Tumor-targeted T cells modified to secrete IL-12 eradicate systemic tumors without need for prior conditioning

Pegram, Hollie J.; Lee, James C.; Hayman, Erik; Imperato, Gavin H.; Tedder, Thomas F.; Sadelain, Michel; Brentjens, Renier J.

doi:10.1182/blood-2011-12-400044

Cited by 576 publications

(489 citation statements)

References 41 publications

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“…These findings have parallels in CD4 + T cells, where miR-155 is essential for longterm maintenance of T reg cells in lymphoreplete, but not lymphodepleted, mice (20). Other strategies to potentiate adoptive T-cell therapy in the absence of lymphodepletion have been recently proposed, such as PD1 blockade in the presence of IL-2/anti-IL-2 antibody complexes (32) or overexpression of IL-12 in tumorreactive T cells (33). However, it is unclear whether such approaches can replace both lymphodepletion and cytokine support.…”

Section: Discussionmentioning

confidence: 80%

miR-155 augments CD8 ⁺ T-cell antitumor activity in lymphoreplete hosts by enhancing responsiveness to homeostatic γ _c cytokines

Ji¹,

Wrzesinski

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

103

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Lymphodepleting regimens are used before adoptive immunotherapy to augment the antitumor efficacy of transferred T cells by removing endogenous homeostatic "cytokine sinks." These conditioning modalities, however, are often associated with severe toxicities. We found that microRNA-155 (miR-155) enabled tumorspecific CD8 + T cells to mediate profound antitumor responses in lymphoreplete hosts that were not potentiated by immune-ablation. miR-155 enhanced T-cell responsiveness to limited amounts of homeostatic γc cytokines, resulting in delayed cellular contraction and sustained cytokine production. miR-155 restrained the expression of the inositol 5-phosphatase Ship1, an inhibitor of the serinethreonine protein kinase Akt, and multiple negative regulators of signal transducer and activator of transcription 5 (Stat5), including suppressor of cytokine signaling 1 (Socs1) and the protein tyrosine phosphatase Ptpn2. Expression of constitutively active Stat5a recapitulated the survival advantages conferred by miR-155, whereas constitutive Akt activation promoted sustained effector functions. Our results indicate that overexpression of miR-155 in tumorspecific T cells can be used to increase the effectiveness of adoptive immunotherapies in a cell-intrinsic manner without the need for life-threatening, lymphodepleting maneuvers.

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Section: Discussionmentioning

confidence: 80%

miR-155 augments CD8 ⁺ T-cell antitumor activity in lymphoreplete hosts by enhancing responsiveness to homeostatic γ _c cytokines

Ji¹,

Wrzesinski

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

103

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“…36 Additionally, CAR T cells themselves have been modified by the incorporation of co-stimulatory endodomains such as CD28, 4-1BB, and OX40, 37,38 though our results suggest that this is likely insufficient to provide long term in vivo benefit at the tumor site ( Figure S1). Other modifications include the transgenic expression of Th1 cytokines to promote autocrine growth 36,[39][40][41] or the incorporation of a dominant-negative TGF-b receptor, which sequesters this tumor-produced immunosuppressive cytokine. 42,43 Our approach extends upon the dominant-negative receptor concept by inverting a soluble immunosuppressive signal present in the tumor microenvironment into one that is immunostimulatory (4/7 ICR).…”

Section: Discussionmentioning

confidence: 99%

Improving Chimeric Antigen Receptor-Modified T Cell Function by Reversing the Immunosuppressive Tumor Microenvironment of Pancreatic Cancer

Sukumaran²,

et al. 2017

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“…The latter approach has been used to deliver CD8 þ T cells specific for melanoma antigens [102][103][104] or engineered to express a chimeric antigen receptor (CAR) against CD19 in B-cell lymphomas. 105 The administered IL-12 was found to activate myeloid cells by increasing the expression of Fas and cross-presentation, leading to the stimulation of tumor antigen-specific CD8 T cells and regression of established tumors 102,106 (Figure 1). More recently, the development of novel approaches that direct IL-12 activity to the tumor site focus on immunocytokines, for example, the fusion of the cytokine to an antibody that binds specifically to the tumor vasculature, 107,108 or to exposed deoxyribonucleic acid (DNA) in the necrotic core of a tumor.…”

Section: Therapeutic Effects Of Il-12 In Preclinical Modelsmentioning

confidence: 99%

New insights into IL-12-mediated tumor suppression

et al. 2014

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During the past two decades, interleukin-12 (IL-12) has emerged as one of the most potent cytokines in mediating antitumor activity in a variety of preclinical models. Through pleiotropic effects on different immune cells that form the tumor microenvironment, IL-12 establishes a link between innate and adaptive immunity that involves different immune effector cells and cytokines depending on the type of tumor or the affected tissue. The robust antitumor response exerted by IL-12, however, has not yet been successfully translated into the clinics. The majority of clinical trials involving treatment with IL-12 failed to show sustained antitumor responses and were associated to toxic side effects. Here we discuss the therapeutic effects of IL-12 from preclinical to clinical studies, and will highlight promising strategies to take advantage of the antitumor activity of IL-12 while limiting adverse effects.

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Tumor-targeted T cells modified to secrete IL-12 eradicate systemic tumors without need for prior conditioning

Cited by 576 publications

References 41 publications

miR-155 augments CD8 ⁺ T-cell antitumor activity in lymphoreplete hosts by enhancing responsiveness to homeostatic γ _c cytokines

miR-155 augments CD8 ⁺ T-cell antitumor activity in lymphoreplete hosts by enhancing responsiveness to homeostatic γ _c cytokines

Improving Chimeric Antigen Receptor-Modified T Cell Function by Reversing the Immunosuppressive Tumor Microenvironment of Pancreatic Cancer

New insights into IL-12-mediated tumor suppression

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Tumor-targeted T cells modified to secrete IL-12 eradicate systemic tumors without need for prior conditioning

Cited by 576 publications

References 41 publications

miR-155 augments CD8 + T-cell antitumor activity in lymphoreplete hosts by enhancing responsiveness to homeostatic γ c cytokines

miR-155 augments CD8 + T-cell antitumor activity in lymphoreplete hosts by enhancing responsiveness to homeostatic γ c cytokines

Improving Chimeric Antigen Receptor-Modified T Cell Function by Reversing the Immunosuppressive Tumor Microenvironment of Pancreatic Cancer

New insights into IL-12-mediated tumor suppression

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Product

Resources

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miR-155 augments CD8 ⁺ T-cell antitumor activity in lymphoreplete hosts by enhancing responsiveness to homeostatic γ _c cytokines

miR-155 augments CD8 ⁺ T-cell antitumor activity in lymphoreplete hosts by enhancing responsiveness to homeostatic γ _c cytokines