Citations to this article

Immune response to type III group B streptococcal polysaccharide-tetanus toxoid conjugate vaccine.
D L Kasper, … , H J Jennings, C J Baker
D L Kasper, … , H J Jennings, C J Baker
Published November 15, 1996
Citation Information: J Clin Invest. 1996;98(10):2308-2314. https://doi.org/10.1172/JCI119042.
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Immune response to type III group B streptococcal polysaccharide-tetanus toxoid conjugate vaccine.

Abstract

Group B Streptococcus (GBS) is an important perinatal pathogen. Because transplacentally acquired maternal antibodies to the GBS capsular polysaccharides (CPS) confer protection, prevention of infant disease may be possible after immunization of women. Unfortunately, the purified CPS of GBS are only variably immunogenic in adults; therefore to enhance immunogenicity we have designed and developed a CPS-protein conjugate vaccine. The lability of a conformationally dependent epitope on the III CPS containing a critical sialic acid residue was important to consider in vaccine design. 100 women were randomized to receive GBS type III CPS-tetanus toxoid conjugate (III-TT) vaccine at one of three doses; unconjugated GBS type III CPS; or saline. Serum samples were obtained before immunization and 2, 4, 8, and 26 wk thereafter, and specific antibody to type III CPS was measured. Vaccines were well tolerated. In sera from recipients of the highest dose of III-TT, CPS-specific IgG levels rose from a geometric mean of 0.09 microg/ml before immunization to 4.53 microg/ml 8 wk later, whereas levels in recipients of unconjugated type III CPS rose from 0.21 microg/ml to 1.41 microg/ml. Lower doses resulted in lower antibody levels. A > or = 4-fold rise in antibody concentration was achieved in 90% of recipients of III-TT compared with 50% of those that received III CPS (P = 0.0015). Antibodies evoked by the conjugate vaccine recognized a conformationally dependent epitope of the III-CPS, promoted opsonophagocytosis and killing of GBS, and, after maternal immunization, protected neonatal mice from lethal challenge with type III GBS. We conclude that directed coupling of type III GBS polysaccharide to a carrier protein yielded a conjugate vaccine with preserved expression of a highly labile conformational epitope involving sialic acid and enhanced immunogenicity compared with uncoupled CPS.

Authors

D L Kasper, L C Paoletti, M R Wessels, H K Guttormsen, V J Carey, H J Jennings, C J Baker

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Citations to this article in year 1999 (12)

Title and authors Publication Year
Neonatal group B streptococcal disease in Finland: a ten-year nationwide study
S Kalliola, J Vuopio-Varkila, AK Takala, J Eskola 		The Pediatric Infectious Disease Journal 1999
Cognate stimulatory B-cell-T-cell interactions are critical for T-cell help recruited by glycoconjugate vaccines
HK Guttormsen, AH Sharpe, AK Chandraker, AK Brigtsen, MH Sayegh, DL Kasper 		Infection and immunity 1999
Measurement of human antibodies to type III group B Streptococcus
DL Kasper, MR Wessels, HK Guttormsen, LC Paoletti, MS Edwards, CJ Baker 		Infection and immunity 1999
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J Tomašić, B Špoljar, Ð Ljevaković, CP Glaudemans 		Preparative Biochemistry & Biotechnology 1999
Ozonolytic depolymerization of polysaccharides in aqueous solution
Y Wang, RI Hollingsworth, DL Kasper 		Carbohydrate Research 1999
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M Fernandez, CJ Baker 		Seminars in Pediatric Infectious Diseases 1999
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DL Kasper, MR Wessels, HK Guttormsen, LC Paoletti, MS Edwards, CJ Baker 		Infection and immunity 1999
Alpha C Protein as a Carrier for Type III Capsular Polysaccharide and as a Protective Protein in Group B Streptococcal Vaccines
VA Fischetti, C Gravekamp, DL Kasper, LC Paoletti, LC Madoff 		Infection and immunity 1999
Lmb, a Protein with Similarities to the LraI Adhesin Family, Mediates Attachment of Streptococcus agalactiae to Human Laminin
EI Tuomanen, B Spellerberg, E Rozdzinski, S Martin, J Weber-Heynemann, N Schnitzler, R Lütticken, A Podbielski 		Infection and immunity 1999
The preparation of neoglycoconjugates containing inter-saccharide phosphodiester linkages as potential anti-Leishmania vaccines
F H Routier, A V Nikolaev, M A Ferguson 		Glycoconjugate Journal 1999

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