Prolonged survival and tissue trafficking following adoptive transfer of CD4ζ gene-modified autologous CD4+ and CD8+ T cells in human immunodeficiency virus–infected subjects

Mitsuyasu, Ronald T.; Anton, Peter A.; Deeks, Steven G.; Scadden, David T.; Connick, Elizabeth; Downs, Matthew; Bakker, Andreas; Roberts, Michelle; June, Carl H.; Jalali, Sayeh; Lin, Andy; Pennathur-Das, Rukmini; Hege, Kristen

doi:10.1182/blood.v96.3.785.015k10_785_793

Cited by 224 publications

(126 citation statements)

References 37 publications

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“…While the chimeric receptor‐transduced cells described here may be of clinical value, past experience indicates that cells of this type rapidly lose functionality in vivo. 43, 44 This effect is manifest in our own system by our data showing a substantial decrease in tumor‐specific cytokine release during in vitro culture. We also show here that stimulation of transduced T cells with G D2 ‐expressing tumor cells alone does not provide a sufficient stimulus for commitment to proliferation, continued T‐cell expansion and long‐term in vitro persistence.…”

Section: Discussionmentioning

confidence: 71%

Targeting of GD2-positive tumor cells by human T lymphocytes engineered to express chimeric T-cell receptor genes

et al. 2001

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Genetic engineering of human T lymphocytes to express tumor antigen-specific chimeric immune receptors is an attractive means for providing large numbers of effector cells for adoptive immunotherapy while bypassing major mechanisms of tumor escape from immune recognition. We have applied this strategy to the targeting of a G D2 -positive tumor, neuroblastoma, which is the commonest extracranial solid tumor of childhood. Chimeric immune receptors were generated by joining an extracellular antigen-binding domain derived from either of the 2 ganglioside G D2 -specific antibodies sc7A4 and sc14.G2a to a cytoplasmic signaling domain. The variable domains of hybridoma antibody 14.G2a were cloned and selected using a phage display approach. Upon coincubation with G D2 -expressing tumor cell targets, human T lymphocytes transduced with recombinant retroviruses encoding chimeric receptors based on sc14.G2a, but not sc7A4, secreted significant levels of cytokines in a pattern comparable to the cytokine response obtained by engagement of the CD3 receptor. T cells transduced with the sc14.G2a-based chimeric T-cell receptors also displayed specific lysis of G D2 -positive neuroblastoma cells, which was blocked in the presence of monoclonal antibody 14.G2a. In the absence of nonspecific stimulation of transduced cells, their functionality declined over time and antigenic stimulation of the chimeric receptor alone did not induce commitment to proliferation. These results support the feasibility of redirecting human T lymphocytes to a tumor-associated ganglioside epitope but emphasize that successful chimeric receptor-mediated adoptive immunotherapy will require additional strategies that overcome functional inactivation of gene-modified primary T lymphocytes.

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Section: Discussionmentioning

confidence: 71%

Targeting of GD2-positive tumor cells by human T lymphocytes engineered to express chimeric T-cell receptor genes

et al. 2001

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“…Several clinical trials that tested therapeutic infusion of autologous T cells have been completed . These trials included treatments with expanded autologous HIV‐specific T cells, treatments with HIV Env targeting CAR‐T cells, and CCR5‐modified CD4 T cells . While these therapeutic T cell trials were shown to be safe, they did not result in a functional cure for HIV.…”

Section: Discussionmentioning

confidence: 99%

“…Interestingly, the very first clinical tests of CAR technology were directed against HIV‐1 infection, using first‐generation CAR constructs employing CD4 as the targeting motif. Whilst minimal virus suppression was achieved, the CAR‐T cells were found to be safe, and had stable levels of engraftment with a decay half‐life exceeding 16 years . There are several advantages to using HIV targeting CAR‐T cells or CAR‐NK cell immunotherapy.…”

Section: Car‐t and Car‐nk Cellsmentioning

confidence: 99%

Targeting reservoirs of HIV replication in lymphoid follicles with cellular therapies to cure HIV

Skinner

2018

Adv Cell Gene Ther

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There is a need to create improved treatments for HIV infection. Growing evidence indicates that HIV treatment strategies must target and reduce viral replication in lymphoid follicles where HIV replication is most concentrated. In this mini‐review, three cell therapy approaches are described: CAR‐T and CAR‐NK cells, adoptive transfer of autologous HIV‐specific T cells, and HIV‐resistant cells. The potential for these innovative strategies to reduce viral replication in follicles and the potential of combining cell therapies with other treatment strategies to achieve a complete eradication of HIV is discussed.

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“…The transferred T cells were well tolerated in patients and circulating anti‐gp120 CD4 + and CD8 + transduced T cells could be detected up to 42 weeks post infusion, with evidence of trafficking to mucosal HIV reservoirs. Gene‐modified virus‐specific T cells showed sustained cell survival in these patients, independent of exogenous IL‐2 administration (83). In a subsequent Phase II trial involving a cohort of 40 patients, some reduction in levels of HIV burden and a trend toward reduced recurrent viremia was observed (84).…”

Section: Clinical Application Of Gene‐modified T Cellsmentioning

confidence: 94%

Adoptive immunotherapy for cancer: the next generation of gene‐engineered immune cells

2009

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Adoptive cellular immunotherapy involving transfer of tumor-reactive T cells has shown some notable antitumor responses in a minority of cancer patients. In particular, transfer of tumor-infiltrating lymphocytes has resulted in long-term objective responses in patients with advanced melanoma. However, the inability to isolate sufficient numbers of tumor-specific T cells from most malignancies has restricted the broad utility of this approach. An emerging approach to circumvent this limitation involves the genetic modification of effector cells with T cell receptor (TCR) transgenes or chimeric single-chain variable fragment (scFv) receptors that can specifically redirect T cells to tumor. There has been much progress in the design of TCR and scFv receptors to enhance the antigen-specific activation of effector cells and their trafficking and persistence in vivo. Considerable effort has been directed toward improving the safety of this approach and reducing the immunogenicity of the receptor. This review discusses the latest developments in the field of adoptive immunotherapy using genetically modified immune cells that have been transduced with either TCR or scFv receptor transgenes and used in preclinical and clinical settings as anticancer agents.

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Prolonged survival and tissue trafficking following adoptive transfer of CD4ζ gene-modified autologous CD4+ and CD8+ T cells in human immunodeficiency virus–infected subjects

Cited by 224 publications

References 37 publications

Targeting of GD2-positive tumor cells by human T lymphocytes engineered to express chimeric T-cell receptor genes

Targeting of GD2-positive tumor cells by human T lymphocytes engineered to express chimeric T-cell receptor genes

Targeting reservoirs of HIV replication in lymphoid follicles with cellular therapies to cure HIV

Adoptive immunotherapy for cancer: the next generation of gene‐engineered immune cells

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