Anti-Gal constitutes ∼1% of circulating IgG in humans and interacts specifically with α-gal epitopes. We reported previously that expression of α-gal epitopes on HIV gp120 and influenza virus vaccines increases immunogenicity by ∼100-fold. We hypothesize that immunogenicity of any microbial vaccine can be markedly increased by linked α-gal epitopes due to in vivo formation of immune complexes with anti-Gal and the effective internalization of such immune complexes by APC, via Fc/FcγR interaction. The increased transport to lymph nodes and processing of anti-Gal complexed vaccines internalized by APC, results in effective activation of vaccine specific CD4 + and CD8 + T cells, and high cellular and humoral immune response. This universal mechanism for anti-Gal mediated increased immunogenicity is demonstrated in α1,3galactosyltransferase knockout mice with ovalbumin as a model vaccine.