4.8 Article

Characterizing Macrophage Diversity in Metastasis-Bearing Lungs Reveals a Lipid-Associated Macrophage Subset

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CANCER RESEARCH
卷 81, 期 20, 页码 5284-5295

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AMER ASSOC CANCER RESEARCH
DOI: 10.1158/0008-5472.CAN-21-0101

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  1. American Cancer Society Postdoctoral Fellowship [PF-18-140-01-CSM]
  2. [R00HL138163]
  3. [R21CA235285]
  4. [R01CA215052]
  5. [R01HD095858]

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This study used single-cell RNA sequencing to analyze macrophages isolated from the lungs of mice with orthotopic mammary tumors, revealing seven distinct macrophage clusters. The findings highlight the diversity of macrophages present within metastatic lesions, including a novel subset of lipid-associated macrophages previously unidentified in lung metastases. Gene enrichment analysis revealed involvement in pathways related to lipid metabolism, extracellular matrix remodeling, and immunosuppression.
While macrophages are among the most abundant immune cell type found within primary and metastatic mammary tumors, how their complexity and heterogeneity change with metastatic progression remains unknown. Here, macrophages were isolated from the lungs of mice bearing orthotopic mammary tumors for singlecell RNA sequencing (scRNA-seq). Seven distinct macrophage clusters were identified, including populations exhibiting enhanced differential expression of genes related to antigen presentation (H2-Aa, Cd74), cell cycle (Stmn1, Cdk1), and interferon signaling (Isg15, Ifitm3). Interestingly, one cluster demonstrated a profile concordant with lipid-associated macrophages (Lgals3, Trem2). Compared with nontumor-bearing controls, the number of these cells per gram of tissue was significantly increased in lungs from tumor-bearing mice, with the vast majority costaining positively with the alveolar macrophage marker Siglec-F. Enrichment of genes implicated in pathways related to lipid metabolism as well extracellular matrix remodeling and immunosuppression was observed. In addition, these cells displayed reduced capacity for phagocytosis. Collectively, these findings highlight the diversity of macrophages present within metastatic lesions and characterize a lipid-associated macrophage subset previously unidentified in lung metastases. Significance: scRNA-seq of macrophages isolated from lung metastases reveals extensive macrophage heterogeneity and identifies a novel subpopulation enriched for genes involved in lipid metabolism, extracellular matrix remodeling, and immunosuppression.

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