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A Prime-Pull-Amplify Vaccination Strategy To Maximize Induction of Circulating and Genital-Resident Intraepithelial CD8 Memory T Cells.

J. Immunol.. 2019; 
?uburuNicolas,KimRina,GuittardGeoffrey C,ThompsonCynthia D,DayPatricia M,HammDavid E,PangYuk-Ying S,GrahamBarney S,LowyDouglas R,SchillerJo
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Recombinant Antibody Services In vitro peptide stimulation and intracellular cytokine staining Single cell suspensions were incubated for 5 h at 37˚C in RPMI 1640 medium only or supplemented E749–57 peptide (5 mg/ml; GenScript).... Spleen cells were incubated for 3 d at 37˚C in RPMI 1640 medium containing recombinant human IL-2 (100 iu/ml; TECIN) and OVA254–262 (20 ng/ml; Genscript) or gp10025–33 peptide (100 ng/ml; Genscript). Get A Quote

摘要

Recent insight into the mechanisms of induction of tissue-resident memory (T) CD8 T cells (CD8 T) enables the development of novel vaccine strategies against sexually transmitted infections. To maximize both systemic and genital intraepithelial CD8 T cells against vaccine Ags, we assessed combinations of i.m. and intravaginal routes in heterologous prime-boost immunization regimens with unrelated viral vectors. Only i.m. prime followed by intravaginal boost induced concomitant strong systemic and intraepithelial genital-resident CD8 T cell responses. Intravaginal boost with vectors expressing vaccine Ags was far superior to intravaginal instillation of CXCR3 chemokine receptor ligands or TLR 3, 7, and 9 a... More

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