Mutants of Pertussis Toxin Suitable for Vaccine Development

Pizza, Mariagrazia; Covacci, Antonio; Bartoloni, Antonella; Perugini, María Laura Lupano; Nencioni, L; Magistris, Maria Teresa De; Villa, L; Nucci, Daniele; Manetti, Roberto; Bugnoli, M; Giovannoni, Franco; Olivieri, R.; Barbieri, Joseph T.; Sato, Hiroko; Rappuoli, Rino

doi:10.1126/science.2683073

Cited by 298 publications

(208 citation statements)

References 27 publications

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“…The ADP-ribosyltransferase activity of the recombinant S1 (rPTS1) encoded by pTrcHis2/pts1 and pcDNA3.1/ptS1 was inactivated by two point mutations in which Arg-13 was changed to Leu-13 and Glu-129 was changed to Gly-129 (Pizza et al, 1989). Site-directed mutagenesis was carried out using a QuikChange XL mutagenesis kit (Stratagene) according to the manufacturer's instructions.…”

Section: Methodsmentioning

confidence: 99%

“…Therefore, an important aspect in the development of our DNA vaccine was the inactivation of the S1 gene. Pizza et al (1989) showed that substitution of Glu-129 with Gly-129 in combination with either Arg-9 to Lys-9, Arg-13 to Leu-13 or Trp-26 to Ile-26 abolished the ADP-ribosylase activity but did not adversely affect immunogenicity. Nencioni et al (1990) later characterized the 9K/129G toxoid and showed that it had the same physical and immunological properties as wild-type PT.…”

Section: Introductionmentioning

confidence: 99%

“…Nencioni et al (1990) later characterized the 9K/129G toxoid and showed that it had the same physical and immunological properties as wild-type PT. For this study, we chose the 13L/129G mutation as it is reported to have marginally less leukocytosis-promoting activity and greater T-cell recognition, and mice had a higher survival rate following lethal challenge compared with the 9K/129G toxoid (Pizza et al, 1989).…”

Section: Introductionmentioning

confidence: 99%

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Parenteral immunization of mice with a genetically inactivated pertussis toxin DNA vaccine induces cell-mediated immunity and protection

Fry

Chen

Daggard

et al. 2008

Journal of Medical Microbiology

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The immunogenicity and protective efficacy of a DNA vaccine encoding a genetically inactivated S1 domain of pertussis toxin was evaluated using a murine respiratory challenge model of Bordetella pertussis infection. It was found that mice immunized via the intramuscular route elicited a purely cell-mediated immune response to the DNA vaccine, with high levels of gamma interferon (IFN-c) and interleukin (IL)-2 detected in the S1-stimulated splenocyte supernatants and no serum IgG. Despite the lack of an antibody response, the lungs of DNA-immunized mice were cleared of B. pertussis at a significantly faster rate compared with mock-immunized mice following an aerosol challenge. To gauge the true potential of this S1 DNA vaccine, the immune response and protective efficacy of the commercial diphtheria-tetanus-acellular pertussis (DTaP) vaccine were included as the gold standard. Immunization with DTaP elicited a typically strong T-helper (Th)2-polarized immune response with significantly higher titres of serum IgG than in the DNA vaccine group, but a relatively weak Th1 response with low levels of IFN-c and IL-2 detected in the supernatants of antigen-stimulated splenocytes. DTaP-immunized mice cleared the aerosol challenge more efficiently than DNA-immunized mice, with no detectable pathogen after day 7 post-challenge.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Parenteral immunization of mice with a genetically inactivated pertussis toxin DNA vaccine induces cell-mediated immunity and protection

Fry

Chen

Daggard

et al. 2008

Journal of Medical Microbiology

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“…However, chemical treatment lowers to some extent immunogenicity of PT. In contrast, genetically detoxified PT mutants -including PT-9K/129G, that lacks enzymatic activity -retain the functional and immunological properties of wild-type PT [9]. PT-9K/129G was shown to be safe and immunogenic as a component of a DTaP vaccine evaluated in two large Phase III efficacy trial in infants [10,11].…”

Section: Introductionmentioning

confidence: 99%

Addition of a TLR7 agonist to an acellular pertussis vaccine enhances Th1 and Th17 responses and protective immunity in a mouse model

Misiak

Leuzzi

Allen

et al. 2017

Vaccine

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a b s t r a c tA resurgence of whooping cough (pertussis) has been observed in recent years in a number of developed countries, despite widespread vaccine coverage. Although the exact reasons of the recurrence of pertussis are not clear, there are a number of potential causes, like antigenic variation in the circulating strains of Bordetella pertussis, changes in surveillance and diagnostic tools, and potential differences in protection afforded by current acellular pertussis (aP) vaccines compared to more reactogenic whole cell (wP) vaccines, which they replaced. Studies in animal models have shown that induction of cellular as well as humoral immune responses are key to conferring effective and long lasting protection against B. pertussis. wP vaccines induce robust Th1/Th17 responses, which are associated with good protection against lung infection. In contrast, aP vaccines induce mixed Th2/Th17 responses. One research option is to modify current aP vaccines with the intention of inducing protective T cell responses, without compromising on their low reactogenicity profile. Here we found that formulation of an aP vaccine with a novel adjuvant based on a Toll-like receptor 7 agonist (TLR7a) adsorbed to aluminum hydroxide (alum) enhanced B. pertussis-specific Th1 and Th17 responses and serum IgG2a/b antibodies, which had greater functional capacity than those induced by aP formulated with alum alone. Furthermore, addition of a TLR7a enhanced the protective efficacy of the aP vaccine against B. pertussis aerosol challenge; protection was comparable to that of a wP vaccine. These findings suggest that alum-TLR7a is a promising adjuvant for clinical development of next generation pertussis vaccines.

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“…But this time he and colleague Mariagrazia Pizza used sitedirected mutagenesis to specifically alter amino acids in the active site of the toxin. The result was a nontoxic molecule that made a potent vaccine (4).…”

Section: New Generation Of Vaccinesmentioning

confidence: 99%

Profile of Rino Rappuoli

Trivedi¹

2006

Proc. Natl. Acad. Sci. U.S.A.

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Mutants of Pertussis Toxin Suitable for Vaccine Development

Cited by 298 publications

References 27 publications

Parenteral immunization of mice with a genetically inactivated pertussis toxin DNA vaccine induces cell-mediated immunity and protection

Parenteral immunization of mice with a genetically inactivated pertussis toxin DNA vaccine induces cell-mediated immunity and protection

Addition of a TLR7 agonist to an acellular pertussis vaccine enhances Th1 and Th17 responses and protective immunity in a mouse model

Profile of Rino Rappuoli

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