| Literature DB >> 33322574 |
Lu Lu1, Carol Ho-Yan Fong1, Anna Jinxia Zhang1, Wai-Lan Wu1, Iris Can Li1, Andrew Chak-Yiu Lee1, Thrimendra Kaushika Dissanayake1, Linlei Chen1, Ivan Fan-Ngai Hung2, Kwok-Hung Chan1, Hin Chu1, Kin-Hang Kok1, Kwok-Yung Yuen1,2, Kelvin Kai-Wang To1,2.
Abstract
We previously reported that topical imiquimod can improve the immunogenicity of the influenza vaccine. This study investigated another FDA-approved drug, miltefosine (MTF), as a vaccine adjuvant. Mice immunized with an influenza vaccine with or without MTF adjuvant were challenged by a lethal dose of influenza virus 3 or 7 days after vaccination. Survival, body weight, antibody response, histopathological changes, viral loads, cytokine levels, and T cell frequencies were compared. The MTF-adjuvanted vaccine (MTF-VAC) group had a significantly better survival rate than the vaccine-only (VAC) group, when administered 3 days (80% vs. 26.7%, p = 0.0063) or 7 days (96% vs. 65%, p = 0.0041) before influenza virus challenge. Lung damage was significantly ameliorated in the MTF-VAC group. Antibody response was significantly augmented in the MTF-VAC group against both homologous and heterologous influenza strains. There was a greater T follicular helper cell (TFH) response and an enhanced germinal center (GC) reaction in the MTF-VAC group. MTF-VAC also induced both TH1 and TH2 antigen-specific cytokine responses. MTF improved the efficacy of the influenza vaccine against homologous and heterologous viruses by improving the TFH and antibody responses. Miltefosine may also be used for other vaccines, including the upcoming vaccines for COVID-19.Entities:
Keywords: TFH; adjuvant; influenza vaccine; miltefosine; vaccine
Year: 2020 PMID: 33322574 PMCID: PMC7768360 DOI: 10.3390/vaccines8040754
Source DB: PubMed Journal: Vaccines (Basel) ISSN: 2076-393X