Intranasal Vaccination with Pneumococcal Surface Protein A and Interleukin-12 Augments Antibody-Mediated Opsonization and Protective Immunity against<i>Streptococcus pneumoniae</i>Infection

Arulanandam, Bernard P.; Lynch, Joyce M.; Briles, David E.; Hollingshead, Susan K.; Metzger, Dennis W.

doi:10.1128/iai.69.11.6718-6724.2001

Cited by 137 publications

(109 citation statements)

References 44 publications

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“…In addition, intranasal vaccination with PspA and IL-12 provided increased protection against nasopharyngeal carriage. The aforementioned results were obtained using a T-dependent pneumococcal protein antigen as the vaccine but, importantly, similar results have been observed using pneumococcal and meningococcal polysaccharide vaccines, given either as T-dependent conjugate vaccines, for example Prevnar ® , or as T-independent nonconjugated vaccines, such as Pneumovax ® [23][24][25]28,32]. In both cases, it was found that IL-12 treatment at the time of immunization induced significantly elevated levels of IgG2a and IgG3 anti-polysaccharide antibodies in serum, as well as IgA and IgG antibodies in the lung.…”

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confidence: 65%

“…For example, upon transfer of sera to naive recipients and intranasal challenge with a lethal dose of S. pneumoniae, all mice that received normal mouse serum succumbed to infection within 5 days, and mice receiving serum from animals vaccinated with pneumococcal surface protein A (PspA) alone showed no significantly increased protection [31]. Strikingly, every mouse that received serum from animals treated with both PspA and IL-12 survived the infection.…”

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confidence: 99%

“…These include infections induced with influenza virus [22], Streptococcus pneumoniae [23][24][25], Francisella tularensis [26] and Yersinia pestis [Kumar D, Metzger DW, Unpublished Data]. We and others have repeatedly found that intranasal treatment of mice with IL-12 leads to increases in expression of both Th1-and Th2-associated antibodies in the serum [9][10][11][12][13][14] as well as in the lung [22][23][24][25][26][27]. In a typical experiment, mice are inoculated intranasally with vaccine only or vaccine plus IL-12.…”

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confidence: 99%

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IL-12 as an adjuvant for the enhancement of protective humoral immunity

Metzger¹

2009

Expert Review of Vaccines

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confidence: 65%

Section: For Reprint Orders Please Contact Reprints@expert-reviewscommentioning

confidence: 99%

Section: For Reprint Orders Please Contact Reprints@expert-reviewscommentioning

confidence: 99%

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IL-12 as an adjuvant for the enhancement of protective humoral immunity

Metzger¹

2009

Expert Review of Vaccines

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“…Proteins are, generally, antigenically conserved across all serotypes and stimulate a T-cell-dependent immune response resulting in more robust immunological memory (28). Several pneumococcal surface proteins have been shown to be effective immunogens and can prevent sepsis, pneumonia, and carriage in animal models (1,2,5,6,23,26).…”

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confidence: 99%

Immunization with Polyamine Transport Protein PotD Protects Mice against Systemic Infection with Streptococcus pneumoniae

Shah

Swiatlo

2006

Infect Immun

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The human pathogen Streptococcus pneumoniae contains genes for a putative polyamine ABC transporter which are organized in an operon and designated potABCD. Polyamine transport protein D (PotD) is an extracellular protein which binds polyamines and possibly other structurally related molecules. PotD has been shown to contribute to virulence in both a murine sepsis model and a pneumonia model with capsular type 3 pneumococci. The protective efficacy of recombinant PotD was evaluated by active immunization and intravenous challenge with capsular type 3 pneumococci in CBA/N mice. Immunized mice had 91.7% survival following lethal pneumococcal challenge, compared with 100% mortality in the control group. Immunized animals had high-titer anti-PotD antibodies following three immunizations with alum. Protection in a sepsis model was also seen after passive administration of rabbit antiserum raised against PotD (P < 0.004). These results suggest that antibodies to PotD confer protection against invasive pneumococcal disease and that this protein should be studied further as a potential vaccine candidate for protection against invasive pneumococcal infections.

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“…24 In addition, co-administration of PspA antigen and IL-12 as a nasal adjuvant enhanced PspA-specific IgG and IgA responses, with increased protection from nasal carriage. 25 In addition, nasal immunization with chitosan–DNA nanoparticles that express PspA elicited protective immunity against nasal colonization by S. pneumoniae . 26 Furthermore, an antigen-delivery method has been developed that targets claudin-4, a major cell-adhesion molecule in tight junctions that is highly expressed on the epithelium of nasopharynx-associated lymphoid tissue.…”

Section: Development Of a Nanogel-based Nasal Vaccine Against Pneumoniamentioning

confidence: 99%

Cationic pullulan nanogel as a safe and effective nasal vaccine delivery system for respiratory infectious diseases

Nakahashi-Ouchida

Yuki

Kiyono

2018

Human Vaccines & Immunotherapeutics

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The mucosal surfaces of the respiratory and gastrointestinal tracts are continuously exposed to countless beneficial and pathologic antigens. These mucosal surfaces are thus equipped with an immune system that is unique from those elsewhere in the body; this unique system provides the first line of immune surveillance and defense against pathogen invasion. The sophisticated immune induction machinery in the aero–digestive tract involves mucosa-associated lymphoid tissues, including nasopharyngeal- and gut-associated lymphoid tissues, for the generation of antigen-specific humoral and cellular immune responses. Consequently, nasal or oral immunization with an appropriate vaccine delivery vehicle prompts the induction of protective immunity in both the mucosal and systemic compartments, leading to a double layer of protection against pathogens. To harness the benefits of mucosal vaccines, various mucosal antigen delivery vehicles are under development, and a cationic cholesteryl-group-bearing pullulan nanogel (cCHP nanogel) has emerged as a potent nasal vaccine delivery system for the induction of protective immunity against respiratory infections.

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Intranasal Vaccination with Pneumococcal Surface Protein A and Interleukin-12 Augments Antibody-Mediated Opsonization and Protective Immunity againstStreptococcus pneumoniaeInfection

Cited by 137 publications

References 44 publications

IL-12 as an adjuvant for the enhancement of protective humoral immunity

IL-12 as an adjuvant for the enhancement of protective humoral immunity

Immunization with Polyamine Transport Protein PotD Protects Mice against Systemic Infection with Streptococcus pneumoniae

Cationic pullulan nanogel as a safe and effective nasal vaccine delivery system for respiratory infectious diseases

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