Your search keyword '"Kelly L. Warfield"' showing total 8 results

1. Combination Therapy with UV-4B and Molnupiravir Enhances SARS-CoV-2 Suppression

Author

Evelyn J. Franco, George L. Drusano, Kaley C. Hanrahan, Kelly L. Warfield, and Ashley N. Brown

Subjects

UV-4B, EIDD-1931, combination therapy, SARS-CoV-2, COVID-19, variant, Microbiology, QR1-502

Abstract

The host targeting antiviral, UV-4B, and the RNA polymerase inhibitor, molnupiravir, are two orally available, broad-spectrum antivirals that have demonstrated potent activity against SARS-CoV-2 as monotherapy. In this work, we evaluated the effectiveness of UV-4B and EIDD-1931 (molnupiravir’s main circulating metabolite) combination regimens against the SARS-CoV-2 beta, delta, and omicron BA.2 variants in a human lung cell line. Infected ACE2 transfected A549 (ACE2-A549) cells were treated with UV-4B and EIDD-1931 both as monotherapy and in combination. Viral supernatant was sampled on day three when viral titers peaked in the no-treatment control arm, and levels of infectious virus were measured by plaque assay. The drug–drug effect interaction between UV-4B and EIDD-1931 was also defined using the Greco Universal Response Surface Approach (URSA) model. Antiviral evaluations demonstrated that treatment with UV-4B plus EIDD-1931 enhanced antiviral activity against all three variants relative to monotherapy. These results were in accordance with those obtained from the Greco model, as these identified the interaction between UV-4B and EIDD-1931 as additive against the beta and omicron variants and synergistic against the delta variant. Our findings highlight the anti-SARS-CoV-2 potential of UV-4B and EIDD-1931 combination regimens, and present combination therapy as a promising therapeutic strategy against SARS-CoV-2.

Published

2023

2. A Novel Iminosugar UV-12 with Activity against the Diverse Viruses Influenza and Dengue (Novel Iminosugar Antiviral for Influenza and Dengue)

Author

Kelly L. Warfield, Emily Plummer, Dominic S. Alonzi, Gary W. Wolfe, Aruna Sampath, Tam Nguyen, Terry D. Butters, Sven G. Enterlein, Eric J. Stavale, Sujan Shresta, and Urban Ramstedt

Subjects

glucosidase, glycosylation, Flaviviridae, flavivirus, Orthomyxoviridae, orthomyxovirus, mouse, Microbiology, QR1-502

Abstract

Iminosugars are capable of targeting the life cycles of multiple viruses by blocking host endoplasmic reticulum α-glucosidase enzymes that are required for competent replication of a variety of enveloped, glycosylated viruses. Iminosugars as a class are approved for use in humans with diseases such as diabetes and Gaucher’s disease, providing evidence for safety of this class of compounds. The in vitro antiviral activity of iminosugars has been described in several publications with a subset of these demonstrating in vivo activity against flaviviruses, herpesviruses, retroviruses and filoviruses. Although there is compelling non-clinical in vivo evidence of antiviral efficacy, the efficacy of iminosugars as antivirals has yet to be demonstrated in humans. In the current study, we report a novel iminosugar, UV-12, which has efficacy against dengue and influenza in mouse models. UV-12 exhibits drug-like properties including oral bioavailability and good safety profile in mice and guinea pigs. UV-12 is an example of an iminosugar with activity against multiple virus families that should be investigated in further safety and efficacy studies and demonstrates potential value of this drug class as antiviral therapeutics.

Published

2015

3. Filovirus RefSeq Entries: Evaluation and Selection of Filovirus Type Variants, Type Sequences, and Names

Author

Jens H. Kuhn, Kristian G. Andersen, Yīmíng Bào, Sina Bavari, Stephan Becker, Richard S. Bennett, Nicholas H. Bergman, Olga Blinkova, Steven Bradfute, J. Rodney Brister, Alexander Bukreyev, Kartik Chandran, Alexander A. Chepurnov, Robert A. Davey, Ralf G. Dietzgen, Norman A. Doggett, Olga Dolnik, John M. Dye, Sven Enterlein, Paul W. Fenimore, Pierre Formenty, Alexander N. Freiberg, Robert F. Garry, Nicole L. Garza, Stephen K. Gire, Jean-Paul Gonzalez, Anthony Griffiths, Christian T. Happi, Lisa E. Hensley, Andrew S. Herbert, Michael C. Hevey, Thomas Hoenen, Anna N. Honko, Georgy M. Ignatyev, Peter B. Jahrling, Joshua C. Johnson, Karl M. Johnson, Jason Kindrachuk, Hans-Dieter Klenk, Gary Kobinger, Tadeusz J. Kochel, Matthew G. Lackemeyer, Daniel F. Lackner, Eric M. Leroy, Mark S. Lever, Elke Mühlberger, Sergey V. Netesov, Gene G. Olinger, Sunday A. Omilabu, Gustavo Palacios, Rekha G. Panchal, Daniel J. Park, Jean L. Patterson, Janusz T. Paweska, Clarence J. Peters, James Pettitt, Louise Pitt, Sheli R. Radoshitzky, Elena I. Ryabchikova, Erica Ollmann Saphire, Pardis C. Sabeti, Rachel Sealfon, Aleksandr M. Shestopalov, Sophie J. Smither, Nancy J. Sullivan, Robert Swanepoel, Ayato Takada, Jonathan S. Towner, Guido van der Groen, Viktor E. Volchkov, Valentina A. Volchkova, Victoria Wahl-Jensen, Travis K. Warren, Kelly L. Warfield, Manfred Weidmann, and Stuart T. Nichol

Subjects

Bundibugyo virus, cDNA clone, cuevavirus, Ebola, Ebola virus, ebolavirus, filovirid, Filoviridae, filovirus, genome annotation, ICTV, International Committee on Taxonomy of Viruses, Lloviu virus, Marburg virus, marburgvirus, mononegavirad, Mononegavirales, mononegavirus, Ravn virus, RefSeq, Reston virus, reverse genetics, Sudan virus, Taï Forest virus, virus classification, virus isolate, virus nomenclature, virus strain, virus taxonomy, virus variant, Microbiology, QR1-502

Abstract

Sequence determination of complete or coding-complete genomes of viruses is becoming common practice for supporting the work of epidemiologists, ecologists, virologists, and taxonomists. Sequencing duration and costs are rapidly decreasing, sequencing hardware is under modification for use by non-experts, and software is constantly being improved to simplify sequence data management and analysis. Thus, analysis of virus disease outbreaks on the molecular level is now feasible, including characterization of the evolution of individual virus populations in single patients over time. The increasing accumulation of sequencing data creates a management problem for the curators of commonly used sequence databases and an entry retrieval problem for end users. Therefore, utilizing the data to their fullest potential will require setting nomenclature and annotation standards for virus isolates and associated genomic sequences. The National Center for Biotechnology Information’s (NCBI’s) RefSeq is a non-redundant, curated database for reference (or type) nucleotide sequence records that supplies source data to numerous other databases. Building on recently proposed templates for filovirus variant naming [ ()////-], we report consensus decisions from a majority of past and currently active filovirus experts on the eight filovirus type variants and isolates to be represented in RefSeq, their final designations, and their associated sequences.

Published

2014

4. Mouse Models for Filovirus Infections

Author

Kelly L. Warfield, Steven B. Bradfute, and Mike Bray

Subjects

filovirus, Ebola, Marburg, mouse models, hemorrhagic fever, Microbiology, QR1-502

Abstract

The filoviruses marburg- and ebolaviruses can cause severe hemorrhagic fever (HF) in humans and nonhuman primates. Because many cases have occurred in geographical areas lacking a medical research infrastructure, most studies of the pathogenesis of filoviral HF, and all efforts to develop drugs and vaccines, have been carried out in biocontainment laboratories in non-endemic countries, using nonhuman primates (NHPs), guinea pigs and mice as animal models. NHPs appear to closely mirror filoviral HF in humans (based on limited clinical data), but only small numbers may be used in carefully regulated experiments; much research is therefore done in rodents. Because of their availability in large numbers and the existence of a wealth of reagents for biochemical and immunological testing, mice have become the preferred small animal model for filovirus research. Since the first experiments following the initial 1967 marburgvirus outbreak, wild-type or mouse-adapted viruses have been tested in immunocompetent or immunodeficient mice. In this paper, we review how these types of studies have been used to investigate the pathogenesis of filoviral disease, identify immune responses to infection and evaluate antiviral drugs and vaccines. We also discuss the strengths and weaknesses of murine models for filovirus research, and identify important questions for further study.

Published

2012

5. Virus-Like Particle Vaccination Protects Nonhuman Primates from Lethal Aerosol Exposure with Marburgvirus (VLP Vaccination Protects Macaques against Aerosol Challenges)

Author

John M. Dye, Kelly L. Warfield, Jay B. Wells, Robert C. Unfer, Sergey Shulenin, Hong Vu, Donald K. Nichols, M. Javad Aman, and Sina Bavari

Subjects

Marburg virus, virus-like particle, vaccine, macaque, aerosol, adjuvant, Microbiology, QR1-502

Abstract

Marburg virus (MARV) was the first filovirus to be identified following an outbreak of viral hemorrhagic fever disease in Marburg, Germany in 1967. Due to several factors inherent to filoviruses, they are considered a potential bioweapon that could be disseminated via an aerosol route. Previous studies demonstrated that MARV virus-like particles (VLPs) containing the glycoprotein (GP), matrix protein VP40 and nucleoprotein (NP) generated using a baculovirus/insect cell expression system could protect macaques from subcutaneous (SQ) challenge with multiple species of marburgviruses. In the current study, the protective efficacy of the MARV VLPs in conjunction with two different adjuvants: QS-21, a saponin derivative, and poly I:C against homologous aerosol challenge was assessed in cynomolgus macaques. Antibody responses against the GP antigen were equivalent in all groups receiving MARV VLPs irrespective of the adjuvant; adjuvant only-vaccinated macaques did not demonstrate appreciable antibody responses. All macaques were subsequently challenged with lethal doses of MARV via aerosol or SQ as a positive control. All MARV VLP-vaccinated macaques survived either aerosol or SQ challenge while animals administered adjuvant only exhibited clinical signs and lesions consistent with MARV disease and were euthanized after meeting the predetermined criteria. Therefore, MARV VLPs induce IgG antibodies recognizing MARV GP and VP40 and protect cynomolgus macaques from an otherwise lethal aerosol exposure with MARV.

Published

2016

6. The Iminosugar UV-4 is a Broad Inhibitor of Influenza A and B Viruses ex Vivo and in Mice

Author

Kelly L. Warfield, Dale L. Barnard, Sven G. Enterlein, Donald F. Smee, Mansoora Khaliq, Aruna Sampath, Michael V. Callahan, Urban Ramstedt, and Craig W. Day

Subjects

Iminosugar, UV-4B, influenza, human bronchial epithelial cells, antiviral, mice, Microbiology, QR1-502

Abstract

Iminosugars that are competitive inhibitors of endoplasmic reticulum (ER) α-glucosidases have been demonstrated to have antiviral activity against a diverse set of viruses. A novel iminosugar, UV-4B, has recently been shown to provide protection against lethal infections with dengue and influenza A (H1N1) viruses in mice. In the current study, the breadth of activity of UV-4B against influenza was examined ex vivo and in vivo. Efficacy of UV-4B against influenza A and B viruses was shown in primary human bronchial epithelial cells, a principal target tissue for influenza. Efficacy of UV-4B against influenza A (H1N1 and H3N2 subtypes) and influenza B was demonstrated using multiple lethal mouse models with readouts including mortality and weight loss. Clinical trials are ongoing to demonstrate safety of UV-4B and future studies to evaluate antiviral activity against influenza in humans are planned.

Published

2016

7. Filovirus RefSeq Entries: Evaluation and Selection of Filovirus Type Variants, Type Sequences, and Names

Author

Stephen K. Gire, Kristian G. Andersen, James Pettitt, Victoria Wahl-Jensen, Rachel Sealfon, Peter B. Jahrling, Janusz T. Paweska, Mark S. Lever, Eric M. Leroy, Nancy J. Sullivan, Louise Pitt, Erica Ollmann Saphire, Jonathan S. Towner, Olga Dolnik, Viktor E. Volchkov, Alexander N. Freiberg, Jean-Paul Gonzalez, Guido van der Groen, Lisa E. Hensley, Gary P. Kobinger, Christian T. Happi, Clarence J. Peters, Pardis C. Sabeti, Stuart T. Nichol, Kelly L. Warfield, Nicole L. Garza, Sina Bavari, Sunday Omilabu, Pierre Formenty, J. Rodney Brister, Jean L. Patterson, Stephan Becker, Aleksandr M. Shestopalov, Michael Hevey, Sophie J. Smither, Valentina A. Volchkova, Jason Kindrachuk, Yiming Bao, Kartik Chandran, Ralf G. Dietzgen, Sheli R. Radoshitzky, Elke Mühlberger, Robert F. Garry, Thomas Hoenen, Robert Swanepoel, Daniel J. Park, Steven B. Bradfute, Paul W. Fenimore, Jens H. Kuhn, Alexander A. Chepurnov, Tadeusz J. Kochel, Manfred Weidmann, Anna N. Honko, Elena I. Ryabchikova, John M. Dye, Karl M. Johnson, Nicholas H. Bergman, Gustavo Palacios, Ayato Takada, Daniel F. Lackner, Gene G. Olinger, Hans-Dieter Klenk, Olga Blinkova, Sven Enterlein, Robert A. Davey, Sergey V. Netesov, Andrew S. Herbert, Richard S. Bennett, Rekha G. Panchal, Norman A. Doggett, Georgy M. Ignatyev, Matthew G. Lackemeyer, Joshua C. Johnson, Alexander Bukreyev, Travis K. Warren, and Anthony Griffiths

Subjects

virus strain, Letter, genome annotation, marburgvirus, lcsh:QR1-502, virus nomenclature, medicine.disease_cause, lcsh:Microbiology, virus variant, Ebola virus, ICTV, Bundibugyo virus, RefSeq, Lloviu virus, cDNA clone, virus classification, Ravn virus, Marburg virus, biology, Genome project, Cuevavirus, Sudan virus, Infectious Diseases, Ebola, Reston virus, Databases, Nucleic Acid, cuevavirus, filovirus, filovirid, Computational biology, virus taxonomy, International Committee on Taxonomy of Viruses, Evolution, Molecular, Annotation, reverse genetics, Virology, medicine, Humans, virus isolate, Selection, Genetic, Virus classification, ebolavirus, Sequence (medicine), mononegavirus, mononegavirad, biology.organism_classification, Filoviridae, Mononegavirales, Taï Forest virus

Abstract

Sequence determination of complete or coding-complete genomes of viruses is becoming common practice for supporting the work of epidemiologists, ecologists, virologists, and taxonomists. Sequencing duration and costs are rapidly decreasing, sequencing hardware is under modification for use by non-experts, and software is constantly being improved to simplify sequence data management and analysis. Thus, analysis of virus disease outbreaks on the molecular level is now feasible, including characterization of the evolution of individual virus populations in single patients over time. The increasing accumulation of sequencing data creates a management problem for the curators of commonly used sequence databases and an entry retrieval problem for end users. Therefore, utilizing the data to their fullest potential will require setting nomenclature and annotation standards for virus isolates and associated genomic sequences. The National Center for Biotechnology Information’s (NCBI’s) RefSeq is a non-redundant, curated database for reference (or type) nucleotide sequence records that supplies source data to numerous other databases. Building on recently proposed templates for filovirus variant naming [ ()////-], we report consensus decisions from a majority of past and currently active filovirus experts on the eight filovirus type variants and isolates to be represented in RefSeq, their final designations, and their associated sequences.

Published

2014

8. The Iminosugar UV-4 is a Broad Inhibitor of Influenza A and B Viruses ex Vivo and in Mice

Author

Michael V. Callahan, Kelly L. Warfield, Dale L. Barnard, Donald F. Smee, Craig W. Day, Mansoora Khaliq, Sven Enterlein, Aruna Sampath, and Urban Ramstedt

Subjects

0301 basic medicine, 1-Deoxynojirimycin, mice, 030106 microbiology, lcsh:QR1-502, Iminosugar, Biology, medicine.disease_cause, Antiviral Agents, lcsh:Microbiology, Dengue fever, 03 medical and health sciences, chemistry.chemical_compound, UV-4B, Orthomyxoviridae Infections, In vivo, Virology, human bronchial epithelial cells, Influenza A virus, medicine, Animals, Humans, Cells, Cultured, Communication, Endoplasmic reticulum, Body Weight, virus diseases, Epithelial Cells, Influenza a, medicine.disease, Survival Analysis, antiviral, Disease Models, Animal, Influenza B virus, Treatment Outcome, 030104 developmental biology, Infectious Diseases, chemistry, influenza, Ex vivo

Abstract

Iminosugars that are competitive inhibitors of endoplasmic reticulum (ER) α-glucosidases have been demonstrated to have antiviral activity against a diverse set of viruses. A novel iminosugar, UV-4B, has recently been shown to provide protection against lethal infections with dengue and influenza A (H1N1) viruses in mice. In the current study, the breadth of activity of UV-4B against influenza was examined ex vivo and in vivo. Efficacy of UV-4B against influenza A and B viruses was shown in primary human bronchial epithelial cells, a principal target tissue for influenza. Efficacy of UV-4B against influenza A (H1N1 and H3N2 subtypes) and influenza B was demonstrated using multiple lethal mouse models with readouts including mortality and weight loss. Clinical trials are ongoing to demonstrate safety of UV-4B and future studies to evaluate antiviral activity against influenza in humans are planned.

Published

2016