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Literature DB >> 9284163

Evaluation of a bivalent (CVD 103-HgR/CVD 111) live oral cholera vaccine in adult volunteers from the United States and Peru.

D N Taylor¹, C O Tacket, G Losonsky, O Castro, J Gutierrez, R Meza, J P Nataro, J B Kaper, S S Wasserman, R Edelman, M M Levine, S J Cryz.

Abstract

To provide optimum protection against classical and El Tor biotypes of Vibrio cholerae O1, a single-dose, oral cholera vaccine was developed by combining two live, attenuated vaccine strains, CVD 103-HgR (classical, Inaba) and CVD 111 (El Tor, Ogawa). The vaccines were formulated in a double-chamber sachet; one chamber contained lyophilized bacteria, and the other contained buffer. In the first study, 23 U.S. adult volunteers received CVD 103-HgR at 10(8) CFU plus CVD 111 at 10(8), 10(7), or 10(6) CFU, CVD 111 alone at 10(7) CFU, or placebo. In the second study, 275 Peruvian adults were randomized to receive CVD 103-HgR at 10(9) CFU plus CVD 111 at 10(9) or 10(8) CFU, CVD 111 alone at 10(9) CFU, CVD 103-HgR alone at 10(9) CFU, or placebo. Three of 15 U.S. volunteers who received CVD 111 at 10(7) or 10(8) CFU developed mild diarrhea, compared to none of 4 who received CVD 111 at 10(6) CFU and 1 of 4 who received placebo. Twelve (63%) of 19 vaccine recipients shed the El Tor vaccine strain. All but one volunteer developed significant Ogawa and Inaba vibriocidal antibody titers. Volunteers who received CVD 111 at 10(7) CFU had geometric mean Ogawa titers four to five times higher than those of volunteers who received the lower dose. In the second study, all dosage regimens were well tolerated in Peruvians. About 20% of volunteers who received CVD 111 at the high dose excreted the El Tor organism, compared to 7% in the low-dose group. CVD 111 was detected in the stools of two placebo recipients, neither of whom had symptoms or seroconverted. In all vaccine groups, 69 to 76% developed fourfold rises in Inaba vibriocidal antibodies. Among those who received the bivalent vaccine, 53 to 75% also developed significant rises in Ogawa vibriocidal antibodies. We conclude that it is feasible to produce a single-dose, oral bivalent vaccine that is safe and immunogenic against both biotypes (El Tor and classical) and both serotypes (Inaba and Ogawa) of cholera for populations in both developed and developing parts of the world.

RCT Entities: Population Interventions Outcomes

Entities: Disease Species

Mesh：

Substances：

Year: 1997 PMID： 9284163 PMCID： PMC175550 DOI： 10.1128/iai.65.9.3852-3856.1997

Source DB: PubMed Journal: Infect Immun ISSN： 0019-9567 Impact factor: 3.441

19 in total

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16 in total

1. Expanded safety and immunogenicity of a bivalent, oral, attenuated cholera vaccine, CVD 103-HgR plus CVD 111, in United States military personnel stationed in Panama.

Authors: D N Taylor; J L Sanchez; J M Castro; C Lebron; C M Parrado; D E Johnson; C O Tacket; G A Losonsky; S S Wasserman; M M Levine; S J Cryz
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Journal: Infect Immun Date: 2005-08 Impact factor: 3.441

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Journal: Vaccine (Auckl) Date: 2011-10

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8. Quantitative PCR for detection of Shigella improves ascertainment of Shigella burden in children with moderate-to-severe diarrhea in low-income countries.

Authors: Brianna Lindsay; John B Ochieng; Usman N Ikumapayi; Aliou Toure; Dilruba Ahmed; Shan Li; Sandra Panchalingam; Myron M Levine; Karen Kotloff; David A Rasko; Carolyn R Morris; Jane Juma; Barry S Fields; Michel Dione; Dramane Malle; Stephen M Becker; Eric R Houpt; James P Nataro; Halvor Sommerfelt; Mihai Pop; Joe Oundo; Martin Antonio; Anowar Hossain; Boubou Tamboura; O Colin Stine
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Journal: Scand J Infect Dis Date: 2010