Abstract

Cancer immunoediting is the process whereby the immune system not only recognizes and destroys developing tumors but also shapes tumor immunogenicity. We formulated this hypothesis 7 years ago and we now know that it occurs in three phases-Elimination, Equilibrium and Escape. Although roles for the interferons (IFN) i.e., Type I IFN and IFN? in this process have been recognized for several years, the critical cellular targets of their action that mediate anti-tumor immunity have remained obscure. In this renewal application, we propose to use mice that we generated on a C57BL/6 background that display tissue specific deficits in either Type I IFN- or IFN?-receptor expression to identify the critical IFN responsive cells needed for immune elimination of tumors and to define their mechanisms of action. We will pursue two Specific Aims.
Specific Aim I : Identify the cellular targets of Type I IFN critical for sarcoma elimination and define the functional consequences of Type I IFN effects on these cells. We will assess in vivo rejection of transplanted unedited sarcomas in mice lacking IFNAR1 in different cellular compartments paying particular attention to CD8?+ dendritic cells (DC). Concomitantly we will continue our ongoing studies exploring whether Type I IFN sensitivity is required for cross presentation of tumor antigens by CD11c+ cells and the CD8?+ DC subset and define Type I IFN's mechanism of action in the process. We will determine whether all Type I IFN subtypes (including IFN?) display equivalent activity on these cells and then stringently test the validity of our findings by performing primary MCA tumor induction studies on mice with IFNAR1 deficits in cellular compartments that render them incapable of rejecting unedited tumors.
Specific Aim II : Identify the cellular targets of IFN? critical for sarcoma elimination and define the functional consequences of IFN? on these cells. We will assess in vivo rejection of transplanted unedited sarcomas in mice lacking IFNGR1 in different cellular compartments paying particular attention to T cells, macrophages and endothelial cells. Using IFN? sensitive and insensitive T cells, macrophages and/or endothelial cells we will then explore in detail how IFN? alters their cellular biology to induce their participation in either (a) development of anti-tumor immune responses or (b) to act as direct mediators of tumor destruction. Ultimately we will stringently test the validity of our findings by performing primary MCA tumor induction studies on mice with IFNAR1 deficits in cellular compartments that render them incapable of rejecting unedited tumors.

Public Health Relevance

This proposal seeks to identify the particular immune cells that must respond to immune hormones known as interferons. Identifying these cells and defining how they function may lead to new therapeutic strategies that use the immune system to fight cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA043059-26
Application #
8617230
Study Section
Transplantation, Tolerance, and Tumor Immunology (TTT)
Program Officer
Mccarthy, Susan A
Project Start
1986-02-01
Project End
2015-02-28
Budget Start
2014-03-01
Budget End
2015-02-28
Support Year
26
Fiscal Year
2014
Total Cost
$312,787
Indirect Cost
$107,006

  Institution

Name
Washington University
Department
Pathology
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Noguchi, Takuro; Ward, Jeffrey P; Gubin, Matthew M et al. (2017) Temporally Distinct PD-L1 Expression by Tumor and Host Cells Contributes to Immune Escape. Cancer Immunol Res 5:106-117
Ward, Jeffrey P; Gubin, Matthew M; Schreiber, Robert D (2016) The Role of Neoantigens in Naturally Occurring and Therapeutically Induced Immune Responses to Cancer. Adv Immunol 130:25-74
Griffith, Obi L; Chan, Szeman Ruby; Griffith, Malachi et al. (2016) Truncating Prolactin Receptor Mutations Promote Tumor Growth in Murine Estrogen Receptor-Alpha Mammary Carcinomas. Cell Rep 17:249-260
Gubin, Matthew M; Artyomov, Maxim N; Mardis, Elaine R et al. (2015) Tumor neoantigens: building a framework for personalized cancer immunotherapy. J Clin Invest 125:3413-21
Sheehan, Kathleen C F; Lazear, Helen M; Diamond, Michael S et al. (2015) Selective Blockade of Interferon-? and -? Reveals Their Non-Redundant Functions in a Mouse Model of West Nile Virus Infection. PLoS One 10:e0128636
Chang, Chih-Hao; Qiu, Jing; O'Sullivan, David et al. (2015) Metabolic Competition in the Tumor Microenvironment Is a Driver of Cancer Progression. Cell 162:1229-41
Mittal, Deepak; Gubin, Matthew M; Schreiber, Robert D et al. (2014) New insights into cancer immunoediting and its three component phases--elimination, equilibrium and escape. Curr Opin Immunol 27:16-25
Gubin, Matthew M; Zhang, Xiuli; Schuster, Heiko et al. (2014) Checkpoint blockade cancer immunotherapy targets tumour-specific mutant antigens. Nature 515:577-81
Lee, Sang Hun; Carrero, Javier A; Uppaluri, Ravindra et al. (2013) Identifying the initiating events of anti-Listeria responses using mice with conditional loss of IFN-? receptor subunit 1 (IFNGR1). J Immunol 191:4223-34
Pan, Hua; Myerson, Jacob W; Hu, Lingzhi et al. (2013) Programmable nanoparticle functionalization for in vivo targeting. FASEB J 27:255-64

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