| Literature DB >> 32302573 |
Lei Zhang1, Ziyi Li2, Katarzyna M Skrzypczynska3, Qiao Fang1, Wei Zhang4, Sarah A O'Brien3, Yao He1, Lynn Wang3, Qiming Zhang2, Aeryon Kim3, Ranran Gao2, Jessica Orf3, Tao Wang2, Deepali Sawant3, Jiajinlong Kang2, Dev Bhatt3, Daniel Lu3, Chi-Ming Li3, Aaron S Rapaport3, Kristy Perez3, Yingjiang Ye4, Shan Wang4, Xueda Hu5, Xianwen Ren2, Wenjun Ouyang3, Zhanlong Shen6, Jackson G Egen7, Zemin Zhang8, Xin Yu9.
Abstract
Single-cell RNA sequencing (scRNA-seq) is a powerful tool for defining cellular diversity in tumors, but its application toward dissecting mechanisms underlying immune-modulating therapies is scarce. We performed scRNA-seq analyses on immune and stromal populations from colorectal cancer patients, identifying specific macrophage and conventional dendritic cell (cDC) subsets as key mediators of cellular cross-talk in the tumor microenvironment. Defining comparable myeloid populations in mouse tumors enabled characterization of their response to myeloid-targeted immunotherapy. Treatment with anti-CSF1R preferentially depleted macrophages with an inflammatory signature but spared macrophage populations that in mouse and human expresses pro-angiogenic/tumorigenic genes. Treatment with a CD40 agonist antibody preferentially activated a cDC population and increased Bhlhe40+ Th1-like cells and CD8+ memory T cells. Our comprehensive analysis of key myeloid subsets in human and mouse identifies critical cellular interactions regulating tumor immunity and defines mechanisms underlying myeloid-targeted immunotherapies currently undergoing clinical testing.Entities:
Keywords: Cell-cell interaction; Conventional DCs; Myeloid-targeted therapy; Single-cell RNA sequencing; Th1-like cells; Tumor-associated macrophages; Tumor-infiltrating myeloid cells; anti-CD40 treatment; anti-CSF1R treatment
Year: 2020 PMID: 32302573 DOI: 10.1016/j.cell.2020.03.048
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582