Your search keyword '"Newman, Frances K."' showing total 5 results

1. Influenza virus vaccination of patients with chronic lung disease

Author

Gorse, Geoffrey J., Otto, Esther E., Daughaday, Carlos C., Newman, Frances K., Eickhoff, Christopher S., Powers, Douglas C., and Lusk, Rodney H.

Subjects

Influenza vaccines -- Usage, Influenza -- Prevention, Health, Prevention, Usage

Abstract

Study objectives: To evaluate the safety of, and mucosal and systemic immune responses induced by two influenza virus vaccine regimens in subjects with COPD. Design: Single-center, blinded, randomized, prospective clinical trial evaluating two vaccine regimens. Setting: Outpatient clinics of St. Louis Department of Veterans Affairs Medical Center. Participants: Volunteers (age range, 42 to 88 years) had preexisting COPD with severe obstruction to airflow on average, were male, and were not receiving immunosuppressive medication. Interventions: Twenty-nine volunteers were randomly assigned to receive either bivalent live attenuated influenza A virus vaccine (CAV) or saline solution placebo . All subjects also received an IM injection of trivalent inactivated influenza virus vaccine (TVV) simultaneously. Measurements and results: Clinical status and pulmonary function measured by spirometry did not change significantly after vaccination. Using hemagglutinins (H1 and H3 HA) which more closely resembled dose in CAV, mean levels of anti-HA immunoglobulin A (IgA) antibodies im nasal washings increased significantly after vaccination with CAV and TVV compared to prevaccination, but they did not increase significantly after TVV and intranasal placebo. Mean levels of influenza A virus-stimulated interleukin-2 and -4 produced by peripheral blood mononuclear cells in vitro increased significantly after administration of the combination vaccine regimen and to a lesser extent after TVV and intranasal placebo compared to respective prevaccination levels. The timing of the cytokine response appeared different following CAV and TVV compared to TVV and intranasal placebo. Conclusions: Intranasally administered CAV was safe when given with IM administered TVV and there may be an immunologic advantage to administration of the combination vaccine regimen compared to TVV with intranasal placebo. (CHEST 1997; 112:1221-33) Key words: cellular immunity; chronic lung disease; immune response; influenza A Virus; mucosal immunity; vaccines Abbreviations: CAV=bivalent, cold-recombinant, live attenuated influenza A virus vaccine; ELISA=enzyme-linked immunosorbent assay; GMT=geometric mean titer; H1, H2, and H3=hemagglutinin subtypes 1, 2, and 3, respectively; HA=hemagglutinin; HAI=hemagglutination inhibition; IFN-[Gamma]=interferon-gamma; Ig=immunoglobulin; IL=interleukin; N1 and N2=neuraminidase subtypes 1 and 2, respectively NS=not significant; PBL=peripheral blood mononuclear cells; [TCID.sub.50] = 50% tissue culture infective dose; TH1 and TH2=helper T-cell subsets 1 and 2, respectively; TVV=trivalent inactivated subvirion influenza virus vaccine, Patients with chronic underlying illnesses such as COPD have an increased risk for respiratory illness-related hospitalization during influenza outbreaks independent of age, and morbidity and mortality in excess of the [...]

Published

1997

2. Comparison of the safety and immunogenicity of ACAM1000, ACAM2000 and Dryvax® in healthy vaccinia-naive adults

Author

Frey, Sharon E., Newman, Frances K., Kennedy, Jeffrey S., Ennis, Francis, Abate, Getahun, Hoft, Daniel F., and Monath, Thomas P.

Subjects

*IMMUNOGENETICS, *SMALLPOX vaccines, *MEDICATION safety, *BLIND experiment, *CELL culture, *DRUG development, *VACCINIA, *VIRAL vaccines, *CELLULAR immunity

Abstract

Abstract: Currently, more than half of the world''s population has no immunity against smallpox variola major virus. This phase I double-blind, randomized trial was conducted to compare the safety and immunogenicity of two clonally derived, cell-culture manufactured vaccinia strains, ACAM1000 and ACAM2000, to the parent vaccine, Dryvax®. Thirty vaccinia-naïve subjects were enrolled into each of three groups and vaccines were administered percutaneously using a bifurcated needle at a dose of 1.0×108 PFU/mL. All subjects had a primary skin reaction indicating a successful vaccination. The adverse events, 4-fold neutralizing antibody rise and T cell immune responses were similar between the groups. [Copyright &y& Elsevier]

Published

2009

3. Clinical and immunologic responses to multiple doses of IMVAMUNE® (Modified Vaccinia Ankara) followed by Dryvax® challenge

Author

Frey, Sharon E., Newman, Frances K., Kennedy, Jeffrey S., Sobek, Vera, Ennis, Francis A., Hill, Heather, Yan, Lihan K., Chaplin, Paul, Vollmar, Jens, Chaitman, Bernard R., and Belshe, Robert B.

Subjects

*SMALLPOX vaccines, *IMMUNIZATION, *IMMUNITY

Abstract

Abstract: Smallpox vaccination with replication deficient vaccinia strains such as Modified Vaccinia Ankara (MVA) may induce protective immunity with improved safety and tolerability profiles compared with currently available smallpox vaccines. Ninety subjects were randomized equally to six groups in a partially blinded, randomized, controlled clinical trial. IMVAMUNE® (MVA-BN®, Bavarian Nordic A/S, Kvistgård, Denmark) vaccine or placebo was administered at Study Days 0 and 28 by subcutaneous or intramuscular injection and five groups were challenged with Dryvax® at study Day 112. Vaccination with two doses of IMVAMUNE® was safe and well tolerated compared to Dryvax®. IMVAMUNE® produced comparable cellular and humoral immune responses to one dose of Dryvax® and the immunity induced appears robust 90 days post-vaccination by evidence of attenuated primary cutaneous reaction responses following Dryvax®. IMVAMUNE® vaccination prior to Dryvax® reduced virus replication at the Dryvax® site, decreased the size of the primary cutaneous lesion, and decreased the time to healing but did not completely ameliorate the immune response. [Copyright &y& Elsevier]

Published

2007

4. Comparative immunogenicity of trivalent influenza vaccine administered by intradermal or intramuscular route in healthy adults

Author

Belshe, Robert B., Newman, Frances K., Wilkins, Ken, Graham, Irene L., Babusis, Elizabeth, Ewell, Marian, and Frey, Sharon E.

Subjects

*PREVENTIVE medicine, *INFLUENZA prevention, *INFLUENZA viruses, *CLINICAL trials

Abstract

Abstract: The present study was undertaken with controls using equal doses ID and IM plus the standard full dose IM to assess the role of route of vaccine in immunogenicity of inactivated influenza vaccine. The study was a prospective, randomized, active-controlled, open label clinical trial conducted in healthy young adult outpatients to compare the effect of route (IM versus ID) on antibody responses to influenza vaccine. Volunteers received 3, 6 or 9μg of vaccine by ID or IM route; 15μg IM was also studied. Low doses of vaccine given by either route were almost as immunogenic as the standard 15μg IM dose of influenza vaccine. ID route was not superior to IM vaccine at inducing antibodies. ID vaccine induced significantly more local inflammatory response than IM vaccine. [Copyright &y& Elsevier]

Published

2007

5. Safety and immunogenicity of IMVAMUNE smallpox vaccine using different strategies for a post event scenario.

Author

Frey, Sharon E., Winokur, Patricia L., Salata, Robert A., El-Kamary, Samer S., Turley, Christine B., Walter, Emmanuel B., Hay, Christine Mhorag, Newman, Frances K., Hill, Heather R., Zhang, Ying, Chaplin, Paul, Tary-Lehmann, Magdalena, and Belshe, Robert B.

Subjects

*SMALLPOX vaccines, *VACCINE safety, *IMMUNOGENETICS, *BIOTERRORISM, *INF (Computer program language), *IMMUNOGLOBULINS, *IMMUNE response, *DRUG dosage

Abstract

Highlights: [•] Reintroduction of Variola major as an agent of bioterrorism remains a concern. [•] A compressed schedule of MVA was evaluated for use in a post event scenario. [•] MVA is well tolerated when given as two standard doses at Days 0 and 28 or 0 and 7. [•] A 2nd dose of MVA at Day 28 compared to Day 7 provided greater antibody responses. [•] INF-γ expression was greatest within 2 weeks after last vaccination. [ABSTRACT FROM AUTHOR]

Published

2013