Interactome analysis of myeloid-derived suppressor cells in murine models of colon and breast cancer.

Alexander M Aliper,Victoria P Frieden-Korovkina,Alex Zhavoronkov,Anton Buzdin,Sergey A Roumiantsev

doi:10.18632/oncotarget.2489

Abstract

In solid cancers, myeloid derived suppressor cells (MDSC) infiltrate (peri)tumoral tissues to induce immune tolerance and hence to establish a microenvironment permissive to tumor growth. Importantly, the mechanisms that facilitate such infiltration or a subsequent immune suppression are not fully understood. Hence, in this study, we aimed to delineate disparate molecular pathways which MDSC utilize in murine models of colon or breast cancer. Using pathways enrichment analysis, we completed interactome maps of multiple signaling pathways in CD11b+/Gr1(high/low) MDSC from spleens and tumor infiltrates of mice with c26GM colon cancer and tumor infiltrates of MDSC in 4T1 breast cancer. In both cancer models, infiltrating MDSC, but not CD11b+ splenic cells, have been found to be enriched in multiple signaling molecules suggestive of their enhanced proliferative and invasive phenotypes. The interactome data has been subsequently used to reconstruct a previously unexplored regulation of MDSC cell cycle by the c-myc transcription factor which was predicted by the analysis. Thus, this study represents a first interactome mapping of distinct multiple molecular pathways whereby MDSC sustain cancer progression.

Highlights

Myeloid-derived suppressor cells (MDSC) are a heterogeneous group of progenitors of granulocytes, macrophages or dendritic cells (DC)
We utilized GEO GSE21927 dataset originally derived from a study by Marigo et al where c26GM colon carcinoma or 4T1 breast carcinoma tumors were induced in BALB/c mice [29]
Namely: 1) CD11b+ cells from spleens of c26GM colon cancer ; 2) CD11b+ cells from tumor infiltrates of c26GM colon cancer ; and 3) CD11b+ cells from tumor infiltrates of 4T1 breast cancer have been chosen based on the aforementioned dataset

Summary

Introduction

Myeloid-derived suppressor cells (MDSC) are a heterogeneous group of progenitors of granulocytes, macrophages or dendritic cells (DC). Differential expression of Gr1 is used to subdivide MDSC into a granulocytic group (CD11b+/ Gr1 high) or a monocytic one (CD11b+/Gr1 low) and can be implemented for discovery of anti-neoplastic targets in murine models [1]. MDSC infiltrate peritumoral tissues where they suppress CD4+ and CD8+ T-cells contributing to the immune tolerance [3]. Because of their functions, MDSC could even be implemented in differentiation systems for drug discovery in murine models [5]

Objectives

Methods

Results

Conclusion