Mucosal Immunization with an Unadjuvanted Vaccine That Targets Streptococcus pneumoniae PspA to Human Fcγ Receptor Type I Protects against Pneumococcal Infection through Complement- and Lactoferrin-Mediated Bactericidal Activity

Bitsaktsis, Constantine; Iglesias, Bibiana V.; Li, Ying; Colino, Jesus; Snapper, Clifford M.; Hollingshead, Susan K.; Pham, Giang; Gosselin, Diane; Gosselin, Edmund J.

doi:10.1128/iai.05511-11

Cited by 33 publications

(43 citation statements)

References 73 publications

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“…This result supports the importance of the complement system in the protection elicited by PspA5-wP. Similarly, a nasal vaccine composed of a hybrid protein that targets PspA to the human Fc␥ receptor type I (anti-hFc␥RI-PspA) induced high levels of anti-PspA antibodies and complement-dependent protection against a challenge with a serotype 3 pneumococcal strain in transgenic mice expressing hFc␥RI (40).…”

Section: Discussionsupporting

confidence: 59%

“…Cobra venom factor (CVF) from Naja naja kaouthia (Quidel Corporation, Darmstadt, Germany) was used for the depletion of complement in vivo, as described previously (40,41), and depletion was confirmed by the absence of rabbit erythrocyte hemolytic activity in the sera of mice treated with CVF (41). BALB/c mice (14 animals) were immunized with the PspA5-wP formulation using the sixdose schedule.…”

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confidence: 99%

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Pertussis Toxin Improves Immune Responses to a Combined Pneumococcal Antigen and Leads to Enhanced Protection against Streptococcus pneumoniae

Salcedo-Rivillas

Debrie

Miyaji

et al. 2014

Clin. Vaccine Immunol.

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Pneumococcal surface protein A (PspA) is a candidate antigen for the composition of protein-based vaccines against Streptococcus pneumoniae. While searching for efficient adjuvants for PspA-based vaccines, our group has described the potential of combining PspA with the whole-cell pertussis vaccine (wP). When given to mice through the nasal route, a formulation composed of PspA from clade 5 (PspA5) and wP (PspA5-wP) induced high levels of antibodies and protection against challenges with different pneumococcal strains. PspA5-wP also induced the secretion of interleukin 17 (IL-17) by splenocytes and the infiltration of leukocytes in the lungs after challenge. Here, we show that protection against a pneumococcal invasive challenge was completely abrogated in MT ؊/؊ mice, which are deficient in the maturation of B cells, illustrating the importance of antibodies in the survival elicited by the PspA5-wP vaccine. Moreover, passive immunization showed that IgG purified from the sera of mice immunized with PspA5-wP conferred significant protection to naive mice, whereas the respective F(ab=) 2 did not. Additionally, in vivo depletion of complement abolished protection against the pneumococcal challenge. The combination of PspA5 with wild-type or mutant Bordetella pertussis strains or with purified components showed that the pertussis toxin (PT)-containing formulations induced the highest levels of antibodies and protection. This suggests that the adjuvant activity of wP in the PspA5 model is mediated at least in part by PT. The sera from mice immunized with such formulations displayed high IgG binding and induction of complement deposition on the pneumococcal surface in vitro, which is consistent with the in vivo results.

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Section: Discussionsupporting

confidence: 59%

mentioning

confidence: 99%

Pertussis Toxin Improves Immune Responses to a Combined Pneumococcal Antigen and Leads to Enhanced Protection against Streptococcus pneumoniae

Salcedo-Rivillas

Debrie

Miyaji

et al. 2014

Clin. Vaccine Immunol.

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“…These properties of PspA make it likely that the mediation of phagocytosis in vivo is a major protective mechanism of immunity to PspA. Antibodies to PspA also enhance the killing of pneumococci by the antibacterial peptides of apolactoferrin (22,37).…”

mentioning

confidence: 99%

Modified Opsonization, Phagocytosis, and Killing Assays To Measure Potentially Protective Antibodies against Pneumococcal Surface Protein A

Daniels¹,

Kim²,

Burton³

et al. 2013

Clin. Vaccine Immunol.

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eThe standard opsonophagocytosis killing assay (OPKA) for antibodies to pneumococcal capsular polysaccharide was modified to permit an evaluation of the protection-mediating antibodies to pneumococcal surface protein A (PspA). We found that by increasing the incubation time with the complement and phagocytes from 45 min to 75 min, the protective activity was readily detected. In another modification, we used a capsule type 2 target strain that expressed PspA but not pneumococcal surface protein C (PspC). With these modifications separately or in combination, rabbit antisera to the recombinant ␣-helical or prolinerich domains of PspA mediated >50% killing of the target strain. The ability of normal human sera to mediate the killing of pneumococci in this modified OPKA correlated with their levels of antibodies to PspA and their ability to protect mice against fatal infection with a type 3 strain. Passive protection of mice against pneumococci and killing in the modified OPKA were lost when normal human sera were adsorbed with recombinant PspA (rPspA) on Sepharose, thus supporting the potential utility of the modified OPKA to detect protective antibodies to PspA. In the standard OPKA, monoclonal antibodies to PspA were strongly protective in the presence of subprotective amounts of anti-capsule. Thus, the currently established high-throughput OPKA for antibodies to capsule could be modified in one of two ways to permit an evaluation of the opsonic efficacy of antibodies to PspA.

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“…Broad-coverage vaccines based on PspA would thus depend on the use of more than one molecule or on the choice of specific PspA molecules (37). In animal models, protection elicited by vaccines composed of PspA is often accompanied by the induction of high levels of specific antibodies (10,22,24,44) which, upon binding to pneumococcal surface, promote the deposition of complement (9,12,47,57) and enhance killing by lactoferrin (9,48). In addition, the use of adjuvants that elicit Th1 immune responses against PspA seems to optimize protection (4,19,20).…”

mentioning

confidence: 99%

Controlled Inflammatory Responses in the Lungs Are Associated with Protection Elicited by a Pneumococcal Surface Protein A-Based Vaccine against a Lethal Respiratory Challenge with Streptococcus pneumoniae in Mice

Lima

Ferreira

Moreno

et al. 2012

Clin Vaccine Immunol

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Streptococcus pneumoniae is a pathogen of great importance worldwide. We have previously described the efficacy of a nasal vaccine composed of the pneumococcal surface protein A and the whole-cell pertussis vaccine as an adjuvant against a pneumococcal invasive challenge in mice. Spread of bacteria to the bloodstream was probably prevented by the high levels of systemic antibodies induced by the vaccine, but bacteria were only cleared from the lungs 3 weeks later, indicating that local immune responses may contribute to survival. Here we show that a strict control of inflammatory responses in lungs of vaccinated mice occurs even in the presence of high numbers of pneumococci. This response was characterized by a sharp peak of neutrophils and lymphocytes with a simultaneous decrease in macrophages in the respiratory mucosa at 12 h postchallenge. Secretion of interleukin-6 (IL-6) and gamma interferon (IFN-␥) was reduced at 24 h postchallenge, and the induction of tumor necrosis factor alpha (TNF-␣) secretion, observed in the first hours postchallenge, was completely abolished at 24 h. Before challenge and at 12 h postchallenge, vaccinated mice displayed higher numbers of CD4 ؉ T, CD8 ؉ T, and B lymphocytes in the lungs. However, protection still occurs in the absence of each of these cells during the challenge, indicating that other effectors may be related to the prevention of lung injuries in this model. High levels of mucosal anti-PspA antibodies were maintained in vaccinated mice during the challenge, suggesting an important role in protection.

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Mucosal Immunization with an Unadjuvanted Vaccine That Targets Streptococcus pneumoniae PspA to Human Fcγ Receptor Type I Protects against Pneumococcal Infection through Complement- and Lactoferrin-Mediated Bactericidal Activity

Cited by 33 publications

References 73 publications

Pertussis Toxin Improves Immune Responses to a Combined Pneumococcal Antigen and Leads to Enhanced Protection against Streptococcus pneumoniae

Pertussis Toxin Improves Immune Responses to a Combined Pneumococcal Antigen and Leads to Enhanced Protection against Streptococcus pneumoniae

Modified Opsonization, Phagocytosis, and Killing Assays To Measure Potentially Protective Antibodies against Pneumococcal Surface Protein A

Controlled Inflammatory Responses in the Lungs Are Associated with Protection Elicited by a Pneumococcal Surface Protein A-Based Vaccine against a Lethal Respiratory Challenge with Streptococcus pneumoniae in Mice

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