Dendritic cells (DCs) initiate adaptive immune responses after their migration to secondary lymphoid organs. The LXR ligands/oxysterols and the RXR ligand 9-cis Retinoic Acid (9-cis RA) were shown to dampen DC migration to lymphoid organs through the inhibition of CCR7 expression. We performed transcriptomics of DCs undergoing maturation in the presence of the LXR ligand 22R-Hydroxycholesterol (22R-HC). The analysis highlighted more than 1500 genes modulated by 22R-HC treatment, including the triggering receptor expressed on myeloid cells (TREM)-1, which was found markedly up-regulated. We tested the effect of other nuclear receptor ligands (NRL) and we reported the induction of TREM-1 following RXR, RAR and VDR activation. From a functional point of view, triggering of TREM-1 induced by retinoids increased TNFα and IL-1β release, suggesting an active role of NRL-activated TREM-1(+) DCs in inflammation-driven diseases, including cancer. Consistently with this hypothesis we detected DCs expressing TREM-1 in pleural effusions and ascites of cancer patients, an observation validated by the induction of TREM-1, LXR and RAR target genes when monocyte-DCs were activated in the presence of tumor-conditioned fluids. Finally, we observed a better control of LLC tumor growth in Trem-1(-/-) bone marrow chimera mice as compared to wild type chimera mice. Future studies will be necessary to shed light on the mechanism of TREM-1 induction by distinct NRL, and to characterize the role of TREM-1(+) DCs in tumor growth.
Nuclear receptor ligands induce TREM-1 expression on dendritic cells: analysis of their role in tumors.
核受体配体诱导树突状细胞表达TREM-1:分析其在肿瘤中的作用
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作者:Fontana Raffaella, Raccosta Laura, Rovati Lucrezia, Steffensen Knut R, Paniccia Aida, Jakobsson Tomas, Melloni Giulio, Bandiera Alessandro, Mangili Giorgia, Bergamini Alice, Maggioni Daniela, Doglioni Claudio, Crocchiolo Roberto, Cella Marina, Mattioli Michela, Battaglia Cristina, Colonna Marco, Russo Vincenzo
| 期刊: | Oncoimmunology | 影响因子: | 6.300 |
| 时间: | 2019 | 起止号: | 2018 Dec 13; 8(3):1554967 |
| doi: | 10.1080/2162402X.2018.1554967 | 研究方向: | 细胞生物学、肿瘤 |
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