| Literature DB >> 32289156 |
Carly E Whyte1, Maleika Osman1, Ervin E Kara1, Caitlin Abbott1, Jade Foeng1, Duncan R McKenzie1, Kevin A Fenix1, Yuka Harata-Lee1, Kerrie L Foyle1, Sarah T Boyle2, Marina Kochetkova2, Amelia Roman Aguilera3, Jiajie Hou3, Xian-Yang Li3, Mark A Armstrong4, Stephen M Pederson4, Iain Comerford1, Mark J Smyth3, Shaun R McColl1.
Abstract
Current immunotherapies involving CD8+ T cell responses show remarkable promise, but their efficacy in many solid tumors is limited, in part due to the low frequency of tumor-specific T cells in the tumor microenvironment (TME). Here, we identified a role for host atypical chemokine receptor 4 (ACKR4) in controlling intratumor T cell accumulation and activation. In the absence of ACKR4, an increase in intratumor CD8+ T cells inhibited tumor growth, and nonhematopoietic ACKR4 expression was critical. We show that ACKR4 inhibited CD103+ dendritic cell retention in tumors through regulation of the intratumor abundance of CCL21. In addition, preclinical studies indicate that ACKR4 and CCL21 are potential therapeutic targets to enhance responsiveness to immune checkpoint blockade or T cell costimulation.Entities:
Year: 2020 PMID: 32289156 DOI: 10.1084/jem.20190634
Source DB: PubMed Journal: J Exp Med ISSN: 0022-1007 Impact factor: 14.307