| Literature DB >> 30277474 |
Enguang Bi1, Rong Li2, Laura C Bover3, Haiyan Li1, Pan Su1, Xingzhe Ma1, Chunjian Huang1, Qiang Wang1, Lintao Liu1, Maojie Yang1, Zhijuan Lin1, Jianfei Qian1, Weijun Fu2, Yong-Jun Liu4, Qing Yi1.
Abstract
Plasmacytoid dendritic cells (pDCs) play a key role in antiviral responses by producing type-1 IFNs. However, recent studies showed that pDCs induce immune suppression and promote tumor growth in human ovarian cancer and myeloma. The molecular mechanisms underlying pDC acquisition of these properties are unknown. Here we show that human pDCs activated by CpG inhibited growth and induced apoptosis in myeloma cells via secreted IFN-α, but direct contact with myeloma cells converted pDCs into tumor-promoting cells by suppressing pDC IFN-α production. E-cadherin, expressed on both myeloma cells and pDCs, mediated these effects via a homophilic interaction - activation of E-cadherin signaling upregulated and activated TNFAIP3 to interact with TLR9, resulting in TLR9 ubiquitination and degradation, and inhibition of IFN-α production in pDCs. These findings were supported by an in vivo study in which pDC depletion induced tumor regression and better survival in the Vk*MYC myeloma mouse model. Furthermore, IFNAR1 expression level positively correlated to overall survival of patients with multiple myeloma (MM), and the IFN-α level in patient bone marrow was significantly lower than that in marrow of healthy individuals. This study reveals a novel mechanism underlying how MM tumors educate pDCs in their microenvironment and provides new targets for improving the treatment of MM.Entities:
Keywords: Bone marrow; Cancer; Cancer immunotherapy; Immunology; Therapeutics
Mesh:
Substances:
Year: 2018 PMID: 30277474 PMCID: PMC6205396 DOI: 10.1172/JCI121421
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808