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Abstract
Proteoliposomes purified from the Outer Membrane of Neisseria meningitidis B, have been successfully used as core for adjuvants and vaccine formulations. We have tried to increase their structural definition and to conserve their efficacy and stability avoiding the addition of the aluminum hydroxide to the final formulation. Liposomal particle systems were prepared from components of defined molecular structure, such as a Neisseria meningitidis B protein complex, extracted and purified without forming vesicle structures. Liposomes were prepared from a mixture of dioleoyl phosphatidyl serine and cholesterol, using the classical dehydration-rehydration method. Transmission Electron Microscopy (TEM) was used to characterize the liposomes. BALB/c mice were used for animal testing procedures. Analysis of specific IgG response, serum bactericidal activity as well as DTH reaction was carried out. Isolation and purification of mRNA and real-time PCR, was performed to determine the dominating Th lymphokine pattern. The new antimeningococcal formulation without aluminum hydroxide prepared with components of defined molecular structure assembled itself into Neoproteoliposomes (NPL) ranging from 50 to 70 nm in diameter. The extraction and purification of selected membrane proteins to provide the antigen for this new formulation (PD-Tp), as well as the NPL-formulation favors a Th1 response pattern, suggested by the higher percentages of DTH, increased expression of proinflamatory lymphokine mRNAs when administered by intramuscular and intranasal routes. It stimulates a systemic bactericidal antibody response against Neisseria meningitidis B and immunologic memory similar to the Cuban VA-MENGOC-BC® vaccine, even at lower dosages and is less reactogenic at the injection site in comparison with the formulation with aluminum hydroxide. This new adjuvant formulation could be applicable to the development of new and improved vaccines against meningococcal disease, and eventually as modulators of the immune response against other diseases.
Highlights
Production of serogroup B N. meningitidis membrane proteins into vesicles or proteoliposomes (PL) and their use as the main antigenic component in the Cuban meningococcal vaccine VA-MENGOC-BC®, has been one of the most adjuvanted twice: by the proteoliposomal conformation adopted by membrane proteins and by aluminum hydroxide gel
The aim of the present study was to investigate the immune response and local reactogenicity induced in BALB/c mice, immunized with an adjuvant formulation prepared from components of the N. meningitides B with defined molecular structure, which are assembled in the form of proteoliposomes, without adding aluminum hydroxide gel
Material and methods Liposomal particle systems were prepared from a Neisseria meningitidis B protein complex, extracted and purified without forming vesicle structures (PD) and assembled in the form of proteoliposomal nanoparticles designated as NPL
Summary
Production of serogroup B N. meningitidis membrane proteins into vesicles or proteoliposomes (PL) and their use as the main antigenic component in the Cuban meningococcal vaccine VA-MENGOC-BC®, has been one of the most adjuvanted twice: by the proteoliposomal conformation adopted by membrane proteins and by aluminum hydroxide gel. Different adjuvants, based on nanoparticle systems, have been developed to release antigens in subunit vaccines. It is necessary to increase molecular definition preserving efficiency and stability, without adding aluminum hydroxide to the final formulation, reducing reactogenicity [6]. The aim of the present study was to investigate the immune response and local reactogenicity induced in BALB/c mice, immunized with an adjuvant formulation prepared from components of the N. meningitides B with defined molecular structure, which are assembled in the form of proteoliposomes, without adding aluminum hydroxide gel
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