Your search keyword '"Leong, Meredith"' showing total 4 results

1. Magnitude of Therapeutic STING Activation Determines CD8 + T Cell-Mediated Anti-tumor Immunity.

Author

Sivick KE, Desbien AL, Glickman LH, Reiner GL, Corrales L, Surh NH, Hudson TE, Vu UT, Francica BJ, Banda T, Katibah GE, Kanne DB, Leong JJ, Metchette K, Bruml JR, Ndubaku CO, McKenna JM, Feng Y, Zheng L, Bender SL, Cho CY, Leong ML, van Elsas A, Dubensky TW Jr, and McWhirter SM

Subjects

Animals, CTLA-4 Antigen metabolism, Cell Line, Tumor, Cytokines metabolism, Dose-Response Relationship, Immunologic, Drug Resistance, Neoplasm, Hematopoiesis, Mice, Inbred BALB C, Mice, Inbred C57BL, Neoplasms pathology, Programmed Cell Death 1 Receptor metabolism, S100 Proteins administration & dosage, S100 Proteins immunology, CD8-Positive T-Lymphocytes immunology, Immunity, Membrane Proteins metabolism, Neoplasms immunology

Abstract

Intratumoral (IT) STING activation results in tumor regression in preclinical models, yet factors dictating the balance between innate and adaptive anti-tumor immunity are unclear. Here, clinical candidate STING agonist ADU-S100 (S100) is used in an IT dosing regimen optimized for adaptive immunity to uncover requirements for a T cell-driven response compatible with checkpoint inhibitors (CPIs). In contrast to high-dose tumor ablative regimens that result in systemic S100 distribution, low-dose immunogenic regimens induce local activation of tumor-specific CD8 + effector T cells that are responsible for durable anti-tumor immunity and can be enhanced with CPIs. Both hematopoietic cell STING expression and signaling through IFNAR are required for tumor-specific T cell activation, and in the context of optimized T cell responses, TNFα is dispensable for tumor control. In a poorly immunogenic model, S100 combined with CPIs generates a survival benefit and durable protection. These results provide fundamental mechanistic insights into STING-induced anti-tumor immunity., (Copyright © 2018 Aduro Biotech, Inc. Published by Elsevier Inc. All rights reserved.)

Published

2018

2. STING-Activating Adjuvants Elicit a Th17 Immune Response and Protect against Mycobacterium tuberculosis Infection

Author

Van Dis, Erik, Sogi, Kimberly M, Rae, Chris S, Sivick, Kelsey E, Surh, Natalie H, Leong, Meredith L, Kanne, David B, Metchette, Ken, Leong, Justin J, Bruml, Jacob R, Chen, Vivian, Heydari, Kartoosh, Cadieux, Nathalie, Evans, Tom, McWhirter, Sarah M, Dubensky, Thomas W, Portnoy, Daniel A, and Stanley, Sarah A

Subjects

Biological Sciences, Biodefense, Infectious Diseases, Orphan Drug, Tuberculosis Vaccine, Rare Diseases, Prevention, Vaccine Related, Immunization, Emerging Infectious Diseases, Tuberculosis, 3.4 Vaccines, Infection, Good Health and Well Being, Adjuvants, Immunologic, Animals, BCG Vaccine, Disease Models, Animal, Immunity, Cellular, Membrane Proteins, Mice, Mice, Knockout, Mycobacterium tuberculosis, Th1 Cells, Th17 Cells, Tuberculosis, Pulmonary, Vaccines, Subunit, Th17, cyclic dinucleotides, vaccine adjuvant, Biochemistry and Cell Biology, Medical Physiology, Biological sciences

Abstract

There are a limited number of adjuvants that elicit effective cell-based immunity required for protection against intracellular bacterial pathogens. Here, we report that STING-activating cyclic dinucleotides (CDNs) formulated in a protein subunit vaccine elicit long-lasting protective immunity to Mycobacterium tuberculosis in the mouse model. Subcutaneous administration of this vaccine provides equivalent protection to that of the live attenuated vaccine strain Bacille Calmette-Guérin (BCG). Protection is STING dependent but type I IFN independent and correlates with an increased frequency of a recently described subset of CXCR3-expressing T cells that localize to the lung parenchyma. Intranasal delivery results in superior protection compared with BCG, significantly boosts BCG-based immunity, and elicits both Th1 and Th17 immune responses, the latter of which correlates with enhanced protection. Thus, a CDN-adjuvanted protein subunit vaccine has the capability of eliciting a multi-faceted immune response that results in protection from infection by an intracellular pathogen.

Published

2018

3. Listeria-Based Cancer Vaccines That Segregate Immunogenicity from Toxicity

Author

Brockstedt, Dirk G., Giedlin, Martin A., Leong, Meredith L., Bahjat, Keith S., Gao, Yi, Luckett, William, Liu, Weiqun, Cook, David N., Portnoy, Daniel A., Dubensky,, Thomas W., and Allison, James P.

Published

2004

4. Recombinant Listeria promotes tumor rejection by CD8+ T cell-dependent remodeling of the tumor microenvironment.

Author

Weiwen Deng, Lira, Victor, Hudson, Thomas E., Lemmens, Edward E., Hanson, William G., Flores, Ruben, Barajas, Gonzalo, Katibah, George E., Desbien, Anthony L., Lauer, Peter, Leong, Meredith L., Portnoy, Daniel A., and Dubensky Jr., Thomas W.

Subjects

T cells, TYPE I interferons, LISTERIA monocytogenes, IMMUNITY, GENE expression

Abstract

Agents that remodel the tumor microenvironment (TME), prime functional tumor-specific T cells, and block inhibitory signaling pathways are essential components of effective immunotherapy. We are evaluating live-attenuated, double-deleted Listeria monocytogenes expressing tumor antigens (LADD-Ag) in the clinic. Here we show in numerous mouse models that while treatment with nonrecombinant LADD induced some changes in the TME, no antitumor efficacy was observed, even when combined with immune checkpoint blockade. In contrast, LADD-Ag promoted tumor rejection by priming tumor-specific KLRG1+PD1loCD62L- CD8+ T cells. These IFNγ-producing effector CD8+ T cells infiltrated the tumor and converted the tumor from an immunosuppressive to an inflamed microenvironment that was characterized by a decrease in regulatory T cells (Treg) levels, a proinflammatory cytokine milieu, and the shift of M2 macrophages to an inducible nitric oxide synthase (iNOS)+CD206- M1 phenotype. Remarkably, these LADD-Ag-induced tumor-specific T cells persisted for more than 2 months after primary tumor challenge and rapidly controlled secondary tumor challenge. Our results indicate that the striking antitumor efficacy observed in mice with LADD-based immunotherapy stems from TME remodeling which is a direct consequence of eliciting potent, systemic tumor-specific CD8+ T cells. [ABSTRACT FROM AUTHOR]

Published

2018