Abstract

? Project 1 The mononuclear phagocyte system is critical in the host's response to pathogens and inflammation, but it is also critical for removing old or malignant cells. In non-Hodgkin lymphoma (NHL), monocytic cells are central components of the innate immune system and CD14+ monocytes in the peripheral blood as well as CD68+ tumor-associated macrophages (TAMs) in tissue influence the prognosis of patients. We have previously shown that CD14+HLADRlow monocytes are increased in the peripheral blood of NHL patients, are induced by IL-10, and profoundly suppresses T-cell function. However, in lymphoma tissue biopsies, we found that many CD68+ TAMs downregulate CD14 expression. While CD14+ TAMs typically expressed common macrophage markers, we found that the CD68+CD14- fraction expressed very few of these markers. To determine whether CD68+CD14- TAMs retained macrophage function, we measured the expression of signal-regulatory protein ? (SIRP?), a receptor that inhibits phagocytic function. Based on SIRP? expression, we identified 2 distinct populations of TAMs in sites involved by lymphoma ? those that were CD14+SIRP?high and those that were CD14-SIRP?low/- ? but the phagocytic ability and role of these two populations is unknown. SIRP? regulates macrophage-mediated removal of apoptotic cells that upregulate `eat-me' signals such as calreticulin. The induction of phagocytosis by `eat-me' signals on tumor cells is countered by `don't-eat-me' signals such as CD47, which binds macrophage SIRP? to inhibit phagocytosis. CD47 has been shown to be highly expressed on lymphoma cells and is a mechanism by which malignant B-cells protect themselves from phagocytosis by activated macrophages. However, CD47/SIRP? interaction not only regulates phagocytosis but also has a role in modulating T-cell function by enhancing antigen presentation, effectively making the CD47/SIRP? axis an immune checkpoint for the innate immune system. We hypothesize that CD14+SIRP?high TAMs are highly functional, able to phagocytose malignant cells, present tumor antigens and activate the immune system but are inhibited by CD47. In contrast, CD14-SIRP?low/- TAMs are immature, fail to phagocytose malignant cells and suppress immune function. To improve the outcome of lymphoma patients, the phagocytosis and T-cell activation by both CD14+SIRP?high and CD14-SIRP?low/- TAMs needs to be augmented. We therefore propose to determine the phagocytic function and immune activation of both CD14+SIRP?high and CD14-SIRP?low/- TAMs, and determine whether blocking CD47/SIRP? signaling clinically using SIRP?-Fc can enhance the tumor-directed phagocytic function of both populations of TAMs. We anticipate that results from this project will lead not only to a comprehensive understanding of the subtypes of TAMs in lymphoma, but an innovative therapy that harnesses the power of both the innate and adaptive immune systems.

Public Health Relevance

Project 1 Macrophage-mediated phagocytosis is an important mechanism to eliminate diseased and malignant cells. Malignant lymphoma cells, by overexpressing CD47, provide a `don't-eat-me' signal and thereby avoid eradication. We propose to block CD47/SIRP? signaling to restore an ?eat-me' message. However, not all macrophages in lymphoma tumors express SIRP? and we have defined populations that are CD14+SIRP?high and those that are CD14-SIRP?low/-. We therefore propose to determine the function of these two populations, to determine whether the innate phagocytic immune system targets lymphoma cells, and test whether blocking an innate immune checkpoint (CD47/SIRP? signaling) improves the anti-tumor immune response.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
5P50CA097274-19
Application #
9988171
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2020-07-01
Budget End
2021-06-30
Support Year
19
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
University of Iowa
Department
Type
DUNS #
062761671
City
Iowa City
State
IA
Country
United States
Zip Code
52242

  Publications

Leelakanok, Nattawut; Geary, Sean M; Salem, Aliasger K (2018) Antitumor Efficacy and Toxicity of 5-Fluorouracil-Loaded Poly(Lactide Co-glycolide) Pellets. J Pharm Sci 107:690-697
Ghesquières, Hervé; Larrabee, Beth R; Casasnovas, Olivier et al. (2018) A susceptibility locus for classical Hodgkin lymphoma at 8q24 near MYC/PVT1 predicts patient outcome in two independent cohorts. Br J Haematol 180:286-290
Sharma, Ayush; Oishi, Naoki; Boddicker, Rebecca L et al. (2018) Recurrent STAT3-JAK2 fusions in indolent T-cell lymphoproliferative disorder of the gastrointestinal tract. Blood 131:2262-2266
Fama, Angelo; Xiang, Jinhua; Link, Brian K et al. (2018) Human Pegivirus infection and lymphoma risk and prognosis: a North American study. Br J Haematol 182:644-653
Jalali, Shahrzad; Price-Troska, Tammy; Paludo, Jonas et al. (2018) Soluble PD-1 ligands regulate T-cell function in Waldenstrom macroglobulinemia. Blood Adv 2:1985-1997
Bachy, Emmanuel; Maurer, Matthew J; Habermann, Thomas M et al. (2018) A simplified scoring system in de novo follicular lymphoma treated initially with immunochemotherapy. Blood 132:49-58
Franqui-Machin, Reinaldo; Hao, Mu; Bai, Hua et al. (2018) Destabilizing NEK2 overcomes resistance to proteasome inhibition in multiple myeloma. J Clin Invest 128:2877-2893
Ghahramani, Grant K; Goetz, Kirsten E; Liu, Vincent (2018) Dermoscopic characterization of cutaneous lymphomas: a pilot survey. Int J Dermatol 57:339-343
Hu, G; Dasari, S; Asmann, Y W et al. (2018) Targetable fusions of the FRK tyrosine kinase in ALK-negative anaplastic large cell lymphoma. Leukemia 32:565-569
Moss, Jennifer L; Xiao, Qian; Matthews, Charles E (2018) Patterns of cancer-related health behaviors among middle-aged and older adults: Individual- and area-level socioeconomic disparities. Prev Med 115:31-38

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