2012]. Strategies to improve influenza vaccine efficacy in older individuals are needed. Thus, Carroll and colleagues determined whether CLDC (JVRS-100) could improve the efficacy of the influenza purchase vaccine Fluzone (Sanofi Pasteur, Lyon, France) in older rhesus macaques. Vaccination with Fluzone with or without CLDC and challenge with human H1N1 influenza virus showed that only the Fluzone/CLDC-vaccinated animals had lower virus replication. Thus, CLDC enhances immunogenicity and efficacy of a licensed
vaccine in immunosenescent monkeys [Lay et al. 2009; Carroll et al. 2014]. CLDC (JVRS-100) was also evaluated as adjuvant for HBsAg in mice expressing hepatitis B virus (HBV). HBsAg+JVRS-100 elicited T- and B-cell responses, whereas HBsAg elicited only a B-cell response. However, the response by HBsAg+JVRS-100 was not sufficient
to cause destruction of infected liver cells, but it suppressed HBV DNA noncytolytically [Morrey et al. 2011]. Similar results were obtained using the woodchuck model of HBV. HBV infection induced T-cell responses to Woodchuck hepatitis surface antigen (WHsAg) and selected WH peptides and expression of CD8+ CTL and TH1 cytokines. WHsAg plus CLDCs elicited antibodies earlier, in more woodchucks and with higher titers than WHsAg and alum [Cote et al. 2009]. There is a need for mucosal vaccines for pulmonary Yersinia pestis infections. The ability of an oral CLDC-adjuvanted vaccine against lethal pneumonic plague was investigated by Jones and colleagues.
Oral immunization with Y. pestis F1 antigen combined with CLDC produced high titers of anti-F1 antibodies and long-lasting CD4+ T-cell-dependent protection from lethal pulmonary challenge with Y. pestis [Jones et al. 2010]. Other cationic lipid complexes Several other cationic lipid adjuvant complexes were evaluated in various vaccine models. Phillips and colleagues tested an alphavirus vaccine composed of cationic lipid nucleic acid complexes (CLNCs) and the ectodomain (E1ecto) of WEEV. Interestingly, CLNC alone had therapeutic efficacy, as it increased survival of mice following lethal WEEV infection. Immunization with the CLNC/WEEV/E1ecto mixture provided full protection after challenge. Passive serum transfer from immunized to naïve mice conferred protection to challenge, indicating that antibody is sufficient for protection Carfilzomib [Phillips et al. 2014]. Liposomes containing different cationic compounds and neutral DPPC were loaded with influenza HA by adsorption. DC-chol/DPPC liposomes with a high amount of DC-chol had stronger immunogenicity compared with less DC-chol and elicited higher antibody titers compared with the other compounds and nonadjuvanted HA. Liposome-adsorbed HA was more immunogenic than encapsulated HA and incorporation of cholesterol in DC-chol liposomes as well as CpGs enhanced adjuvancy [Barnier-Quer et al. 2013].