Abstract
Background: Colorectal cancer, the fourth leading cause of cancer mortality, is prone to metastasis, especially to the liver. The pre-metastatic microenvironment comprising various resident stromal cells and immune cells is essential for metastasis. However, how the dynamic evolution of immune components facilitates pre-metastatic niche formation remains unclear.Methods: Utilizing RNA-seq data from our orthotopic colorectal cancer mouse model, we applied single sample gene set enrichment analysis and Cell type Identification By Estimating Relative Subsets Of RNA Transcripts to investigate the tumor microenvironment landscape of pre-metastatic liver, and define the exact role of myeloid-derived suppressor cells (MDSCs) acting in the regulation of infiltrating immune cells and gene pathways activation. Flow cytometry analysis was conducted to quantify the MDSCs levels in human and mice samples.Results: In the current work, based on the high-throughput transcriptome data, we depicted the immune cell infiltration pattern of pre-metastatic liver and highlighted MDSCs as the dominant altered cell type. Notably, flow cytometry analysis showed that high frequencies of MDSCs, was detected in the pre-metastatic liver of orthotopic colorectal cancer tumor-bearing mice, and in the peripheral blood of patients with stage I–III colorectal cancer. MDSCs accumulation in the liver drove immunosuppressive factors secretion and immune checkpoint score upregulation, consequently shaping the pre-metastatic niche with sustained immune suppression. Metabolic reprogramming such as upregulated glycolysis/gluconeogenesis and HIF-1 signaling pathways in the primary tumor was also demonstrated to correlate with MDSCs infiltration in the pre-metastatic liver. Some chemokines were identified as a potential mechanism for MDSCs recruitment.Conclusion: Collectively, our study elucidates the alterations of MDSCs during pre-metastatic niche transformation, and illuminates the latent biological mechanism by which primary tumors impact MDSC aggregation in the targeted liver.
Highlights
Distant metastasis, especially liver metastasis, is the top killer among patients with colorectal cancer (CRC)
We examined the proportion of PMN-Myeloid-derived suppressor cells (MDSCs) and monocyte myeloid suppressor cells (M-MDSCs) based on CD15 and CD14 expression, and defined the total MDSCs as the sum of PMN-MDSCs and M-MDSCs
We further focused on the relationship between pre-metastatic MDSCs and the metabolic pathways of the primary tumor
Summary
Especially liver metastasis, is the top killer among patients with colorectal cancer (CRC). Numerous studies have indicated that tumor metastasis is a multi-step process [3, 4]; before circulating tumor cells reach the targeted organ, the preconditioned microenvironment may be reshaped to prompt cancer cell extravasation and extracellular matrix remodeling [5]. This initial step, i.e., pre-metastatic niche establishment, is predominantly derived from the shift of local stromal components and recruitment of non-resident cells [6]. How the dynamic evolution of immune components facilitates pre-metastatic niche formation remains unclear
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