Effect of reduced dose schedules and intramuscular injection of anthrax vaccine adsorbed on immunological response and safety profile: A randomized trial

Jennifer G. Wright; Brian D. Plikaytis; Charles E. Rose; Scott D. Parker; Janiine Babcock; Wendy Keitel; Hana El Sahly; Gregory A. Poland; Robert M. Jacobson; Harry L. Keyserling; Vera A. Semenova; Han Li; Jarad Schiffer; Hanan Dababneh; Sandra K. Martin; Stacey W. Martin; Nina Marano; Nancy E. Messonnier; Conrad P. Quinn

doi:10.1016/j.vaccine.2013.10.039

Effect of reduced dose schedules and intramuscular injection of anthrax vaccine adsorbed on immunological response and safety profile: A randomized trial

Jennifer G. Wright, Brian D. Plikaytis, Charles E. Rose, Scott D. Parker, Janiine Babcock, Wendy Keitel, Hana El Sahly, Gregory A. Poland, Robert M. Jacobson, Harry L. Keyserling, Vera A. Semenova, Han Li, Jarad Schiffer, Hanan Dababneh, Sandra K. Martin, Stacey W. Martin, Nina Marano, Nancy E. Messonnier, Conrad P. Quinn

Research output: Contribution to journal › Article › peer-review

30 Scopus citations

Abstract

Objective: We evaluated an alternative administration route, reduced schedule priming series, and increased intervals between booster doses for anthrax vaccine adsorbed (AVA). AVA's originally licensed schedule was 6 subcutaneous (SQ) priming injections administered at months (m) 0, 0.5, 1, 6, 12 and 18 with annual boosters; a simpler schedule is desired. Methods: Through a multicenter randomized, double blind, non-inferiority Phase IV human clinical trial, the originally licensed schedule was compared to four alternative and two placebo schedules. 8-SQ group participants received 6 SQ injections with m30 and m42 "annual" boosters; participants in the 8-IM group received intramuscular (IM) injections according to the same schedule. Reduced schedule groups (7-IM, 5-IM, 4-IM) received IM injections at m0, m1, m6; at least one of the m0.5, m12, m18, m30 vaccine doses were replaced with saline. All reduced schedule groups received a m42 booster. Post-injection blood draws were taken two to four weeks following injection. Non-inferiority of the alternative schedules was compared to the 8-SQ group at m2, m7, and m43. Reactogenicity outcomes were proportions of injection site and systemic adverse events (AEs). Results: The 8-IM group's m2 response was non-inferior to the 8-SQ group for the three primary endpoints of anti-protective antigen IgG geometric mean concentration (GMC), geometric mean titer, and proportion of responders with a 4-fold rise in titer. At m7 anti-PA IgG GMCs for the three reduced dosage groups were non-inferior to the 8-SQ group GMCs. At m43, 8-IM, 5-IM, and 4-IM group GMCs were superior to the 8-SQ group. Solicited injection site AEs occurred at lower proportions in the IM group compared to SQ. Route of administration did not influence the occurrence of systemic AEs. A 3 dose IM priming schedule with doses administered at m0, m1, and m6 elicited long term immunological responses and robust immunological memory that was efficiently stimulated by a single booster vaccination at 42 months. Conclusions: A priming series of 3 intramuscular doses administered at m0, m1, and m6 with a triennial booster was non-inferior to more complex schedules for achieving antibody response.

Original language	English (US)
Pages (from-to)	1019-1028
Number of pages	10
Journal	Vaccine
Volume	32
Issue number	8
DOIs	https://doi.org/10.1016/j.vaccine.2013.10.039
State	Published - Feb 12 2014

Keywords

Adverse events
Anthrax vaccines
Bacillus anthracis
Bacterial vaccines
Vaccination

ASJC Scopus subject areas

Molecular Medicine
Immunology and Microbiology(all)
veterinary(all)
Public Health, Environmental and Occupational Health
Infectious Diseases

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10.1016/j.vaccine.2013.10.039

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Wright, J. G., Plikaytis, B. D., Rose, C. E., Parker, S. D., Babcock, J., Keitel, W., El Sahly, H., Poland, G. A., Jacobson, R. M., Keyserling, H. L., Semenova, V. A., Li, H., Schiffer, J., Dababneh, H., Martin, S. K., Martin, S. W., Marano, N., Messonnier, N. E., & Quinn, C. P. (2014). Effect of reduced dose schedules and intramuscular injection of anthrax vaccine adsorbed on immunological response and safety profile: A randomized trial. Vaccine, 32(8), 1019-1028. https://doi.org/10.1016/j.vaccine.2013.10.039

Wright, JG, Plikaytis, BD, Rose, CE, Parker, SD, Babcock, J, Keitel, W, El Sahly, H, Poland, GA, Jacobson, RM, Keyserling, HL, Semenova, VA, Li, H, Schiffer, J, Dababneh, H, Martin, SK, Martin, SW, Marano, N, Messonnier, NE & Quinn, CP 2014, 'Effect of reduced dose schedules and intramuscular injection of anthrax vaccine adsorbed on immunological response and safety profile: A randomized trial', Vaccine, vol. 32, no. 8, pp. 1019-1028. https://doi.org/10.1016/j.vaccine.2013.10.039

@article{8f2b75b4852344ac82240f880548959b,

title = "Effect of reduced dose schedules and intramuscular injection of anthrax vaccine adsorbed on immunological response and safety profile: A randomized trial",

abstract = "Objective: We evaluated an alternative administration route, reduced schedule priming series, and increased intervals between booster doses for anthrax vaccine adsorbed (AVA). AVA's originally licensed schedule was 6 subcutaneous (SQ) priming injections administered at months (m) 0, 0.5, 1, 6, 12 and 18 with annual boosters; a simpler schedule is desired. Methods: Through a multicenter randomized, double blind, non-inferiority Phase IV human clinical trial, the originally licensed schedule was compared to four alternative and two placebo schedules. 8-SQ group participants received 6 SQ injections with m30 and m42 {"}annual{"} boosters; participants in the 8-IM group received intramuscular (IM) injections according to the same schedule. Reduced schedule groups (7-IM, 5-IM, 4-IM) received IM injections at m0, m1, m6; at least one of the m0.5, m12, m18, m30 vaccine doses were replaced with saline. All reduced schedule groups received a m42 booster. Post-injection blood draws were taken two to four weeks following injection. Non-inferiority of the alternative schedules was compared to the 8-SQ group at m2, m7, and m43. Reactogenicity outcomes were proportions of injection site and systemic adverse events (AEs). Results: The 8-IM group's m2 response was non-inferior to the 8-SQ group for the three primary endpoints of anti-protective antigen IgG geometric mean concentration (GMC), geometric mean titer, and proportion of responders with a 4-fold rise in titer. At m7 anti-PA IgG GMCs for the three reduced dosage groups were non-inferior to the 8-SQ group GMCs. At m43, 8-IM, 5-IM, and 4-IM group GMCs were superior to the 8-SQ group. Solicited injection site AEs occurred at lower proportions in the IM group compared to SQ. Route of administration did not influence the occurrence of systemic AEs. A 3 dose IM priming schedule with doses administered at m0, m1, and m6 elicited long term immunological responses and robust immunological memory that was efficiently stimulated by a single booster vaccination at 42 months. Conclusions: A priming series of 3 intramuscular doses administered at m0, m1, and m6 with a triennial booster was non-inferior to more complex schedules for achieving antibody response.",

keywords = "Adverse events, Anthrax vaccines, Bacillus anthracis, Bacterial vaccines, Vaccination",

author = "Wright, {Jennifer G.} and Plikaytis, {Brian D.} and Rose, {Charles E.} and Parker, {Scott D.} and Janiine Babcock and Wendy Keitel and {El Sahly}, Hana and Poland, {Gregory A.} and Jacobson, {Robert M.} and Keyserling, {Harry L.} and Semenova, {Vera A.} and Han Li and Jarad Schiffer and Hanan Dababneh and Martin, {Sandra K.} and Martin, {Stacey W.} and Nina Marano and Messonnier, {Nancy E.} and Quinn, {Conrad P.}",

note = "Funding Information: Anthrax Vaccine Research Program (AVRP) Working Group members: Baylor College of Medicine: N. Bond, D. Nino, C. Rangel, C. Tajonera. WRAIR: S. Cicatelli, R. Newcomer, R. Nielsen. Mayo Clinic: P. Targonski, I. Ovsyannikova, N. Pinsky. Emory University School of Medicine: J. Hilinski, M. Leonard, P. Anderson, V. Grimes, K. Luehrs, P. Newsome, J. Skvarich, K. Stephens. University of Alabama, Birmingham: M. Mulligan, F. Johnson, J. Moody, L. Williams, F. Smith. CDC Microbial Pathogenesis & Immune Response (MPIR) Laboratory: D. Aranio, M. Brawner, N. Brown*, J. Caba*, S. Crenshaw*, L. Cronin*, R. Desai, L. Foster*, J. Lewis*, F. Lyde*, A. Milton*, H. Noland*, N. Patel*, D. Schmidt, S. Shields*, D. Smith*, E. Steward-Clark, R. Thompson*, J. Walls. CDC, Division of Bacterial Diseases: W. Holt, J. Jarrell, F. David, S. Shah; M. McNeil; J. Stamper, J. Wheeling, S. Mohammed. * Funded by the Atlanta Research and Education Foundation (AREF) through the Department of Veterans Affairs, Veterans Health Administration, Office of Research and Development, Atlanta, GA. ",

year = "2014",

month = feb,

day = "12",

doi = "10.1016/j.vaccine.2013.10.039",

language = "English (US)",

volume = "32",

pages = "1019--1028",

journal = "Vaccine",

issn = "0264-410X",

publisher = "Elsevier BV",

number = "8",

}

TY - JOUR

T1 - Effect of reduced dose schedules and intramuscular injection of anthrax vaccine adsorbed on immunological response and safety profile

T2 - A randomized trial

AU - Wright, Jennifer G.

AU - Plikaytis, Brian D.

AU - Rose, Charles E.

AU - Parker, Scott D.

AU - Babcock, Janiine

AU - Keitel, Wendy

AU - El Sahly, Hana

AU - Poland, Gregory A.

AU - Jacobson, Robert M.

AU - Keyserling, Harry L.

AU - Semenova, Vera A.

AU - Li, Han

AU - Schiffer, Jarad

AU - Dababneh, Hanan

AU - Martin, Sandra K.

AU - Martin, Stacey W.

AU - Marano, Nina

AU - Messonnier, Nancy E.

AU - Quinn, Conrad P.

N1 - Funding Information: Anthrax Vaccine Research Program (AVRP) Working Group members: Baylor College of Medicine: N. Bond, D. Nino, C. Rangel, C. Tajonera. WRAIR: S. Cicatelli, R. Newcomer, R. Nielsen. Mayo Clinic: P. Targonski, I. Ovsyannikova, N. Pinsky. Emory University School of Medicine: J. Hilinski, M. Leonard, P. Anderson, V. Grimes, K. Luehrs, P. Newsome, J. Skvarich, K. Stephens. University of Alabama, Birmingham: M. Mulligan, F. Johnson, J. Moody, L. Williams, F. Smith. CDC Microbial Pathogenesis & Immune Response (MPIR) Laboratory: D. Aranio, M. Brawner, N. Brown*, J. Caba*, S. Crenshaw*, L. Cronin*, R. Desai, L. Foster*, J. Lewis*, F. Lyde*, A. Milton*, H. Noland*, N. Patel*, D. Schmidt, S. Shields*, D. Smith*, E. Steward-Clark, R. Thompson*, J. Walls. CDC, Division of Bacterial Diseases: W. Holt, J. Jarrell, F. David, S. Shah; M. McNeil; J. Stamper, J. Wheeling, S. Mohammed. * Funded by the Atlanta Research and Education Foundation (AREF) through the Department of Veterans Affairs, Veterans Health Administration, Office of Research and Development, Atlanta, GA.

PY - 2014/2/12

Y1 - 2014/2/12

N2 - Objective: We evaluated an alternative administration route, reduced schedule priming series, and increased intervals between booster doses for anthrax vaccine adsorbed (AVA). AVA's originally licensed schedule was 6 subcutaneous (SQ) priming injections administered at months (m) 0, 0.5, 1, 6, 12 and 18 with annual boosters; a simpler schedule is desired. Methods: Through a multicenter randomized, double blind, non-inferiority Phase IV human clinical trial, the originally licensed schedule was compared to four alternative and two placebo schedules. 8-SQ group participants received 6 SQ injections with m30 and m42 "annual" boosters; participants in the 8-IM group received intramuscular (IM) injections according to the same schedule. Reduced schedule groups (7-IM, 5-IM, 4-IM) received IM injections at m0, m1, m6; at least one of the m0.5, m12, m18, m30 vaccine doses were replaced with saline. All reduced schedule groups received a m42 booster. Post-injection blood draws were taken two to four weeks following injection. Non-inferiority of the alternative schedules was compared to the 8-SQ group at m2, m7, and m43. Reactogenicity outcomes were proportions of injection site and systemic adverse events (AEs). Results: The 8-IM group's m2 response was non-inferior to the 8-SQ group for the three primary endpoints of anti-protective antigen IgG geometric mean concentration (GMC), geometric mean titer, and proportion of responders with a 4-fold rise in titer. At m7 anti-PA IgG GMCs for the three reduced dosage groups were non-inferior to the 8-SQ group GMCs. At m43, 8-IM, 5-IM, and 4-IM group GMCs were superior to the 8-SQ group. Solicited injection site AEs occurred at lower proportions in the IM group compared to SQ. Route of administration did not influence the occurrence of systemic AEs. A 3 dose IM priming schedule with doses administered at m0, m1, and m6 elicited long term immunological responses and robust immunological memory that was efficiently stimulated by a single booster vaccination at 42 months. Conclusions: A priming series of 3 intramuscular doses administered at m0, m1, and m6 with a triennial booster was non-inferior to more complex schedules for achieving antibody response.

AB - Objective: We evaluated an alternative administration route, reduced schedule priming series, and increased intervals between booster doses for anthrax vaccine adsorbed (AVA). AVA's originally licensed schedule was 6 subcutaneous (SQ) priming injections administered at months (m) 0, 0.5, 1, 6, 12 and 18 with annual boosters; a simpler schedule is desired. Methods: Through a multicenter randomized, double blind, non-inferiority Phase IV human clinical trial, the originally licensed schedule was compared to four alternative and two placebo schedules. 8-SQ group participants received 6 SQ injections with m30 and m42 "annual" boosters; participants in the 8-IM group received intramuscular (IM) injections according to the same schedule. Reduced schedule groups (7-IM, 5-IM, 4-IM) received IM injections at m0, m1, m6; at least one of the m0.5, m12, m18, m30 vaccine doses were replaced with saline. All reduced schedule groups received a m42 booster. Post-injection blood draws were taken two to four weeks following injection. Non-inferiority of the alternative schedules was compared to the 8-SQ group at m2, m7, and m43. Reactogenicity outcomes were proportions of injection site and systemic adverse events (AEs). Results: The 8-IM group's m2 response was non-inferior to the 8-SQ group for the three primary endpoints of anti-protective antigen IgG geometric mean concentration (GMC), geometric mean titer, and proportion of responders with a 4-fold rise in titer. At m7 anti-PA IgG GMCs for the three reduced dosage groups were non-inferior to the 8-SQ group GMCs. At m43, 8-IM, 5-IM, and 4-IM group GMCs were superior to the 8-SQ group. Solicited injection site AEs occurred at lower proportions in the IM group compared to SQ. Route of administration did not influence the occurrence of systemic AEs. A 3 dose IM priming schedule with doses administered at m0, m1, and m6 elicited long term immunological responses and robust immunological memory that was efficiently stimulated by a single booster vaccination at 42 months. Conclusions: A priming series of 3 intramuscular doses administered at m0, m1, and m6 with a triennial booster was non-inferior to more complex schedules for achieving antibody response.

KW - Adverse events

KW - Anthrax vaccines

KW - Bacillus anthracis

KW - Bacterial vaccines

KW - Vaccination

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Effect of reduced dose schedules and intramuscular injection of anthrax vaccine adsorbed on immunological response and safety profile: A randomized trial

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