Monocytic Myeloid-Derived Suppressor Cells from Tumor Tissue Are a Differentiated Cell with Limited Fate Plasticity

Author:

Calvert Ryan D.1ORCID,Fleet James C.2ORCID,Fournier Pierrick G. J.3ORCID,Juarez Patricia3,Burcham Grant N.45ORCID,Haverkamp Jessica M.6,Guise Theresa A.7,Ratliff Timothy L.58,Elzey Bennett D.78

Affiliation:

1. *Department of Science and Mathematics, Tabor College, Hillsboro, KS;

2. †Department of Nutrition Science, University of Texas, Austin, TX;

3. ‡Center for Scientific Research and Higher Education at Ensenada, Ensenada, Baja California, Mexico;

4. §Heeke Animal Disease Diagnostic Laboratory, College of Veterinary Medicine, Purdue University, Dubois, IN;

5. ¶Department of Comparative Pathobiology, Purdue University, West Lafayette, IN;

6. ‖BlueRock Therapeutics, Boston, MA;

7. #Division of Internal Medicine, Department of Endocrine Neoplasia and Hormonal Disorders, The University of Texas MD Anderson Cancer Center, Houston, TX; and

8. **Center for Cancer Research, Purdue University, West Lafayette, IN

Abstract

Abstract Owing to ease of access and high yield, most murine myeloid-derived suppressor cell (MDSC) knowledge comes from the study of spleen-derived MDSCs rather than those isolated from the tumor. Although several studies have identified subtle differences in suppressive function between these MDSCs, a recent report demonstrated that the whole peripheral myeloid compartment poorly reflects myeloid populations found at the tumor. We confirm and extend these observations by presenting data that indicate extensive differences exist between peripheral and tumor MDSCs, suggesting that it may be inappropriate to use spleen MDSCs as surrogates for studying tumor MDSCs. Using cytospins, we observed that tumor MDSCs have undergone a morphologic shift from immature myeloid cell forms commonly seen in bone marrow (BM) and spleen MDSCs and acquired mature myeloid cell characteristics. Spleen and BM monocyte-like MDSCs (M-MDSCs) readily responded to differentiation signals for multiple myeloid cell types whereas tumor M-MDSCs had remarkably reduced cellular plasticity. At the time of isolation, M-MDSCs from BM or spleen have little to no T cell suppressive activity whereas those from the tumor possess immediate and efficient T cell suppressive function. Finally, microarray analysis revealed that the transcriptomes of tumor and spleen M-MDSCs possessed >4500 differentially expressed transcripts. We conclude that tumor M-MDSCs are more differentiated and mature, and that they are morphologically, genetically, and functionally distinct from spleen and BM M-MDSCs. These observations have important implications for the design of anti-MDSC therapies and suggest that preclinical studies using nontumor MDSCs could lead to results not applicable to tumor MDSCs.

Publisher

The American Association of Immunologists

Subject

Immunology and Allergy,General Medicine,Immunology

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