Literature DB >> 19395317

IL-12 delivered intratumorally by multilamellar liposomes reactivates memory T cells in human tumor microenvironments.

Michelle R Simpson-Abelson1, Vivek S Purohit, Wing Man Pang, Vandana Iyer, Kunle Odunsi, Todd L Demmy, Sandra J Yokota, Jenni L Loyall, Raymond J Kelleher, Sathy Balu-Iyer, Richard B Bankert.   

Abstract

Using a novel loading technique, IL-12 is reported here to be efficiently encapsulated within large multilamellar liposomes. The preclinical efficacy of the cytokine loaded liposomes to deliver IL-12 into human tumors and to reactive tumor-associated T cells in situ is tested using a human tumor xenograft model. IL-12 is released in vivo from these liposomes in a biologically active form when injected into tumor xenografts that are established by the subcutaneous implantation of non-disrupted pieces of human lung, breast or ovarian tumors into immunodeficient mice. The histological architecture of the original tumor tissue, including tumor-associated leukocytes, tumor cells and stromal cells is preserved anatomically and the cells remain functionally responsive to cytokines in these xenografts. The local and sustained release of IL-12 into the tumor microenvironment reactivates tumor-associated quiescent effector memory T cells to proliferate, produce and release IFN-gamma resulting in the killing of tumor cells in situ. Very little IL-12 is detected in the serum of mice for up to 5 days after an intratumoral injection of the IL-12 liposomes. We conclude that IL-12 loaded large multilamellar liposomes provide a safe method for the local and sustained delivery of IL-12 to tumors and a therapeutically effective way of reactivating existing tumor-associated T cells in human solid tumor microenvironments. The potential of this local in situ T cell re-stimulation to induce a systemic anti-tumor immunity is discussed.

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Year:  2009        PMID: 19395317      PMCID: PMC2693480          DOI: 10.1016/j.clim.2009.03.516

Source DB:  PubMed          Journal:  Clin Immunol        ISSN: 1521-6616            Impact factor:   3.969


  48 in total

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2.  Amount of interleukin 12 available at the tumor site is critical for tumor regression.

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3.  Lymphatic uptake and biodistribution of liposomes after subcutaneous injection. II. Influence of liposomal size, lipid compostion and lipid dose.

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4.  CD3 hyporesponsiveness and in vitro apoptosis are features of T cells from both malignant and nonmalignant secondary lymphoid organs.

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5.  Critical role of NK1+ T cells in IL-12-induced immune responses in vivo.

Authors:  T Kawamura; K Takeda; S K Mendiratta; H Kawamura; L Van Kaer; H Yagita; T Abo; K Okumura
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6.  IL-12 deaths: explanation and a puzzle.

Authors:  J Cohen
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Authors:  M B Atkins; M J Robertson; M Gordon; M T Lotze; M DeCoste; J S DuBois; J Ritz; A B Sandler; H D Edington; P D Garzone; J W Mier; C M Canning; L Battiato; H Tahara; M L Sherman
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Authors:  A J Zajac; J N Blattman; K Murali-Krishna; D J Sourdive; M Suresh; J D Altman; R Ahmed
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9.  Induction and exhaustion of lymphocytic choriomeningitis virus-specific cytotoxic T lymphocytes visualized using soluble tetrameric major histocompatibility complex class I-peptide complexes.

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10.  T helper type 1/T helper type 2 cytokines and T cell death: preventive effect of interleukin 12 on activation-induced and CD95 (FAS/APO-1)-mediated apoptosis of CD4+ T cells from human immunodeficiency virus-infected persons.

Authors:  J Estaquier; T Idziorek; W Zou; D Emilie; C M Farber; J M Bourez; J C Ameisen
Journal:  J Exp Med       Date:  1995-12-01       Impact factor: 14.307

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  21 in total

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Authors:  Heather K Lehman; Michelle R Simpson-Abelson; Thomas F Conway; Raymond J Kelleher; Joel M Bernstein; Richard B Bankert
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2.  Characterization of an IL-12 p40/p35 Truncated Fusion Protein That can Inhibit the Action of IL-12.

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3.  Exosomes Associated with Human Ovarian Tumors Harbor a Reversible Checkpoint of T-cell Responses.

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4.  T cells and stromal fibroblasts in human tumor microenvironments represent potential therapeutic targets.

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6.  Patient-derived xenografts of low-grade B-cell lymphomas demonstrate roles of the tumor microenvironment.

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Review 9.  Localized Interleukin-12 for Cancer Immunotherapy.

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Review 10.  Particle platforms for cancer immunotherapy.

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