Metabolism of primary colorectal tumor facilitate MDSC infiltration in pre-metastatic liver
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https://www.ncbi.nlm.nih.gov/sra/SRP252967
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Through an integrated transcriptome analysis of orthotopic colorectal cancer tumor-bearing mice and sham-operation mice, we showed the distinct immune microenvironment of pre-metastatic liver and identified MDSCs as the dominated cell type mediating pre-metastatic niche formation. MDSCs instead of other immune cell types were highly infiltrated in the pre-metastatic liver when compared with normal liver. Notably, immunosuppressive factors released by MDSCs such as HIF1a, iNOS, TGFÃ were significantly up-regulated in the pre-metastatic liver. Increasing immune checkpoint molecules expression also reflected an immunosuppressive condition of pre-metastatic liver. The primary tumor may induce MDSCs accumulation via metabolic mechanism including glycolysis/gluconeogenesis, HIF-1 signaling pathway, and CCL28 chemokine axis. This study depicts the immune cell landscape of pre-metastatic cancer and primary CRC tumor, and provides insights into how MDSCs reshape the pre-metastatic niche facilitating circulating cancer cells colonization. Overall design: Integrated transcriptomic analysis of orthotopic colorectal cancer tumor-bearing mice and sham-operation mice to identify immune landscape of pre-metastatic liver in comparison with normal liver. The corresponding metabolism and signaling pathways that potentially mediates pre-metastatic niche formation are explored.
创建时间:
2021-04-14



