Combined Skin and Muscle DNA Priming Provides Enhanced Humoral Responses to a Human Immunodeficency Virus Type 1 Clade C Envelope Vaccine.

Hannah Mary Cheeseman; Suzanne Day; Leon Robert McFarlane; Sue Fleck ORCID logo; Aleisha Miller; Tom Cole; Nelson Sousa-Santos; Alethea Cope; Deniz Cizmeci; Monica Tolazzi; +13 more... Edith Hwekwete; Drew Hannaman; Sven Kratochvil; Paul Francis McKay; Amy W Chung; Stephen J Kent; Adrian Cook; Gabriella Scarlatti; Sonya Abraham; Behazine Combadiere; Sheena McCormack; David John Lewis; Robin John Shattock; (2018) Combined Skin and Muscle DNA Priming Provides Enhanced Humoral Responses to a Human Immunodeficency Virus Type 1 Clade C Envelope Vaccine. Human gene therapy, 29 (9). pp. 1011-1028. ISSN 1043-0342 DOI: 10.1089/hum.2018.075
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Intradermal (i.d.) and intramuscular (i.m.) injections when administered with or without electroporation (EP) have the potential to tailor the immune response to DNA vaccination. This Phase I randomized controlled clinical trial in human immunodeficiency virus type 1-negative volunteers investigated whether the site and mode of DNA vaccination influences the quality of induced cellular and humoral immune responses following the DNA priming phase and subsequent protein boost with recombinant clade C CN54 gp140. A strategy of concurrent i.d. and i.m. DNA immunizations administered with or without EP was adopted. Subtle differences were observed in the shaping of vaccine-induced virus-specific CD4+ and CD8+ T cell-mediated immune responses between groups receiving: i.d.EP + i.m., i.d. + i.m.EP, and i.d.EP + i.m.EP regimens. The DNA priming phase induced 100% seroconversion in all of the groups. A single, non-adjuvanted protein boost induced a rapid and profound increase in binding antibodies in all groups, with a trend for higher responses in i.d.EP + i.m.EP. The magnitude of antigen-specific binding immunoglobulin G correlated with neutralization of closely matched clade C 93MW965 virus and Fc-dimer receptor binding (FcγRIIa and FcγRIIIa). These results offer new perspectives on the use of combined skin and muscle DNA immunization in priming humoral and cellular responses to recombinant protein.


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