T Cell Immunogenicity, Gene Expression Profile, and Safety of Four Heterologous Prime-Boost Combinations of HIV Vaccine Candidates in Healthy Volunteers: Results of the Randomized Multi-Arm Phase I/II ANRS VRI01 Trial

被引:8
作者
Richert, Laura [1 ,2 ,3 ,4 ]
Lelievre, Jean-Daniel [4 ,5 ,6 ]
Lacabaratz, Christine [4 ,5 ]
Hardel, Lucile [1 ,4 ]
Hocini, Hakim [4 ,5 ]
Wiedemann, Aurelie [4 ,5 ]
Lucht, Frederic [7 ,8 ,9 ]
Poizot-Martin, Isabelle [10 ]
Bauduin, Claire [1 ,4 ]
Diallo, Alpha [11 ]
Rieux, Veronique [4 ,11 ]
Rouch, Elodie [1 ,4 ]
Surenaud, Mathieu [4 ,5 ]
Lefebvre, Cecile [4 ,5 ]
Foucat, Emile [4 ,5 ]
Tisserand, Pascaline [4 ,5 ]
Guillaumat, Lydia [4 ,5 ]
Durand, Melany [1 ,2 ,3 ,4 ]
Hejblum, Boris [1 ,2 ,3 ,4 ]
Launay, Odile [12 ,13 ]
Thiebaut, Rodolphe [1 ,2 ,3 ,4 ]
Levy, Yves [4 ,5 ,6 ]
机构
[1] Univ Bordeaux, Bordeaux Populat Hlth Res Ctr, INSERM, UMR 1219, Bordeaux, France
[2] Inria, SISTM Team, Talence, France
[3] CHU Bordeaux, Serv Informat Med, Bordeaux, France
[4] Vaccine Res Inst, Creteil, France
[5] Univ Paris Est Creteil, INSERM, Creteil, France
[6] Albert Chenevier, AP HP, Grp Henri Mondor, Creteil, France
[7] CHU St Etienne, St Priest En Jarez, France
[8] Univ Jean Monnet, St Etienne, France
[9] Univ Lyon, St Etienne, France
[10] Aix Marseille Univ, Serv Immuno Hematol Clin, APHM, INSERM,IRD,SESSTIM,SESSTIM,ISS PAM, Marseille, France
[11] INSERM ANRS, Paris, France
[12] Hop Cochin, AP HP, INSERM, CIC 1417 F CRIN REIVAC, Paris, France
[13] Univ Paris 05, Paris, France
关键词
HIGHLY PATHOGENIC SIV; THERAPEUTIC IMMUNIZATION; DOUBLE-BLIND; EFFICACY; IMMUNITY; LIPOPEPTIDE; RESPONSES; STRATEGY; VIREMIA; ALVAC;
D O I
10.4049/jimmunol.2101076
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Heterologous prime-boost strategies are of interest for HIV vaccine development. The order of prime-boost components could be important for the induction of T cell responses. In this phase I/II multi-arm trial, three vaccine candidates were used as prime or boost: modified vaccinia Ankara (MVA) HIV-B (coding for Gag, Pol, Nef); HIV LIPO-5 (five lipopeptides from Gag, Pol, Nef); DNA GTU-MultiHIV B (coding for Rev, Nef, Tat, Gag, Env gp160 Glade B). Healthy human volunteers (n = 92) were randomized to four groups: 1) MVA at weeks 0/8 + LIPO-5 at weeks 20/28 (M/L); 2) LIPO-5 at weeks 0/8 + MVA at weeks 20/28 (L/M); 3) DNA at weeks 0/4/12 + LIPO-5 at weeks 20/28 (G/L); 4) DNA at weeks 0/4/12 + MVA at weeks 20/28 (G/M). The frequency of IFN-gamma-ELISPOT responders at week 30 was 33, 43, 0, and 74%, respectively. Only MVA-receiving groups were further analyzed (n = 62). Frequency of HIV-specific cytokine-positive (IFN-gamma, IL-2, or TNF-alpha) CD4(+) T cells increased significantly from week 0 to week 30 (median change of 0.06, 0.11, and 0.10% for M/L, L/M, and G/M, respectively), mainly after MVA vaccinations, and was sustained until week 52. HIV-specific CD8(+) T cell responses increased significantly at week 30 in M/L and G/M (median change of 0.02 and 0.05%). Significant whole-blood gene expression changes were observed 2 wk after the first MVA injection, regardless of its use as prime or boost. An MVA gene signature was identified, including 86 genes mainly related to cell cycle pathways. Three prime-boost strategies led to CD4(+) and CD8(+) T cell responses and to a whole-blood gene expression signature primarily due to their MVA HIV-B component.
引用
收藏
页码:2663 / +
页数:14
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