AI Article Synopsis
- The study aimed to compare the effectiveness of nanoparticles (110 nm) and microparticles (800-900 nm) as vaccine delivery systems using PLG polymers.
- Two different protein antigens were tested: one from Neisseria meningitides type B and one from HIV-1, with varying administration methods for each.
- Results from three studies showed no significant differences in immune responses between the two particle sizes, suggesting both are viable options for vaccine delivery.
Article Abstract
The objective of this work was to conduct an in vivo comparison of nanoparticles and microparticles as vaccine delivery systems. Poly (lactide-co-glycolide) (PLG) polymers were used to create nanoparticles size 110 nm and microparticles of size 800-900 nm. Protein antigens were then adsorbed to these particles. The efficacy of these delivery systems was tested with two protein antigens. A recombinant antigen from Neisseria meningitides type B (MenB) was administered intramuscularly (i.m.) or intraperitonealy (i.p.). An antigen from HIV-1, env glycoprotein gp140 was administered intranasally (i.n.) followed by an i.m. boost. From three studies, there were no differences between the nanoparticles and micro-particles formulations. Both particles led to comparable immune responses in mice. The immune responses for MenB (serum bactericidal activity and antibody titers) were equivalent to the control of aluminum hydroxide. For the gp140, the LTK63 was necessary for high titers. Both nanoparticles and microparticles are promising delivery systems.
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| http://dx.doi.org/10.4161/hv.4.1.4886 | DOI Listing |
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