Xuan‐Mao Li scite author profile

Polyactide-co-glycolide microparticles, with an entrapped branched octameric peptide from human immunodeficiency virus (HIV-1), were prepared by a solvent evaporation method. The microparticles were characterized for size distribution, antigen loading level, and integrity. Mice in one group were each immunized with a single dose of a controlled-release microparticle formulation containing 300 micrograms of peptide and the serum IgG responses to the antigen were compared with those of mice from a second group that were immunized at 0, 4, and 26 weeks with 100-microgram doses of the same peptide immunogen adsorbed to alum. The controlled-release microparticles induced an antibody response comparable to that from the alum-immunized group. The subcutaneous and the intramuscular routes of administration were compared in additional groups of mice for the microparticles, and both routes induced similar responses. A suspending vehicle for the microparticles was also evaluated and did not affect the immunogenicity of the controlled-release formulation containing both small and large microparticles, although the immunogenicity of smaller microparticles immunized alone was affected.

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CTL induction using synthetic peptides delivered in emulsions— critical role of the formulation procedure

Singh

Hioe

Qiu

et al. 1997

Vaccine

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Xuan‐Mao Li

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Biodegradable Microparticles with an Entrapped Branched Octameric Peptide as a Controlled-Release HIV-1 Vaccine

CTL induction using synthetic peptides delivered in emulsions— critical role of the formulation procedure

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