Mechanism of Protection Induced by Group A Streptococcus Vaccine Candidate J8-DT: Contribution of B and T-Cells Towards Protection

Pandey, Manisha; Batzloff, Michael R.; Good, Michael F.

doi:10.1371/journal.pone.0005147

Cited by 43 publications

(84 citation statements)

References 23 publications

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“…High-pressure liquid chromatography with mass spectrometry controlled fraction collection (LCMS; Shimadzu Corp.) utilizing a reversed-phase C8 column (Waters) with a gradient of acetonitrile in Milli-Q water containing 0.1% formic acid was employed to purify J8 peptide. For J8 peptide amphiphiles, the hydrophobic moiety dipalmitoylglutamic acid (diC 16 ) was synthesized by a previously established method (34). J8 peptide was synthesized similarly to above except the C-terminal lysine was protected with DDE instead of Boc which was used for the other lysines.…”

Section: Peptide and Peptide Amphiphile Synthesismentioning

confidence: 99%

“…J8 peptide was synthesized similarly to above except the C-terminal lysine was protected with DDE instead of Boc which was used for the other lysines. The peptide was treated with 2% hydrazine in DMF to orthogonally deprotect the Cterminal lysine amine group which was covalently coupled to diC 16 by an amidation reaction yielding J8-diC 16 peptide amphiphiles. J8-diC 16 was further processed and purified by the same methods as the J8 peptide.…”

Section: Peptide and Peptide Amphiphile Synthesismentioning

confidence: 99%

“…To fabricate micelles, J8-diC 16 peptide amphiphiles were film cast by dissolving them in methanol and evaporating the solvent using nitrogen as a drying gas. Hydration of the films with water or phosphate-buffered saline (PBS) followed by thorough vortexing induced spontaneous micelle formation.…”

Section: Micelle Formation and Characterizationmentioning

confidence: 99%

“…J8-diC 16 micelles were characterized by previously defined methodologies (33,35,36) including critical micelle concentration (CMC) analysis, transmission electron microscopy (TEM), and circular dichroism (CD). CMC was measured by fluorescent sequestration where varying concentrations of J8-diC 16 were exposed to 1 mM 1,6-diphenyl-1,3,5-hexatriene (DPH) which greatly increases in fluorescence intensity when trapped within the micelle core. Solutions were prepared and allowed to equilibrate for 1 h prior to fluorescent measurement utilizing a TECAN Infinite M200 plate reader (ex.…”

Section: Micelle Formation and Characterizationmentioning

confidence: 99%

“…To enhance the corresponding host immune response, peptide vaccines are often delivered by aid of a delivery vehicle or with immune boosting substances termed adjuvants. While promising experiments have been published that employ J8 peptide delivery vehicles (14,15) or adjuvanted J8 peptide (10,16), this research has yet to lead to a commercially viable GAS vaccine, so novel systems need to be explored. An effective construct should concentrate the peptide antigen, protect it from degradation, enhance its cellular uptake, and adjuvant its immunogenicity in order to induce a robust immune response (17,18).…”

Section: Introductionmentioning

confidence: 99%

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Peptide Amphiphile Micelles Self-Adjuvant Group A Streptococcal Vaccination

Trent

Ulery

Black

et al. 2014

AAPS J

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Abstract. Delivery system design and adjuvant development are crucially important areas of research for improving vaccines. Peptide amphiphile micelles are a class of biomaterials that have the unique potential to function as both vaccine delivery vehicles and self-adjuvants. In this study, peptide amphiphiles comprised of a group A streptococcus B cell antigen (J8) and a dialkyl hydrophobic moiety (diC 16 ) were synthesized and organized into self-assembled micelles, driven by hydrophobic interactions among the alkyl tails. J8-diC 16 formed cylindrical micelles with highly α-helical peptide presented on their surfaces. Both the micelle length and secondary structure were shown to be enhanced by annealing. When injected into mice, J8-diC 16 micelles induced a strong IgG1 antibody response that was comparable to soluble J8 peptide supplemented with two classical adjuvants. It was discovered that micelle adjuvanticity requires the antigen be a part of the micelle since separation of J8 and the micelle was insufficient to induce an immune response. Additionally, the diC 16 tail appears to be non-immunogenic since it does not stimulate a pathogen recognition receptor whose agonist (Pam 3 Cys) possesses a very similar chemical structure. The research presented in this paper demonstrates the promise peptide amphiphile micelles have in improving the field of vaccine engineering.

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Section: Peptide and Peptide Amphiphile Synthesismentioning

confidence: 99%

Section: Peptide and Peptide Amphiphile Synthesismentioning

confidence: 99%

Section: Micelle Formation and Characterizationmentioning

confidence: 99%

Section: Micelle Formation and Characterizationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Peptide Amphiphile Micelles Self-Adjuvant Group A Streptococcal Vaccination

Trent

Ulery

Black

et al. 2014

AAPS J

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Microbially synthesized modular virus‐like particles and capsomeres displaying group A streptococcus hypervariable antigenic determinants

Chuan

Wibowo

Connors

et al. 2013

Biotech & Bioengineering

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Effective and low-cost vaccines are essential to control severe group A streptococcus (GAS) infections prevalent in low-income nations and the Australian aboriginal communities. Highly diverse and endemic circulating GAS strains mandate broad-coverage and customized vaccines. This study describes an approach to deliver cross-reactive antigens from endemic GAS strains using modular virus-like particle (VLP) and capsomere systems. The antigens studied were three heterologous N-terminal peptides (GAS1, GAS2, and GAS3) from the GAS surface M-protein that are specific to endemic strains in Australia Northern Territory Aboriginal communities. In vivo data presented here demonstrated salient characteristics of the modular delivery systems in the context of GAS vaccine design. First, the antigenic peptides, when delivered by unadjuvanted modular VLPs or adjuvanted capsomeres, induced high titers of peptide-specific IgG antibodies (over 1 × 10(4) ). Second, delivery by capsomere was superior to VLP for one of the peptides investigated (GAS3), demonstrating that the delivery system relative effectiveness was antigen-dependant. Third, significant cross-reactivity of GAS2-induced IgG with GAS1 was observed using either VLP or capsomere, showing the possibility of broad-coverage vaccine design using these delivery systems and cross-reactive antigens. Fourth, a formulation containing three pre-mixed modular VLPs, each at a low dose of 5 μg (corresponding to <600 ng of each GAS peptide), induced significant titers of IgGs specific to each peptide, demonstrating that a multivalent, broad-coverage VLP vaccine formulation was possible. In summary, the modular VLPs and capsomeres reported here demonstrate, with promising preliminary data, innovative ways to design GAS vaccines using VLP and capsomere delivery systems amenable to microbial synthesis, potentially adoptable by developing countries.

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Group A Streptococcal Vaccine Candidates: Potential for the Development of a Human Vaccine

Henningham

Gillen

Walker

2012

Host-Pathogen Interactions in Streptococcal Diseases

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Currently there is no commercial Group A Streptococcus (GAS; S. pyogenes) vaccine available. The development of safe GAS vaccines is challenging, researchers are confronted with obstacles such as the occurrence of many unique serotypes (there are greater than 150 M types), antigenic variation within the same serotype, large variations in the geographical distribution of serotypes, and the production of antibodies cross-reactive with human tissue which can lead to host auto-immune disease. Cell wall anchored, cell membrane associated, secreted and anchorless proteins have all been targeted as GAS vaccine candidates. As GAS is an exclusively human pathogen, the quest for an efficacious vaccine is further complicated by the lack of an animal model which mimics human disease and can be consistently and reproducibly colonized by multiple GAS strains.

show abstract

Mechanism of Protection Induced by Group A Streptococcus Vaccine Candidate J8-DT: Contribution of B and T-Cells Towards Protection

Cited by 43 publications

References 23 publications

Peptide Amphiphile Micelles Self-Adjuvant Group A Streptococcal Vaccination

Peptide Amphiphile Micelles Self-Adjuvant Group A Streptococcal Vaccination

Microbially synthesized modular virus‐like particles and capsomeres displaying group A streptococcus hypervariable antigenic determinants

Group A Streptococcal Vaccine Candidates: Potential for the Development of a Human Vaccine

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