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Vaccine-induced immunity in baboons by using DNA and replication-incompetent adenovirus type 5 vectors expressing a human immunodeficiency virus type 1 gag gene
Authors:Casimiro Danilo R  Tang Aimin  Chen Ling  Fu Tong-Ming  Evans Robert K  Davies Mary-Ellen  Freed Daniel C  Hurni William  Aste-Amezaga Jose M  Guan Liming  Long Romnie  Huang Lingyi  Harris Virginia  Nawrocki Denise K  Mach Henryk  Troutman Robert D  Isopi Lynne A  Murthy Krishna K  Rice Karen  Wilson Keith A  Volkin David B  Emini Emilio A  Shiver John W
Institution:Department of Viral Vaccine Research, Merck Research Laboratories, West Point, Pennsylvania 19486, USA. danilo_casimiro@merck.com
Abstract:The cellular immunogenicity of formulated plasmid DNA and replication-defective human adenovirus serotype 5 (Ad5) vaccine vectors expressing a codon-optimized human immunodeficiency virus type 1 gag gene was examined in baboons. The Ad5 vaccine was capable of inducing consistently strong, long-lived CD8(+)-biased T-cell responses and in vitro cytotoxic activities. The DNA vaccine-elicited immune responses were weaker than those elicited by the Ad5 vaccine and highly variable; formulation with chemical adjuvants led to moderate increases in the levels of Gag-specific T cells. Increasing the DNA-primed responses with booster doses of either Ad5 or modified vaccinia virus Ankara vaccines suggests a difference in the relative levels of cytotoxic and helper responses. The implications of these results are discussed.
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