Inducible T-cell receptor expression in precursor T cells for leukemia control

Hoseini, Shahabuddin S; Hapke, Martin; Herbst, Jessica; Wedekind, Dirk; Baumann, Rolf; Heinz, Niels; Schiedlmeier, Bernhard; Vignali, Dario A.A.; Brink, Marcel R.M. van den; Schambach, Axel; Blazar, Bruce R.; Sauer, Martin

doi:10.1038/leu.2015.20

Cited by 8 publications

(12 citation statements)

References 43 publications

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“…Blockade of inhibitory pathways that negatively regulate TCR signaling may prolong T cell function within the TME, but this may also sustain TCR signaling in the tumor-reactive T cells, possibly leading to more profound T cell exhaustion and/or dysfunction, and indeed it appears that such blockade may only transiently restore function (Pauken et al, 2016). However, T cell engineering should allow testing strategies that interrupt chronic TCR signaling within tumors, such as with regulated TCR expression under the control of conditional and tunable promoters (Benabdellah et al, 2016; Hoseini et al, 2015; Roybal et al, 2016), and may make it possible to prevent acquisition of irreversible T cell dysfunction. Given the heterogeneity and TME complexity across the landscape of solid tumors, much remains to be discovered about the relationship between cancer immunity and distinct TMEs.…”

Section: Final Thoughts: Emerging Strategies To Overcome Obstacles Pomentioning

confidence: 99%

Obstacles Posed by the Tumor Microenvironment to T cell Activity: A Case for Synergistic Therapies

2017

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T cell dysfunction in solid tumors results from multiple mechanisms. Altered signaling pathways in tumor cells help produce a suppressive tumor microenvironment enriched for inhibitory cells, posing a major obstacle for cancer immunity. Metabolic constraints to cell function and survival shape tumor progression and immune cell function. In the face of persistent antigen, chronic T cell receptor signaling drives T lymphocytes to a functionally exhausted state. Here we discuss how the tumor and its microenvironment influences T cell trafficking and function with a focus on melanoma, pancreatic and ovarian cancer, and discuss how scientific advances may help overcome these hurdles.

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Section: Final Thoughts: Emerging Strategies To Overcome Obstacles Pomentioning

confidence: 99%

Obstacles Posed by the Tumor Microenvironment to T cell Activity: A Case for Synergistic Therapies

2017

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“…To track the development of CAR-expressing lymphoid progenitors in vivo, irradiated syngeneic C57BL/6 (B6) recipients were transplanted with 3 × 10 6 TCD-BM cells and adoptively transferred with 8 × 10 6 im1928z1-engineered lymphoid progenitors ( Figure 1D and Supplemental Figure 1D). Cotransplanted lymphoid progenitors have been shown to foster early repopulation of the thymus (8,11). The im1928z1-generated lymphoid progenitors did, however, completely fail to repopulate the thymus ( Figure 1E).…”

Section: Im1928z1-car Expression In Hspcs Prevents T Cell But Favors mentioning

confidence: 96%

“…HSPCs transduced with a host HLA-restricted TCR and differentiated into lymphoid progenitors of the T cell lineage have been shown to mediate potent antileukemic activity upon cotransplantation with T cell-depleted BM (TCD-BM) (11). To evaluate the biological consequences of CAR expression in differentiating lymphoid progenitors both in vitro and in vivo, we cloned a previously published murine second-generation CAR directed against mouse CD19 containing a CD28 costimulatory domain and 1 functional ITAM within the CD3ζ signaling domain, termed im1928z1 ( Figure 1A; supplemental material available online with this article; https://doi.org/10.1172/ JCI126350DS1).…”

Section: Im1928z1-car Expression In Hspcs Prevents T Cell But Favors mentioning

confidence: 99%

“…To evaluate the biological consequences of CAR expression in differentiating lymphoid progenitors both in vitro and in vivo, we cloned a previously published murine second-generation CAR directed against mouse CD19 containing a CD28 costimulatory domain and 1 functional ITAM within the CD3ζ signaling domain, termed im1928z1 ( Figure 1A; supplemental material available online with this article; https://doi.org/10.1172/ JCI126350DS1). CAR expression was set under the control of a tetracycline-inducible (Tet-On) T11 promoter to enable studying of the impact of time-dependent CAR expression (11,16). For inducible transgene expression, murine BM-derived Lineage -Sca-1 + c-Kit + (LSK) cells with an rtTA-M2 transactivator knockin were used.…”

Section: Im1928z1-car Expression In Hspcs Prevents T Cell But Favors mentioning

confidence: 99%

“…They give rise to a functional T cell population being both tolerant and MHC restricted to the host even in MHC-mismatched recipients (8)(9)(10). TCRengineered lymphoid precursors with a host-restricted TCR lead to rapid thymic repopulation, and their progeny can mediate potent and long-lasting antileukemia effects (11).…”

Section: Introductionmentioning

confidence: 99%

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Chimeric antigen receptor–induced BCL11B suppression propagates NK-like cell development

Maluski

Ghosh

Herbst

et al. 2019

Journal of Clinical Investigation

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Conflict of interest: MRMVDB has intellectual property licensing with Seres Therapeutics and Juno Therapeutics. MRMVDB has also received honorariums from Flagship Ventures, Novartis, Evelo, Seres Therapeutics, Jazz Pharmaceuticals, Therakos, Amgen, Merck, the Acute Leukemia Forum, and DKMS (board member) and research support from Seres Therapeutics, from which he has stock options. AG has received research support from Aprea Therapeutics and Infinity Pharmaceuticals.

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