Safety and immunogenicity of 26-valent group A streptococcus vaccine in healthy adult volunteers

Shelly A. McNeil; Scott A. Halperin; Joanne M. Langley; Bruce Smith; Andrew Warren; Geoffrey P. Sharratt; Darlene M. Baxendale; Mark A. Reddish; Mary C. Hu; Steven D. Stroop; Janine Linden; Louis F. Fries; Peter E. Vink; James B. Dale

doi:10.1086/444458

Safety and immunogenicity of 26-valent group A streptococcus vaccine in healthy adult volunteers

Shelly A. McNeil, Scott A. Halperin, Joanne M. Langley, Bruce Smith, Andrew Warren, Geoffrey P. Sharratt, Darlene M. Baxendale, Mark A. Reddish, Mary C. Hu, Steven D. Stroop, Janine Linden, Louis F. Fries, Peter E. Vink, James B. Dale

Medicine

Résultat de recherche: Article › examen par les pairs

277 Citations (Scopus)

Résumé

Background. Group A streptococcus (GAS) causes illness ranging from uncomplicated pharyngitis to life-threatening necrotizing fasciitis, toxic shock, and rheumatic fever. Attempts to develop an M protein-based vaccine have been hindered by the fact that some M proteins elicit both protective antibodies and antibodies that cross-react with human tissues. New molecular techniques have allowed the previous obstacles to be largely overcome. Methods. The vaccine is comprised of 4 recombinant proteins adsorbed to aluminum hydroxide that contain N-terminal peptides from streptococcal protective antigen and M proteins of 26 common pharyngitis, invasive, and/or rheumatogenic serotypes. Thirty healthy adult subjects received intramuscular 26-valent GAS vaccine (400 μg) at 0, 1, and 4 months, with clinical and laboratory follow-up for safety and immunogenicity using assays for tissue cross-reactive antibodies, type-specific M antibodies to 27 vaccine antigens, and functional (opsonization) activity of M protein antibodies. Results. The incidence of local reactogenicity was similar to that for other aluminum hydroxide-adsorbed vaccines in adults. No subject developed evidence of rheumatogenicity or nephritogenicity, and no induction of human tissue-reactive antibodies was detected. Overall, 26 of 27 antigenic peptides evoked a >4-fold increase in the geometric mean antibody titer over baseline. The mean log₂ fold-increase in serum antibody titer (± standard error of the mean) for all 27 antigens was 3.67 ± 0.21. A significant mean log₂ reduction in streptococcal bacterial counts in serum samples obtained after immunization was seen in opsonization assays for all M serotypes. Conclusions. On the basis of epidemiological data demonstrating that the majority of cases of pharyngitis, necrotizing fasciitis, and other invasive streptococcal infections are caused by a limited number of serotypes, this 26-valent vaccine could have significant impact on the overall burden of streptococcal disease.

Langue d'origine	English
Pages (de-à)	1114-1122
Nombre de pages	9
Journal	Clinical Infectious Diseases
Volume	41
Numéro de publication	8
DOI	https://doi.org/10.1086/444458
Statut de publication	Published - oct. 15 2005

Note bibliographique

Funding Information:
Potential conflicts of interest. S.A.M, S.A.H., J.M.L., B.S., G.P.S., A.W., and D.M.B. are clinical investigators at the Clinical Trials Research Centre at Dalhousie University and received financial support from the sponsor company, ID Biomedical, for the conduct of this trial; none of these investigators received personal compensation and none hold financial interests in the product. M.C.H., S.D.S., L.F.F., P.E.V., J.L., and M.A.R. are employed by the vaccine manufacturer and study sponsor, ID Biomedical, and own stock and/or stock options in ID Biomedical. J.B.D. is the inventor of the vaccine used in this study and receives research support from ID Biomedical; he owns stock and stock options in ID Biomedical and holds existing and pending patents related to the study product. Financial Support. ID Biomedical.

ASJC Scopus Subject Areas

Microbiology (medical)
Infectious Diseases

ODD de l’ONU

Cette action contribue à la réalisation des objectifs de développement durable suivants

Accès au document

10.1086/444458

Autres fichiers et liens

Citer

McNeil, S. A., Halperin, S. A., Langley, J. M., Smith, B., Warren, A., Sharratt, G. P., Baxendale, D. M., Reddish, M. A., Hu, M. C., Stroop, S. D., Linden, J., Fries, L. F., Vink, P. E., & Dale, J. B. (2005). Safety and immunogenicity of 26-valent group A streptococcus vaccine in healthy adult volunteers. Clinical Infectious Diseases, 41(8), 1114-1122. https://doi.org/10.1086/444458

@article{481407ebd69d4d96b44a352f582fa1c9,

title = "Safety and immunogenicity of 26-valent group A streptococcus vaccine in healthy adult volunteers",

abstract = "Background. Group A streptococcus (GAS) causes illness ranging from uncomplicated pharyngitis to life-threatening necrotizing fasciitis, toxic shock, and rheumatic fever. Attempts to develop an M protein-based vaccine have been hindered by the fact that some M proteins elicit both protective antibodies and antibodies that cross-react with human tissues. New molecular techniques have allowed the previous obstacles to be largely overcome. Methods. The vaccine is comprised of 4 recombinant proteins adsorbed to aluminum hydroxide that contain N-terminal peptides from streptococcal protective antigen and M proteins of 26 common pharyngitis, invasive, and/or rheumatogenic serotypes. Thirty healthy adult subjects received intramuscular 26-valent GAS vaccine (400 μg) at 0, 1, and 4 months, with clinical and laboratory follow-up for safety and immunogenicity using assays for tissue cross-reactive antibodies, type-specific M antibodies to 27 vaccine antigens, and functional (opsonization) activity of M protein antibodies. Results. The incidence of local reactogenicity was similar to that for other aluminum hydroxide-adsorbed vaccines in adults. No subject developed evidence of rheumatogenicity or nephritogenicity, and no induction of human tissue-reactive antibodies was detected. Overall, 26 of 27 antigenic peptides evoked a >4-fold increase in the geometric mean antibody titer over baseline. The mean log2 fold-increase in serum antibody titer (± standard error of the mean) for all 27 antigens was 3.67 ± 0.21. A significant mean log2 reduction in streptococcal bacterial counts in serum samples obtained after immunization was seen in opsonization assays for all M serotypes. Conclusions. On the basis of epidemiological data demonstrating that the majority of cases of pharyngitis, necrotizing fasciitis, and other invasive streptococcal infections are caused by a limited number of serotypes, this 26-valent vaccine could have significant impact on the overall burden of streptococcal disease.",

author = "McNeil, {Shelly A.} and Halperin, {Scott A.} and Langley, {Joanne M.} and Bruce Smith and Andrew Warren and Sharratt, {Geoffrey P.} and Baxendale, {Darlene M.} and Reddish, {Mark A.} and Hu, {Mary C.} and Stroop, {Steven D.} and Janine Linden and Fries, {Louis F.} and Vink, {Peter E.} and Dale, {James B.}",

note = "Funding Information: Potential conflicts of interest. S.A.M, S.A.H., J.M.L., B.S., G.P.S., A.W., and D.M.B. are clinical investigators at the Clinical Trials Research Centre at Dalhousie University and received financial support from the sponsor company, ID Biomedical, for the conduct of this trial; none of these investigators received personal compensation and none hold financial interests in the product. M.C.H., S.D.S., L.F.F., P.E.V., J.L., and M.A.R. are employed by the vaccine manufacturer and study sponsor, ID Biomedical, and own stock and/or stock options in ID Biomedical. J.B.D. is the inventor of the vaccine used in this study and receives research support from ID Biomedical; he owns stock and stock options in ID Biomedical and holds existing and pending patents related to the study product. Financial Support. ID Biomedical.",

year = "2005",

month = oct,

day = "15",

doi = "10.1086/444458",

language = "English",

volume = "41",

pages = "1114--1122",

journal = "Clinical Infectious Diseases",

issn = "1058-4838",

publisher = "Oxford University Press",

number = "8",

}

TY - JOUR

T1 - Safety and immunogenicity of 26-valent group A streptococcus vaccine in healthy adult volunteers

AU - McNeil, Shelly A.

AU - Halperin, Scott A.

AU - Langley, Joanne M.

AU - Smith, Bruce

AU - Warren, Andrew

AU - Sharratt, Geoffrey P.

AU - Baxendale, Darlene M.

AU - Reddish, Mark A.

AU - Hu, Mary C.

AU - Stroop, Steven D.

AU - Linden, Janine

AU - Fries, Louis F.

AU - Vink, Peter E.

AU - Dale, James B.

N1 - Funding Information: Potential conflicts of interest. S.A.M, S.A.H., J.M.L., B.S., G.P.S., A.W., and D.M.B. are clinical investigators at the Clinical Trials Research Centre at Dalhousie University and received financial support from the sponsor company, ID Biomedical, for the conduct of this trial; none of these investigators received personal compensation and none hold financial interests in the product. M.C.H., S.D.S., L.F.F., P.E.V., J.L., and M.A.R. are employed by the vaccine manufacturer and study sponsor, ID Biomedical, and own stock and/or stock options in ID Biomedical. J.B.D. is the inventor of the vaccine used in this study and receives research support from ID Biomedical; he owns stock and stock options in ID Biomedical and holds existing and pending patents related to the study product. Financial Support. ID Biomedical.

PY - 2005/10/15

Y1 - 2005/10/15

N2 - Background. Group A streptococcus (GAS) causes illness ranging from uncomplicated pharyngitis to life-threatening necrotizing fasciitis, toxic shock, and rheumatic fever. Attempts to develop an M protein-based vaccine have been hindered by the fact that some M proteins elicit both protective antibodies and antibodies that cross-react with human tissues. New molecular techniques have allowed the previous obstacles to be largely overcome. Methods. The vaccine is comprised of 4 recombinant proteins adsorbed to aluminum hydroxide that contain N-terminal peptides from streptococcal protective antigen and M proteins of 26 common pharyngitis, invasive, and/or rheumatogenic serotypes. Thirty healthy adult subjects received intramuscular 26-valent GAS vaccine (400 μg) at 0, 1, and 4 months, with clinical and laboratory follow-up for safety and immunogenicity using assays for tissue cross-reactive antibodies, type-specific M antibodies to 27 vaccine antigens, and functional (opsonization) activity of M protein antibodies. Results. The incidence of local reactogenicity was similar to that for other aluminum hydroxide-adsorbed vaccines in adults. No subject developed evidence of rheumatogenicity or nephritogenicity, and no induction of human tissue-reactive antibodies was detected. Overall, 26 of 27 antigenic peptides evoked a >4-fold increase in the geometric mean antibody titer over baseline. The mean log2 fold-increase in serum antibody titer (± standard error of the mean) for all 27 antigens was 3.67 ± 0.21. A significant mean log2 reduction in streptococcal bacterial counts in serum samples obtained after immunization was seen in opsonization assays for all M serotypes. Conclusions. On the basis of epidemiological data demonstrating that the majority of cases of pharyngitis, necrotizing fasciitis, and other invasive streptococcal infections are caused by a limited number of serotypes, this 26-valent vaccine could have significant impact on the overall burden of streptococcal disease.

AB - Background. Group A streptococcus (GAS) causes illness ranging from uncomplicated pharyngitis to life-threatening necrotizing fasciitis, toxic shock, and rheumatic fever. Attempts to develop an M protein-based vaccine have been hindered by the fact that some M proteins elicit both protective antibodies and antibodies that cross-react with human tissues. New molecular techniques have allowed the previous obstacles to be largely overcome. Methods. The vaccine is comprised of 4 recombinant proteins adsorbed to aluminum hydroxide that contain N-terminal peptides from streptococcal protective antigen and M proteins of 26 common pharyngitis, invasive, and/or rheumatogenic serotypes. Thirty healthy adult subjects received intramuscular 26-valent GAS vaccine (400 μg) at 0, 1, and 4 months, with clinical and laboratory follow-up for safety and immunogenicity using assays for tissue cross-reactive antibodies, type-specific M antibodies to 27 vaccine antigens, and functional (opsonization) activity of M protein antibodies. Results. The incidence of local reactogenicity was similar to that for other aluminum hydroxide-adsorbed vaccines in adults. No subject developed evidence of rheumatogenicity or nephritogenicity, and no induction of human tissue-reactive antibodies was detected. Overall, 26 of 27 antigenic peptides evoked a >4-fold increase in the geometric mean antibody titer over baseline. The mean log2 fold-increase in serum antibody titer (± standard error of the mean) for all 27 antigens was 3.67 ± 0.21. A significant mean log2 reduction in streptococcal bacterial counts in serum samples obtained after immunization was seen in opsonization assays for all M serotypes. Conclusions. On the basis of epidemiological data demonstrating that the majority of cases of pharyngitis, necrotizing fasciitis, and other invasive streptococcal infections are caused by a limited number of serotypes, this 26-valent vaccine could have significant impact on the overall burden of streptococcal disease.

UR - http://www.scopus.com/inward/record.url?scp=26444487581&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=26444487581&partnerID=8YFLogxK

U2 - 10.1086/444458

DO - 10.1086/444458

M3 - Article

C2 - 16163629

AN - SCOPUS:26444487581

SN - 1058-4838

VL - 41

SP - 1114

EP - 1122

JO - Clinical Infectious Diseases

JF - Clinical Infectious Diseases

IS - 8

ER -

Safety and immunogenicity of 26-valent group A streptococcus vaccine in healthy adult volunteers

Résumé

Note bibliographique

ASJC Scopus Subject Areas

ODD de l’ONU

Accès au document

Autres fichiers et liens

Empreinte numérique

Citer