Literature DB >> 15845509

The vaccine candidate Vibrio cholerae 638 is protective against cholera in healthy volunteers.

Luis García1, Manuel Díaz Jidy, Hilda García, Boris L Rodríguez, Roberto Fernández, Gemma Año, Bárbara Cedré, Tania Valmaseda, Edith Suzarte, Margarita Ramírez, Yadira Pino, Javier Campos, Jorge Menéndez, Rodrigo Valera, Daniel González, Irma González, Oliver Pérez, Teresita Serrano, Miriam Lastre, Fernando Miralles, Judith Del Campo, Jorge Luis Maestre, José Luis Pérez, Arturo Talavera, Antonio Pérez, Karen Marrero, Talena Ledón, Rafael Fando.   

Abstract

Vibrio cholerae 638 is a living candidate cholera vaccine strain attenuated by deletion of the CTXPhi prophage from C7258 (O1, El Tor Ogawa) and by insertion of the Clostridium thermocellum endoglucanase A gene into the hemagglutinin/protease coding sequence. This vaccine candidate was previously found to be well tolerated and immunogenic in volunteers. This article reports a randomized, double-blind, placebo-controlled trial conducted to test short-term protection conferred by 638 against subsequent V. cholerae infection and disease in volunteers in Cuba. A total of 45 subjects were enrolled and assigned to receive vaccine or placebo. The vaccine contained 10(9) CFU of freshly harvested 638 buffered with 1.3% NaHCO(3), while the placebo was buffer alone. After vaccine but not after placebo intake, 96% of volunteers had at least a fourfold increase in vibriocidal antibody titers, and 50% showed a doubling of at least the lipopolysaccharide-specific immunoglobulin A titers in serum. At 1 month after vaccination, five volunteers from the vaccine group and five from the placebo group underwent an exploratory challenge study with 10(9) CFU of DeltaCTXPhi attenuated mutant strain V. cholerae 81. Only two volunteers from the vaccine group shed strain 81 in their feces, but none of them experienced diarrhea; in the placebo group, all volunteers excreted the challenge strain, and three had reactogenic diarrhea. An additional 12 vaccinees and 9 placebo recipients underwent challenge with 7 x 10(5) CFU of virulent strain V. cholerae 3008 freshly harvested from a brain heart infusion agar plate and buffered with 1.3% NaHCO(3). Three volunteers (25%) from the vaccine group and all from the placebo group shed the challenge agent in their feces. None of the 12 vaccinees but 7 volunteers from the placebo group had diarrhea, and 2 of the latter exhibited severe cholera (>5,000 g of diarrheal stool). These results indicate that at 1 month after ingestion of a single oral dose (10(9) CFU) of strain 638, volunteers remained protected against cholera infection and disease provoked by the wild-type challenge agent V. cholerae 3008. We recommend that additional vaccine lots of 638 be prepared under good manufacturing practices for further evaluation.

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Year:  2005        PMID: 15845509      PMCID: PMC1087340          DOI: 10.1128/IAI.73.5.3018-3024.2005

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


  22 in total

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  24 in total

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2.  Hemolysin and the multifunctional autoprocessing RTX toxin are virulence factors during intestinal infection of mice with Vibrio cholerae El Tor O1 strains.

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Review 3.  Enteric infections, diarrhea, and their impact on function and development.

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4.  Attenuation of bacterial virulence by quorum sensing-regulated lysis.

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5.  Insights from natural infection-derived immunity to cholera instruct vaccine efforts.

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Review 6.  The potential for a controlled human infection platform in Singapore.

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Review 8.  Vibrio cholerae hemagglutinin(HA)/protease: An extracellular metalloprotease with multiple pathogenic activities.

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