| Literature DB >> 33463049 |
Wei Wang1,2,3, Yu Zhong1,2,3, Zhenkun Zhuang1,2,3, Jiarui Xie1,2,3, Yueer Lu1, Chengzhi Huang4, Yan Sun2,3, Liang Wu2,3, Jianhua Yin2,3, Hang Yu1, Zhiqiang Jiang1, Shanshan Wang2,3, Chunqing Wang2,3, Yuanhang Zhang2,3, Yilin Huang1, Chongyin Han1, Zhenggang Zhong1, Jialin Hu1, Ying Ouyang1, Huisheng Liu1, Mengya Yu4, Xiaochan Wei2, Dandan Chen2, Lizhen Huang1, Yong Hou2,3,5, Zhanglin Lin1, Shiping Liu2,3,5,6, Fei Ling1, Xueqing Yao4.
Abstract
The tumor microenvironment is a complex ecosystem formed by distinct and interacting cell populations, and its composition is related to cancer prognosis and response to clinical treatment. In this study, we have taken the advantage of two single-cell RNA sequencing technologies (Smart-seq2 and DNBelab C4) to generate an atlas of 15,115 immune and nonimmune cells from primary tumors and hepatic metastases of 18 colorectal cancer (CRC) patients. We observed extensive changes in the proportions and functional states of T cells and B cells in tumor tissues, compared to those of paired non-tumor tissues. Importantly, we found that B cells from early CRC tumor were identified to be pre-B like expressing tumor suppressors, whereas B cells from advanced CRC tumors tended to be developed into plasma cells. We also identified the association of IgA+ IGLC2+ plasma cells with poor CRC prognosis, and demonstrated a significant interaction between B-cell and myeloid-cell signaling, and found CCL8+ cycling B cells/CCR5+ T-cell interactions as a potential antitumoral mechanism in advanced CRC tumors. Our results provide deeper insights into the immune infiltration within CRC, and a new perspective for the future research in immunotherapies for CRC.Entities:
Mesh:
Year: 2021 PMID: 33463049 PMCID: PMC7775989 DOI: 10.1002/ctm2.253
Source DB: PubMed Journal: Clin Transl Med ISSN: 2001-1326