Lentiviral vector induces high-quality memory T cells via dendritic cells transduction

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作者
Min Wen Ku
Pierre Authié
Fabien Nevo
Philippe Souque
Maryline Bourgine
Marta Romano
Pierre Charneau
Laleh Majlessi
机构
[1] Laboratoire Commun Pasteur-TheraVectys,
[2] Institut Pasteur,undefined
[3] Unité de Virologie Moléculaire et Vaccinologie,undefined
[4] Institut Pasteur,undefined
[5] Université Paris Diderot,undefined
[6] Sorbonne Paris Cité,undefined
[7] Ecole Doctorale Frontières du Vivant (FdV),undefined
[8] Unit In Vivo Models,undefined
[9] Sciensano,undefined
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摘要
We report a lentiviral vector harboring the human β2-microglobulin promoter, with predominant expression in immune cells and minimal proximal enhancers to improve vector safety. This lentiviral vector efficiently transduces major dendritic cell subsets in vivo. With a mycobacterial immunogen, we observed distinct functional signatures and memory phenotype in lentiviral vector- or Adenovirus type 5 (Ad5)-immunized mice, despite comparable antigen-specific CD8+ T cell magnitudes. Compared to Ad5, lentiviral vector immunization resulted in higher multifunctional and IL-2-producing CD8+ T cells. Furthermore, lentiviral vector immunization primed CD8+ T cells towards central memory phenotype, while Ad5 immunization favored effector memory phenotype. Studies using HIV antigens in outbred rats demonstrated additional clear-cut evidence for an immunogenic advantage of lentiviral vector over Ad5. Additionally, lentiviral vector provided enhance therapeutic anti-tumor protection than Ad5. In conclusion, coupling lentiviral vector with β2-microglobulin promoter represents a promising approach to produce long-lasting, high-quality cellular immunity for vaccinal purposes.
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