusion (F) glycoprotein epitopes. Lack of a substantial reduction in serum neutralization of mutant measles viruses that retain even one of the co-dominant antigenic sites makes evolution of pathogenic measles viruses capable of escaping serum neutralization in vaccinated individuals extremely unlikely.

Published

2021

12. Preclinical Development of Oncolytic Immunovirotherapy for Treatment of HPVPOS Cancers

Author

Lukkana Suksanpaisan, Rong Xu, Mulu Z. Tesfay, Carolyn Bomidi, Stefan Hamm, Rianna Vandergaast, Nathan Jenks, Michael B. Steele, Ayuko Ota-Setlik, Hinna Akhtar, Amara Luckay, Rebecca Nowak, Kah Whye Peng, John H. Eldridge, David K. Clarke, Stephen J. Russell, and Rosa Maria Diaz

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Immunotherapy for HPVPOS malignancies is attractive because well-defined, viral, non-self tumor antigens exist as targets. Several approaches to vaccinate therapeutically against HPV E6 and E7 antigens have been adopted, including viral platforms such as VSV. A major advantage of VSV expressing these antigens is that VSV also acts as an oncolytic virus, leading to direct tumor cell killing and induction of effective anti-E6 and anti-E7 T cell responses. We have also shown that addition of immune adjuvant genes, such as IFNβ, further enhances safety and/or efficacy of VSV-based oncolytic immunovirotherapies. However, multiple designs of the viral vector are possible—with respect to levels of immunogen expression and method of virus attenuation—and optimal designs have not previously been tested head-to-head. Here, we tested three different VSV engineered to express a non-oncogenic HPV16 E7/6 fusion protein for their immunotherapeutic and oncolytic properties. We assessed their profiles of efficacy and toxicity against HPVPOS and HPVNEG murine tumor models and determined the optimal route of administration. Our data show that VSV is an excellent platform for the oncolytic immunovirotherapy of tumors expressing HPV target antigens, combining a balance of efficacy and safety suitable for evaluation in a first-in-human clinical trial. Keywords: VSV immunovirotherapy, HPV positive cancer, preclinical

Published

2018

13. Coalescence efficiency of surface modified PBT meltblown nonwovens in the separation of water from diesel fuel containing surfactants

Author

Hamidreza Arouni, Umer Farooq, Parikshit Goswami, Nikil Kapur, and Stephen J. Russell

Subjects

Technology

Abstract

Removal of water from diesel fuel is essential to ensure efficient operation of High-Pressure Common-Rail (HPCR) fuel injection systems used in modern diesel engines. The presence of surfactants in modern fuels (including biofuels) can create conditions in which the interfacial tension between water and fuel is reduced, leading to coalescing media being “disarmed” and less effective in separation. To elucidate this phenomenon in industrially available depth coalescing media, the coalescence efficiency of surface-modified poly (butylene terephthalate) (PBT) meltblown nonwoven fabrics possessing a wide range of wetting behaviours was studied. Tuning of the wettability was accomplished by alkaline hydrolysis of the medium. Using reference grade diesel fuel with and without added surfactants, the coalescence efficiency and quality factor were studied by means of a purpose-built coalescence test rig. The coalescence efficiency was found to depend on both the fuel composition and the wettability of the treated PBT and the optimum efficiency for each test fuel required a difference in wettability of the PBT. For reference grade diesel, increasing the wettability to ‘intermediate’ level improved coalescence efficiency, but the quality factor can be negatively affected by water droplet retention within the medium. The reduced quality factor associated with hydrophilic media was even more pronounced in fuels containing surfactants due to increased pressure drop and re-emulsification of the fuel in water. These findings highlight the practical challenges that exist in engineering a “universal” coalescing medium suitable for removing water from diesel fuels containing surfactants, based solely on the modulation of fibre wettability and hydrophilicity. Keywords: Coalescence, Filter media, Diesel fuel, Fuel surfactant, Water separation, Wettability

Published

2019

14. Dexamethasone-Induced Oxidative Stress Enhances Myeloma Cell Radiosensitization While Sparing Normal Bone Marrow Hematopoiesis

Author

Soumen Bera, Suzanne Greiner, Amit Choudhury, Angela Dispenzieri, Douglas R. Spitz, Stephen J. Russell, and Apollina Goel

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Dexamethasone (Dex) and radiation therapy are established modalities in multiple myeloma. In this study, we propose a novel combination of Dex plus radiation that shows superior clonogenic cell killing and apoptosis of myeloma cells and selectively eliminates myeloma cells when cocultured with bone marrow stromal cells (BMSCs). Dex was found to inhibit the release of interleukin-6 from irradiated BMSCs, which is an established myeloma cell proproliferative cytokine. In 5TGM1 model, the combination of Dex with skeletal targeted radiotherapy (153-Sm-EDTMP) prolonged median survival time and inhibited radiation-induced myelosuppression. A two-cycle treatment of Dex plus 153-Sm-EDTMP was well tolerated and further improved median survival time. Mechanistically, Dex increased superoxide and hydrogen peroxide production and augmented radiation-induced oxidative stress and cell death of myeloma cells. In contrast, Dex inhibited radiation-induced increase in pro-oxidant levels and enhanced the clonogenic survival in normal hematopoietic stem and progenitor cells. Treatment with either N-acetylcysteine or the combination of polyethylene glycol (PEG)-conjugated copper, zinc-superoxide dismutase, and PEG-catalase significantly protected myeloma cells from Dex-induced clonogenic death. Overall, these results demonstrate that Dex in combination with radiotherapy enhances the killing of myeloma cells while protecting normal bone marrow hematopoiesis through a mechanism that involves selective increases in oxidative stress.

Published

2010

15. A brief review of reporter gene imaging in oncolytic virotherapy and gene therapy

Author

Kah Whye Peng, Susanna C. Concilio, and Stephen J. Russell

Subjects

0301 basic medicine, Cancer Research, Biodistribution, positron emission tomography, viral vectors, Computer science, Computational biology, Review, Single-photon emission computed tomography, Viral vector, single photon emission computed tomography, 03 medical and health sciences, optical imaging, 0302 clinical medicine, medicine, magnetic resonance imaging, Pharmacology (medical), Cerenkov luminescence, oncolytic virotherapy, RC254-282, nuclear imaging, Reporter gene, medicine.diagnostic_test, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Magnetic resonance imaging, molecular imaging, bioluminescence, gene therapy, Oncolytic virus, 030104 developmental biology, PET, Oncology, Positron emission tomography, 030220 oncology & carcinogenesis, SPECT, Molecular Medicine, photoacoustic imaging, reporter gene imaging, fluorescence, Molecular imaging, MRI

Abstract

Reporter gene imaging (RGI) can accelerate development timelines for gene and viral therapies by facilitating rapid and noninvasive in vivo studies to determine the biodistribution, magnitude, and durability of viral gene expression and/or virus infection. Functional molecular imaging systems used for this purpose can be divided broadly into deep-tissue and optical modalities. Deep-tissue modalities, which can be used in animals of any size as well as in human subjects, encompass single photon emission computed tomography (SPECT), positron emission tomography (PET), and functional/molecular magnetic resonance imaging (f/mMRI). Optical modalities encompass fluorescence, bioluminescence, Cerenkov luminescence, and photoacoustic imaging and are suitable only for small animal imaging. Here we discuss the mechanisms of action and relative merits of currently available reporter gene systems, highlighting the strengths and weaknesses of deep tissue versus optical imaging systems and the hardware/reagents that are used for data capture and processing. In light of recent technological advances, falling costs of imaging instruments, better availability of novel radioactive and optical tracers, and a growing realization that RGI can give invaluable insights across the entire in vivo translational spectrum, the approach is becoming increasingly essential to facilitate the competitive development of new virus- and gene-based drugs., Graphical abstract, Reporter gene imaging can accelerate the clinical translation and development of oncolytic virotherapy and gene therapy vectors. Here we review common reporter genes for radionuclide, magnetic resonance, and optical imaging modalities. We highlight the elegance of the sodium iodide symporter (NIS) that is amenable to SPECT or PET imaging in mice, large animals, and humans.

Published

2021

16. Coalescence efficiency of surface modified PBT meltblown nonwovens in the separation of water from diesel fuel containing surfactants

Author

Stephen J. Russell, Hamidreza Arouni, Umer Farooq, Nikil Kapur, and Parikshit Goswami

Subjects

Surface tension, Pressure drop, Coalescence (physics), Diesel fuel, Materials science, Chemical engineering, Biofuel, lcsh:T, General Engineering, Wetting, Fuel injection, Alkaline hydrolysis, lcsh:Technology

Abstract

Removal of water from diesel fuel is essential to ensure efficient operation of High-Pressure Common-Rail (HPCR) fuel injection systems used in modern diesel engines. The presence of surfactants in modern fuels (including biofuels) can create conditions in which the interfacial tension between water and fuel is reduced, leading to coalescing media being “disarmed” and less effective in separation. To elucidate this phenomenon in industrially available depth coalescing media, the coalescence efficiency of surface-modified poly (butylene terephthalate) (PBT) meltblown nonwoven fabrics possessing a wide range of wetting behaviours was studied. Tuning of the wettability was accomplished by alkaline hydrolysis of the medium. Using reference grade diesel fuel with and without added surfactants, the coalescence efficiency and quality factor were studied by means of a purpose-built coalescence test rig. The coalescence efficiency was found to depend on both the fuel composition and the wettability of the treated PBT and the optimum efficiency for each test fuel required a difference in wettability of the PBT. For reference grade diesel, increasing the wettability to ‘intermediate’ level improved coalescence efficiency, but the quality factor can be negatively affected by water droplet retention within the medium. The reduced quality factor associated with hydrophilic media was even more pronounced in fuels containing surfactants due to increased pressure drop and re-emulsification of the fuel in water. These findings highlight the practical challenges that exist in engineering a “universal” coalescing medium suitable for removing water from diesel fuels containing surfactants, based solely on the modulation of fibre wettability and hydrophilicity. Keywords: Coalescence, Filter media, Diesel fuel, Fuel surfactant, Water separation, Wettability

Published

2019

17. In-situ crosslinked wet spun collagen triple helices with nanoscale-regulated ciprofloxacin release capability

Author

David Wood, M. Tarik Arafat, Giuseppe Tronci, and Stephen J. Russell

Subjects

Materials science, Stacking, Young's modulus, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, symbols.namesake, Ultimate tensile strength, General Materials Science, Spinning, Mechanical Engineering, technology, industry, and agriculture, Biomolecules (q-bio.BM), 021001 nanoscience & nanotechnology, Condensed Matter Physics, Controlled release, 0104 chemical sciences, Quantitative Biology - Biomolecules, Chemical engineering, Mechanics of Materials, Covalent bond, FOS: Biological sciences, symbols, Elongation, 0210 nano-technology, Triple helix

Abstract

The design of antibacterial-releasing coatings or wrapping materials with controlled drug release capability is a promising strategy to minimise risks of infection and medical device failure in vivo. Collagen fibres have been employed as medical device building block, although they still fail to display controlled release capability, competitive wet-state mechanical properties, and retained triple helix organisation. We investigated this challenge by pursuing a multiscale design approach integrating drug encapsulation, in-situ covalent crosslinking and fibre spinning. By selecting ciprofloxacin (Cip) as a typical antibacterial drug, wet spinning was selected as a triple helix-friendly route towards Cip-encapsulated collagen fibres; whilst in-situ crosslinking of fibre-forming triple helices with 1,3-phenylenediacetic acid (Ph) was hypothesised to yield Ph-Cip π-π stacking aromatic interactions and enable controlled drug release. Higher tensile modulus and strength were measured in Ph-crosslinked fibres compared to state-of-the-art carbodiimide-crosslinked controls. Cip-encapsulated Ph-crosslinked fibres revealed decreased elongation at break and significantly-enhanced drug retention in vitro with respect to Cip-free variants and carbodiimide-crosslinked controls, respectively. This multiscale manufacturing strategy provides new insight aiming at wet spun collagen triple helices with nanoscale-regulated tensile properties and drug release capability.

Published

2019

18. Enrichment of cellulose acetate nanofibre assemblies for therapeutic delivery of L-tryptophan

Author

Parikshit Goswami, Stephen J. Russell, Richard S. Blackburn, and Behrouz Ghorani

Subjects

Diffusion, Nanofibers, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Biochemistry, chemistry.chemical_compound, Reaction rate constant, Electricity, Structural Biology, Desorption, Polymer chemistry, Acetone, Nanotechnology, QD, Cellulose, Molecular Biology, Drug Carriers, Tryptophan, General Medicine, 021001 nanoscience & nanotechnology, Cellulose acetate, Electrospinning, 0104 chemical sciences, Kinetics, chemistry, Chemical engineering, Methanol, 0210 nano-technology

Abstract

The essential amino acid L-tryptophan is naturally present in the body, and is also available as a water soluble dietary supplement. The feasibility of preparing enriched cellulose acetate (CA)-based fibres as a vehicle for therapeutic delivery of such biomolecules was investigated. A new ternary solvent system consisting of acetone: N,N-dimethylacetamide: methanol (2:1:2) has been demonstrated to permit the solution blending of CA with the water soluble L-tryptophan. Nanofibrous webs substantially free of structural defects were continuously produced with mean fibre diameters in the range of 520-1,010nm, dependent on process parameters. Morphology and diameter of fibres were influenced by concentration of CA spinning solution, applied voltage and flow rates. The kinetic release profile of L-tryptophan from electrospun CA nanofibres was described by the pseudo-second order kinetic model. Fibres with mean diameter of 720 nm provide both the highest initial desorption rate and rate constant, which was partially attributed to the low fibre diameter and high relative surface area, but also the fact that the fibres with mean diameter of 720 nm produced were the most bead-free, providing diffusion advantages over the fibres with lowest mean diameter (520 nm). The feasibility of combining L-tryptophan within fibres provides a promising route for manufacture of transdermal delivery devices.

Published

2017

19. The charging and stability of electret filters

Author

Ali Kilic, Eunkyoung Shim, Stephen J. Russell, and Behnam Pourdeyhimi

Subjects

Pressure drop, Materials science, business.industry, Electrical engineering, Electret, Polarization (electrochemistry), business, Engineering physics, Particle capture

Abstract

Having a long history in aerosol filtration technologies, electret filters are one of the basic solutions to provide high particle capture efficiency at a low pressure drop and energy expense. However, their reliability is still an ongoing issue from the aspects of high efficiency and stability. In this chapter the theory behind electret mechanism, charging of the fibrous materials, their discharging and stability were reviewed in detail. Physics behind the widely used electret filter charging/polarization mechanisms were also discussed.

Published

2017

20. Technical fabric structures – 3. Nonwoven fabrics

Author

Stephen J. Russell and P.A. Smith

Subjects

Materials science, Polymer science, Composite material, Thermal bonding

Abstract

Nonwovens are structurally complex, engineered fabrics that are fundamental to the performance of products used in a diverse range of applications for many different markets. The structure and properties of nonwovens are heavily influenced by the way in which the fabrics are manufactured. The purpose of this section is to briefly review some of the key industrial processes.

Published

2016

21. Dexamethasone-Induced Oxidative Stress Enhances Myeloma Cell Radiosensitization While Sparing Normal Bone Marrow Hematopoiesis

Author

Amit Choudhury, Suzanne Greiner, Soumen Bera, Douglas R. Spitz, Stephen J. Russell, Angela Dispenzieri, and Apollina Goel

Subjects

Cancer Research, Stromal cell, medicine.medical_treatment, Biology, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, medicine, polycyclic compounds, Progenitor cell, Clonogenic assay, Multiple myeloma, 030304 developmental biology, 0303 health sciences, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 3. Good health, Haematopoiesis, medicine.anatomical_structure, Cytokine, Apoptosis, 030220 oncology & carcinogenesis, Immunology, Cancer research, Bone marrow, hormones, hormone substitutes, and hormone antagonists

Abstract

Dexamethasone (Dex) and radiation therapy are established modalities in multiple myeloma. In this study, we propose a novel combination of Dex plus radiation that shows superior clonogenic cell killing and apoptosis of myeloma cells and selectively eliminates myeloma cells when cocultured with bone marrow stromal cells (BMSCs). Dex was found to inhibit the release of interleukin-6 from irradiated BMSCs, which is an established myeloma cell proproliferative cytokine. In 5TGM1 model, the combination of Dex with skeletal targeted radiotherapy (153-Sm-EDTMP) prolonged median survival time and inhibited radiation-induced myelosuppression. A two-cycle treatment of Dex plus 153-Sm-EDTMP was well tolerated and further improved median survival time. Mechanistically, Dex increased superoxide and hydrogen peroxide production and augmented radiation-induced oxidative stress and cell death of myeloma cells. In contrast, Dex inhibited radiation-induced increase in pro-oxidant levels and enhanced the clonogenic survival in normal hematopoietic stem and progenitor cells. Treatment with either N-acetylcysteine or the combination of polyethylene glycol (PEG)-conjugated copper, zinc-superoxide dismutase, and PEG-catalase significantly protected myeloma cells from Dex-induced clonogenic death. Overall, these results demonstrate that Dex in combination with radiotherapy enhances the killing of myeloma cells while protecting normal bone marrow hematopoiesis through a mechanism that involves selective increases in oxidative stress.

Published

2010

22. Wet-spinnability and crosslinked fibre properties of two collagen polypeptides with varied molecular weight

Author

David J. Wood, M. Tarik Arafat, Giuseppe Tronci, Stephen J. Russell, Ramya Sri Kanuparti, and Jie Yin

Subjects

food.ingredient, Swine, FOS: Physical sciences, Biocompatible Materials, 02 engineering and technology, Condensed Matter - Soft Condensed Matter, 010402 general chemistry, 01 natural sciences, Gelatin, Biochemistry, Fibre, chemistry.chemical_compound, Hydrolysis, food, Structural Biology, Physics - Chemical Physics, Tensile Strength, Ultimate tensile strength, Materials Testing, Spectroscopy, Fourier Transform Infrared, Acetone, Animals, Molecular Biology, Chemical Physics (physics.chem-ph), Chemistry, Dimethyl sulfoxide, Viscosity, General Medicine, 021001 nanoscience & nanotechnology, Condensation reaction, Wet-spinning, Crosslink density, 0104 chemical sciences, Solvent, Molecular Weight, Chemical engineering, Covalent bond, Soft Condensed Matter (cond-mat.soft), Collagen, Polypeptide, 0210 nano-technology, Peptides

Abstract

The formation of naturally-derived materials with wet stable fibrous architectures is paramount in order to mimic the features of tissues at the molecular and microscopic scale. Here, we investigated the formation of wet-spun fibres based on collagen-derived polypeptides with comparable chemical composition and varied molecular weight. Gelatin and hydrolysed fish collagen (HFC) were selected as widely-available linear amino-acidic chains of high and low molecular weight, respectively, and functionalised in the wet-spun fibre state in order to preserve the material geometry in physiological conditions. Wet-spun fibre diameter and morphology were dramatically affected depending on the polypeptide molecular weight, wet-spinning solvent (i.e. 2,2,2-Trifluoroethanol and dimethyl sulfoxide) and coagulating medium (i.e. acetone and ethanol), resulting in either bulky or porous internal geometry. Dry-state tensile moduli were significantly enhanced in gelatin and HFC samples following covalent crosslinking with activated 1,3 phenylenediacetic acid (Ph) (E: 726 +/- 43 - 844 +/- 85 MPa), compared to samples crosslinked via intramolecular carbodiimide-mediated condensation reaction (E: 588 +/- 38 MPa). Resulting fibres displayed a dry diameter in the range of 238 +/- 18 - 355 +/- 28 micron and proved to be mechanically-stable (E: 230 kPa) following equilibration with PBS, whilst a nearly-complete degradation was observed after 5-day incubation in physiological conditions., Comment: 26 pages, 7 figures, 3 tables- accepted in 'International Journal of Biological Macromolecules'

Published

2015

23. LCA of wool textiles and clothing

Author

Stephen Wiedemann, Stephen J. Russell, Paul Swan, Barbara Nebel, Dave Maslen, Sebastian Gollnow, Beverley Henry, and Stewart Ledgard

Subjects

Engineering, Waste management, Product life-cycle management, business.industry, Wool, Natural resource economics, Resource use, Production (economics), Context (language use), Reuse, Clothing, business, Life-cycle assessment

Abstract

This chapter examines life cycle assessment (LCA) of wool textiles and clothing, focussing on the specific elements of the wool value chain where methodology and data significantly affect quantification of environmental impacts and resource use. Recent methodological developments, particularly for handling co-products from production on sheep farms, and emerging understanding of the benefits of reuse and recycling of wool clothing are discussed in the context of the diversity of production and use of wool. A case study for two merino products demonstrates the relative contributions of life cycle stages and identifies progress and remaining gaps in data and methodology, and future prospects for improved estimates of the environmental performance of wool products using LCA thinking.

Published

2015

24. Technical design for recycling of clothing

Author

Elaine R. Durham, Stephen J. Russell, Andrew D. Hewitt, and Robert Stuart Ellis Bell

Subjects

Engineering drawing, Garment design, Engineering, business.industry, Yarn, Reuse, Design for recycling, Clothing, Fabric structure, Technical design, Manufacturing engineering, Hardware_GENERAL, visual_art, Compatibility (mechanics), visual_art.visual_art_medium, business

Abstract

Clothing is rarely designed to aid recycling at the end of life. Design can influence both the active life of clothing and suitability for reuse or recycling when discarded by its user. This chapter discusses some important aspects of design for recycling, such as durability, homogeneity of composition, compatibility with industrial recycling processes, yarn and fabric structure, coatings and printed surfaces, adhesives and lamination, joint selection, disassembly time, and labeling. Small design modifications in clothing to facilitate automated disassembly are also considered for the removal of labels, logos, buttons, and zippers without damaging the surrounding fabric.

Published

2015

25. Oncolytic potency of HER-2 retargeted VSV-FH hybrid viruses: the role of receptor ligand affinity

Author

Stephen J. Russell, Duncan R. Smith, Nitwara Wikan, Kah Whye Peng, Camilo Breton, and Arinda Abbuhl

Subjects

Cancer Research, viruses, Hemagglutinin (influenza), Biology, lcsh:RC254-282, Article, Virus, Epitope, Measles virus, 03 medical and health sciences, 0302 clinical medicine, Potency, Pharmacology (medical), Tropism, 030304 developmental biology, 0303 health sciences, biology.organism_classification, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Virology, Molecular biology, 3. Good health, Oncolytic virus, Oncology, Vesicular stomatitis virus, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine

Abstract

The hybrid oncolytic vesicular stomatitis virus (VSV-FH) deleted for its G glycoprotein and displaying the measles virus (MV) envelope glycoproteins (hemagglutinin H and fusion F) is fusogenic, infects cells via any of the three MV receptors and has potent oncolytic activity against subcutaneous and disseminated myeloma tumors. To tailor VSV-FH as an oncolytic virus for ovarian cancer, we ablated its natural tropism and retargeted the virus by display of a single-chain antibody (scFv) with specificity to the HER-2/neu receptor. A panel of six VSVFH-αHER2 viruses displaying anti-HER2 scFv that bind to the same HER2 epitope but with different K d (10(-6) to 10(-11) M, VSVFH-αHER2#6 to #11, respectively) were rescued and characterized. A K d of at least 10(-8) M is required for infection of HER-2 positive SKOV3ip.1 cells. The higher affinity viruses (10(-8) M) were able to infect and fuse SKOV3ip.1 cells more efficiently, inducing more extensive cytopathic effects. We next compared the antitumor potency of the viruses against SKOV3ip.1 tumor xenografts. In contrast to the saline-treated animals, one intratumoral injection of VSVFH-αHER2#9, #10, or #11 resulted in efficient tumor control. There was no significant difference between viruses with an affinity higher than 10(-9) M in terms of oncolytic potency. VSVFH-αHER2 virus may be a promising agent for the treatment of HER-2 positive malignancies.

Published

2015

26. Fibre to Fabric

Author

Stephen J. Russell and Ningtao Mao

Subjects

Materials science, Nonwoven fabric, Composite material, Fabric structure

Abstract

This chapter gives an outline of some of the main fabric formation technologies in the nonwovens industry as well as aspects of fabric structure, properties and fabric characterisation. The basic influence of nonwoven fabric structure on properties is explained, as well as end-use applications and functional requirements.

Published

2015

27. Nonwoven scaffolds for bone regeneration

Author

Giuseppe Tronci, Stephen J. Russell, Elaine R. Durham, David J. Wood, and Xuebin Yang

Subjects

Engineering, Medical device, business.industry, 02 engineering and technology, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, Construction engineering, Load bearing, 0104 chemical sciences, Textile technology, 0210 nano-technology, Bone regeneration, business

Abstract

Recent concerns over the possible effects of metal-on-metal orthopaedic implants and the evolution of more natural structures made from fibre have made medical device manufacturers consider the potential of fibre. Textiles offer the potential to replace traditional materials with novel fibres which are more suitable for many load bearing applications. Orthopaedics, in particular, is embracing textile technology for repairing, replacing, and regenerating integral pieces of the skeletal system and its associated components. This important new book will provide readers with a comprehensive overview of the role biomedical textiles can play in the orthopaedic field. Chapters in part one will discuss the fundamentals of textiles for orthopaedic applications. Part two will cover textiles for implantable orthopaedic applications whilst the final set of chapters will discuss the role of textiles in orthopaedic tissue engineering. - Provides a comprehensive overview of the role biomedical textiles can play in the orthopaedic field.

Published

2015

28. Reporter gene imaging identifies intratumoral infection voids as a critical barrier to systemic oncolytic virus efficacy

Author

Lukkana Suksanpaisan, Amber Miller, Shruthi Naik, Rebecca A. Nace, Stephen J. Russell, Kah Whye Peng, and Mark J. Federspiel

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Reporter gene, Biology, biology.organism_classification, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, Virus, Article, 3. Good health, Oncolytic virus, Oncology, In vivo, Vesicular stomatitis virus, Symporter, Systemic administration, medicine, Molecular Medicine, Immunohistochemistry, Pharmacology (medical)

Abstract

Systemically administered oncolytic viruses have the ability to cause tumor destruction through the expansion and coalescence of intratumoral infectious centers. Efficacy is therefore dependent upon both the density and intratumoral distribution of virus-infected cells achieved after initial virus infusion, and delivery methods are being developed to enhance these critical parameters. However, the three-dimensional (3D) mapping of intratumoral infectious centers is difficult using conventional immunohistochemical methodology, requiring painstaking 3D reconstruction of numerous sequential stained tumor sections, with no ability to study the temporal evolution of spreading infection in a single animal. We therefore developed a system using very high-resolution noninvasive in vivo micro single-photon emitted computed tomography/computed tomography (microSPECT/CT) imaging to determine the intratumoral distribution of thyroid radiotracers in tumors infected with an oncolytic virus encoding the thyroidal sodium–iodide symporter (NIS). This imaging system was used for longitudinal analysis of the density, distribution, and evolution of intratumoral infectious centers after systemic administration of oncolytic vesicular stomatitis virus in tumor-bearing mice and revealed heterogeneous delivery of virus particles both within and between tumors in animals receiving identical therapy. This study provides compelling validation of high resolution in vivo reporter gene mapping as a convenient method for serial monitoring of intratumoral virus spread that will be necessary to address critical barriers to systemic oncolytic virus efficacy such as intratumoral delivery.

Published

2014

29. Modelling of nonwoven materials

Author

Stephen J. Russell and Ningtao Mao

Subjects

Materials science, Nonwoven fabric, Composite material, Porosity

Abstract

Nonwovens are porous fibre assemblies that are engineered to meet the technical requirements of numerous industrial, medical and consumer products. In this chapter, the properties of nonwoven fabrics that govern their suitability for use in various applications are briefly summarised, and examples of analytical and empirical models that link nonwoven fabric properties and structural parameters are given. The fabric structural parameters include fibre dimensions and properties, fibre alignment, the structural properties of the bond points, the pore structure and fabric porosity, and the fabric dimensions and variation.

Published

2010

30. GENE THERAPY

Author

Stephen J. Russell and Kah Whye Peng

Published

2009

31. CONTRIBUTORS

Author

Darrell R. Abernethy, Viola Andresen, Arthur J. Atkinson, Michel Azizi, Helen L. Baron, Carol L. Beck, Atta Behfar, Rodney Bell, Eduardo E. Benarroch, Neal L. Benowitz, Wade Berrettini, Joseph S. Bertino, Alfredo Bianchi, Michael J. Blake, Ann F. Bolger, Glenn D. Braunstein, David Brock, Peter A. Calabresi, Michael Camilleri, Mark Chaballa, Omer Chaudhry, Doo-Sup Choi, Bart L. Clarke, Mary E. Dankert, Dawood Darbar, Mark Davis, Daniel Deck, Jan de Gans, Joseph A. DeSimone, Robert B. Diasio, André Diedrich, Darin D. Dougherty, Laurence J. Egan, Claudine El-Beyrouty, Jean-Luc Elghozi, Arthur M. Feldman, Joanne Filicko-O'Hara, Charles W. Flexner, Neal Flomenberg, Joseph F. Foss, Adam M. Frank, Mark A. Frye, Kishor Gandhi, Joseph Genebriera, William R. Gilliland, Jean Gray, Benjamin M. Greenberg, Naomi Gronich, Dolores Grosso, Andrew R. Haas, Wael N. Haidar, Christine A. Haller, Daniel K. Hall-Flavin, Lisa Hamaker, William F. Harvey, James W. Heitz, Steven K. Herrine, Raymond J. Hohl, Sarah A. Holstein, Dorothy Holt, Linda S. Hostelley, Eric R. Houpt, Shiew-Mei Huang, David J. Hunter, Serge Jabbour, Robert M. Jacobson, Arshad Jahangir, Michael A. Jenike, Kristine E. Johnson, Victor M. Karpyak, Gregory L. Kearns, Richard M. Keating, Michael P. Keith, Sundeep Khosla, Julia Kirchheiner, Walter J. Koch, Bruce C. Kone, Walter K. Kraft, Robert F. Kushner, Christine Laine, Richard L. Lalonde, Kiwon Lee, Teofilo Lee-Chiong, Frank T. Leone, Lawrence J. Lesko, Barbara A. Levey, Lionel D. Lewis, Joseph Loscalzo, Anastasios Lymperopoulos, Joseph P. Lynch, Christian Maaser, Viqar Maria, Paul E. Marik, Marco A. Maurtua, Steven E. McKenzie, Alex Mejia, Michael C. Milone, Scott Mintzer, Thomas P. Moyer, David A. Mrazek, Matthew S. Murphy, Filip Mussen, Jasmine Nabi, Victor J. Navarro, Timothy J. Nelson, Dionissios Neofytos, Kathleen A. Neville, Myaing Nyunt, Timothy O'Brien, Inna G. Ovsyannikova, Chi-Un Pae, James F. Pagel, Ashwin A. Patkar, Kah Whye Peng, Edith A. Perez, Ronald C. Petersen, Paul A. Pham, Jennifer M. Phillips, Carissa Pineda, Mark R. Pittelkow, Pierre-François Plouin, Christopher V. Plowe, Gregory A. Poland, Azad Raiesdana, John N. Ratchford, Nandi J. Reddy, Michael D. Reed, Douglas J. Rhee, Robert A. Rizza, David Robertson, Dan M. Roden, Anne M. Rompalo, Simona Rossi, Vivek Roy, Stephen J. Russell, Steven Ryder, Muhammad Wasif Saif, Rajiv Saini, Kyoko Sato, Kathryn M. Schak, Matthias Schwab, Kumar Sharma, Robert G. Sharrar, Leslie M. Shaw, Ludy Shih, Steven J. Siegel, Peter A. Singer, David R. Staskin, Dale W. Stovall, Jerome F. Strauss, Paul V. Targonski, Daniel Tarsy, William S. Tasman, Robert Temple, Andre Terzic, John E. Tetzlaff, Pritish K. Tosh, Erev E. Tubb, Kathleen Uhl, Patrick Vallance, Diederik van de Beek, Adrian Vella, Eugene R. Viscusi, John L. Wagner, Scott A. Waldman, Philip B. Wedegaertner, Alan J. Wein, Ethan Weiner, Richard Weinshilboum, Martijn Weisfelt, Lisa G. Winston, Run Yu, and Ying Zhang

Published

2009

32. Nonwovens used in automobiles

Author

Matthew James Tipper and Stephen J. Russell

Subjects

Engineering, Polymer composition, business.industry, Automotive industry, Mechanical engineering, Structural engineering, Technical design, law.invention, law, In vehicle, Current (fluid), business, Vehicle type, Acoustic insulation, Filtration

Abstract

Nonwoven fabrics are essential components in modern vehicles with over forty areas of application depending on the vehicle type and technical design specifications. An overview of the main uses and functions of nonwoven fabrics in vehicle interiors, filtration and acoustic insulation is provided with reference to polymer composition and fabric construction. Current and future requirements for nonwoven automotive fabrics are summarised including the need for recyclability at the end of life.

Published

2008

33. REPAIR OF ARTICULAR CARTILAGE DEFECTS USING 3-DIMENSIONAL TISSUE ENGINEERING TEXTILE ARCHITECTURES

Author

Richard J. Bibb, P. Moliter, S. Young, R.J. Minns, and Stephen J. Russell

Subjects

Textile, Materials science, Repair tissue, Tissue engineering, Orientation (computer vision), business.industry, Full thickness, Articular cartilage, Biological tissue, business, Joint (geology), Biomedical engineering

Abstract

The successful repair of articular cartilage must rely on the restoration of the full thickness of the layer with full structural integration laterally with the existing material on the joint surface. The knee is the most commonly affected joint for cartilage degeneration and it is this joint that will be used as the basis for our investigations. Previously, textile mesh structures (based on intermeshed yarns) have been designed and used to provide an oriented repair of biological tissue in the body e.g. the repair of hernia in men. The repair of articular cartilage defects in lesions of the knee has also been described using a nonwoven structure with random fibre orientation into which repair tissue grows to provide a load-bearing surface. It is proposed that shape data (using the selection criteria of cartilage thickness 1 mm and associated underlying bony changes) is generated in 3D space by imaging methods, and used together with structural information from the current knowledge base arising from previous studies and published material. This will allow a computer model of the architecture to be constructed. The “male’ form of the shape data will be used to design and manufacture textile engineered implants. It is envisaged that the ‘female’ shape around the lesion could be used as a surgical positioning tool to cut out (If necessary) the desired shape of the lesion to seat the final implant material. It is anticipated that a textile implant of pre-defined structure will be in a rigid or semi-rigid form, with the ‘zonal’ information relating to the structural architecture of the lesion built-in. In any generic class of textile material, including nonwovens, there is no single form of 3D structural architecture and this can be manipulated during manufacture. This has been overlooked in other studies using textile scaffolds. The fibre orientation, the porosity and the physical properties of the structure may be adjusted within wide limits. Different generic textile structures containing yarns, mechanically entangled fibres, films and membranes can also be combined depending on the required functionality of the material. Using the shape and thickness data obtained from imaging, it is proposed to design and evaluate textile structures of selected physical and mechanical properties that would reproduce a repair of similar structural design to the original articular cartilage at that site.

Published

2006

34. NONWOVEN SCAFFOLDS OF IMPROVED DESIGN FOR THE TISSUE ENGINEERING OF THE ANTERIOR CRUCIATE LIGAMENT

Author

Sharon Lee Edwards, J.B. Matthews, Stephen J. Russell, W. Mitchell, and Eileen Ingham

Subjects

Extracellular matrix, Scaffold, Materials science, medicine.anatomical_structure, Tissue engineering, Biocompatibility, Anterior cruciate ligament, medicine, Tissue formation, Biomedical engineering, Structural factor

Abstract

This work is concerned with improving nonwoven scaffold design for the tissue engineering of the anterior cruciate ligament. When designing a scaffold two important design criteria to consider are scaffold's internal structure and biocompatibility, both of which are addressed in this paper. The role of a scaffold is to provide a framework for cells to attach, proliferate and secrete extra cellular matrix. The scaffold also acts as a template, directing the growth of cells and newly formed tissue. It is the scaffold's internal structure, together with polymer surface chemistry and morphology, which directly influence the cellular activities that lead to tissue formation. With regard to scaffold's internal structure, structural parameters are discussed in relation to specific scaffold function; for example the effect of scaffold pore-size on cell proliferation, migration and nutrient supply. Another structural factor discussed is the role of fibre orientation as a means of guiding and organising new tissue growth. With the aim of creating a scaffold of optimum design, for the tissue engineering of the anterior cruciate ligament, nonwoven scaffolds of differing structure have been constructed. In order to understand the relationship between manufacturing method and scaffold structure characterisation techniques have been employed to analyse the structural parameters of these scaffolds. Obtained scaffold structural properties are discussed in relation to manufacturing method. Regarding the second scaffold criteria biocompatibility tests have been conducted by the authors on a range of generic fibre types. The results of these tests are provided in the form of cell attachment, with reference to fibre morphology.

Published

2006

35. Anisotropic Fluid Transmission in Nonwoven Wound Dressings

Author

Stephen J. Russell and Ningtao Mao

Subjects

Transmission properties, Orientation function, Materials science, Personal hygiene, Permeability (electromagnetism), Wound dressing, Anisotropic fluid, Composite material, Fluid transport

Abstract

Many of the nonwoven structures used for absorbent wound dressing applications as well as other personal hygiene products exhibit anisotropic fluid transmission characteristics which, depending on the application, can markedly influence performance in use. Fibre orientation in such structures is believed to have a major influence on anisotropic fluid transmission and can be manipulated (as required) to engineer desirable fluid transport properties. Experimental results are presented which demonstrate the anisotropic fluid transmission properties of typical wound dressing structures. A new model of directional permeability is presented which takes into account the fibre orientation function of the structure and is capable of predicting the permeability in both the cross and machine directions of the fabric. A new method of measuring fluid transmission in multiple directions is also introduced.

Published

2001

36. Recombinant mumps virus as a cancer therapeutic agent

Author

Arun Ammayappan, Stephen J Russell, and Mark J Federspiel

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Mumps virus belongs to the family of Paramyxoviridae and has the potential to be an oncolytic agent. Mumps virus Urabe strain had been tested in the clinical setting as a treatment for human cancer four decades ago in Japan. These clinical studies demonstrated that mumps virus could be a promising cancer therapeutic agent that showed significant antitumor activity against various types of cancers. Since oncolytic virotherapy was not in the limelight until the beginning of the 21st century, the interest to pursue mumps virus for cancer treatment slowly faded away. Recent success stories of oncolytic clinical trials prompted us to resurrect the mumps virus and to explore its potential for cancer treatment. We have obtained the Urabe strain of mumps virus from Osaka University, Japan, which was used in the earlier human clinical trials. In this report we describe the development of a reverse genetics system from a major isolate of this Urabe strain mumps virus stock, and the construction and characterization of several recombinant mumps viruses with additional transgenes. We present initial data demonstrating these recombinant mumps viruses have oncolytic activity against tumor cell lines in vitro and some efficacy in preliminary pilot animal tumor models.

Published

2016

37. A Broad Range of Dose Optima Achieve High-level, Long-term Gene Expression After Hydrodynamic Delivery of Sleeping Beauty Transposons Using Hyperactive SB100x Transposase

Author

Kelly M Podetz-Pedersen, Erik R Olson, Nikunj V Somia, Stephen J Russell, and R Scott McIvor

Subjects

hydrodynamic, liver, Sleeping Beauty, transposase, transposon, Therapeutics. Pharmacology, RM1-950

Abstract

The Sleeping Beauty (SB) transposon system has been shown to enable long-term gene expression by integrating new sequences into host cell chromosomes. We found that the recently reported SB100x hyperactive transposase conferred a surprisingly high level of long-term expression after hydrodynamic delivery of luciferase-encoding reporter transposons in the mouse. We conducted dose-ranging studies to determine the effect of varying the amount of SB100x transposase-encoding plasmid (pCMV-SB100x) at a set dose of luciferase transposon and of varying the amount of transposon-encoding DNA at a set dose of pCMV-SB100x in hydrodynamically injected mice. Animals were immunosuppressed using cyclophosphamide in order to prevent an antiluciferase immune response. At a set dose of transposon DNA (25 µg), we observed a broad range of pCMV-SB100x doses (0.1–2.5 µg) conferring optimal levels of long-term expression (>1011 photons/second/cm2). At a fixed dose of 0.5 μg of pCMV-SB100x, maximal long-term luciferase expression (>1010 photons/second/cm2) was achieved at a transposon dose of 5–125 μg. We also found that in the linear range of transposon doses (100 ng), co-delivering the CMV-SB100x sequence on the same plasmid was less effective in achieving long-term expression than delivery on separate plasmids. These results show marked flexibility in the doses of SB transposon plus pCMV-SB100x that achieve maximal SB-mediated gene transfer efficiency and long-term gene expression after hydrodynamic DNA delivery to mouse liver.

Published

2016

38. Oncolytic potency of HER-2 retargeted VSV-FH hybrid viruses: the role of receptor ligand affinity

Author

Camilo Ayala Breton, Nitwara Wikan, Arinda Abbuhl, Duncan R Smith, Stephen J Russell, and Kah-Whye Peng

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The hybrid oncolytic vesicular stomatitis virus (VSV-FH) deleted for its G glycoprotein and displaying the measles virus (MV) envelope glycoproteins (hemagglutinin H and fusion F) is fusogenic, infects cells via any of the three MV receptors and has potent oncolytic activity against subcutaneous and disseminated myeloma tumors. To tailor VSV-FH as an oncolytic virus for ovarian cancer, we ablated its natural tropism and retargeted the virus by display of a single-chain antibody (scFv) with specificity to the HER-2/neu receptor. A panel of six VSVFH-αHER2 viruses displaying anti-HER2 scFv that bind to the same HER2 epitope but with different Kd (10â6 to 10â11 M, VSVFH-αHER2#6 to #11, respectively) were rescued and characterized. A Kd of at least 10â8 M is required for infection of HER-2 positive SKOV3ip.1 cells. The higher affinity viruses (>10â8 M) were able to infect and fuse SKOV3ip.1 cells more efficiently, inducing more extensive cytopathic effects. We next compared the antitumor potency of the viruses against SKOV3ip.1 tumor xenografts. In contrast to the saline-treated animals, one intratumoral injection of VSVFH-αHER2#9, #10, or #11 resulted in efficient tumor control. There was no significant difference between viruses with an affinity higher than 10â9 M in terms of oncolytic potency. VSVFH-αHER2 virus may be a promising agent for the treatment of HER-2 positive malignancies.

Published

2015

39. Reporter gene imaging identifies intratumoral infection voids as a critical barrier to systemic oncolytic virus efficacy

Author

Amber Miller, Lukkana Suksanpaisan, Shruthi Naik, Rebecca Nace, Mark Federspiel, Kah Whye Peng, and Stephen J Russell

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Systemically administered oncolytic viruses have the ability to cause tumor destruction through the expansion and coalescence of intratumoral infectious centers. Efficacy is therefore dependent upon both the density and intratumoral distribution of virus-infected cells achieved after initial virus infusion, and delivery methods are being developed to enhance these critical parameters. However, the three-dimensional (3D) mapping of intratumoral infectious centers is difficult using conventional immunohistochemical methodology, requiring painstaking 3D reconstruction of numerous sequential stained tumor sections, with no ability to study the temporal evolution of spreading infection in a single animal. We therefore developed a system using very high-resolution noninvasive in vivo micro single-photon emitted computed tomography/computed tomography (microSPECT/CT) imaging to determine the intratumoral distribution of thyroid radiotracers in tumors infected with an oncolytic virus encoding the thyroidal sodium–iodide symporter (NIS). This imaging system was used for longitudinal analysis of the density, distribution, and evolution of intratumoral infectious centers after systemic administration of oncolytic vesicular stomatitis virus in tumor-bearing mice and revealed heterogeneous delivery of virus particles both within and between tumors in animals receiving identical therapy. This study provides compelling validation of high resolution in vivo reporter gene mapping as a convenient method for serial monitoring of intratumoral virus spread that will be necessary to address critical barriers to systemic oncolytic virus efficacy such as intratumoral delivery.

Published

2014