Pre-clinical data supporting immunotherapy for HIV using CMV-HIV-specific CAR T cells with CMV vaccine

被引:11
|
作者
Guan, Min [1 ]
Lim, Laura [1 ]
Holguin, Leo [2 ,3 ]
Han, Tianxu [2 ,3 ]
Vyas, Vibhuti [1 ]
Urak, Ryan [2 ,3 ]
Miller, Aaron [3 ,4 ]
Browning, Diana L. [2 ,3 ]
Echavarria, Liliana [2 ,3 ]
Li, Shasha [2 ,3 ]
Li, Shirley [2 ,3 ]
Chang, Wen-Chung [1 ]
Scott, Tristan [2 ,3 ]
Yazaki, Paul [3 ,4 ]
Morris, Kevin, V [2 ,3 ]
Cardoso, Angelo A. [2 ,3 ]
Blanchard, M. Suzette [3 ,5 ]
Le Verche, Virginia [2 ,3 ]
Forman, Stephen J. [1 ]
Zaia, John A. [2 ,3 ]
Burnett, John C. [2 ,3 ]
Wang, Xiuli [1 ]
机构
[1] City Hope Natl Med Ctr, Dept Hematol & Hematopoiet Cell Transplantat, T Cell Therapeut Res Lab, 1500 East Duarte Rd, Duarte, CA 91010 USA
[2] City Hope Natl Med Ctr, Ctr Gene Therapy, Dept Hematol & Hematopoiet Cell Transplantat, Duarte, CA 91010 USA
[3] Beckman Res Inst, Duarte, CA USA
[4] City Hope Natl Med Ctr, Dept Mol Imaging & Therapy, Duarte, CA 91010 USA
[5] City Hope Natl Med Ctr, Div Biostat, Duarte, CA 91010 USA
关键词
CHIMERIC ANTIGEN RECEPTORS; ANTITUMOR EFFICACY; BONE-MARROW; PERSISTENCE; VIVO; SURVIVAL; IDENTIFICATION; ACTIVATION; RESISTANT; IMMUNITY;
D O I
10.1016/j.omtm.2022.04.007
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
T cells engineered to express HIV-specific chimeric antigen receptors (CARs) represent a promising strategy to clear HIV-infected cells, but to date have not achieved clinical benefits. A likely hurdle is the limited T cell activation and persistence when HIV antigenemia is low, particularly during antiretroviral therapy (ART). To overcome this issue, we propose to use a cytomegalovirus (CMV) vaccine to stimulate CMV-specific T cells that express CARs directed against the HIV-1 envelope protein gp120. In this study, we use a GMP-compliant platform to engineer CMV-specific T cells to express a second-generation CAR derived from the N6 broadly neutralizing antibody, one of the broadest anti-gp120 neutralizing antibodies. These CMV-HIV CAR T cells exhibit dual effector functions upon in vitro stimulation through their endogenous CMV-specific T cell receptors or the introduced CARs. Using a humanized HIV mouse model, we show that CMV vaccination during ART accelerates CMV-HIV CAR T cell expansion in the peripheral blood and that higher numbers of CMV-HIV CAR T cells were associated with a better control of HIV viral load and fewer HIV antigen p24(+) cells in the bone marrow upon ART interruption. Collectively, these data support the clinical development of CMV-HIV CART cells in combination with a CMV vaccine in HIV-infected individuals.
引用
收藏
页码:344 / 359
页数:16
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