1. TREM-2 serves as a negative immune regulator through Syk pathway in an IL-10 dependent manner in lung cancer
- Author
-
Dajing Xia, Guangdie Yang, Guohua Lu, Yinan Yao, Zhang Bao, Shuwen Hu, Weiyi Xu, Hequan Li, Jianying Zhou, and Junjun Chen
- Subjects
0301 basic medicine ,Adult ,Male ,Adoptive cell transfer ,Myeloid ,Lung Neoplasms ,immunoregulation ,Pathological staging ,T cell ,TREM-2 ,Syk ,03 medical and health sciences ,Carcinoma, Lewis Lung ,Mice ,Immune system ,Medicine ,Animals ,Humans ,Syk Kinase ,Receptors, Immunologic ,Aged ,Aged, 80 and over ,Membrane Glycoproteins ,business.industry ,Interleukin ,Middle Aged ,Interleukin-10 ,Mice, Inbred C57BL ,Interleukin 10 ,lung cancer ,030104 developmental biology ,medicine.anatomical_structure ,Oncology ,Immunology ,IL-10 ,Female ,business ,Research Paper - Abstract
During infection, triggering receptor expressed on myeloid cells-2 (TREM-2) restrains dendritic cells (DCs) and macrophages (MΦs) phagocytosis, as well as reduces pro-inflammatory cytokines release through DNAX-activation protein 12 (DAP12) signaling. However, the role of TREM-2 signaling in cancer has never been elucidated. In the current study, we found that TREM-2 was up-regulated on peripheral blood monocytes in tumor-bearing host. More TREM-2+DCs were detected in the lung of 3LL tumor-bearing mice. On the other hand, the level of TREM-2 on pulmonary MΦs positively correlated with the pathological staging of lung cancer. However, surgical or chemotherapeutic reduction of tumor burden led to the obvious decline of TREM-2. In vitro, TREM-2 expression of bone marrow (BM)-derived DCs and MΦs was induced by conditional medium (CM) containing the supernatant of 3LL cells. TREM-2+DCs from CM and/or tumor-bearing mice held altered phenotypes (CD80LowCD86LowMHCIILow) and impaired functions, such as, reduced interleukin (IL)-12 secretion, increased IL-10 production, and weakened ovalbumin (OVA)-endocytic capacity; also developed potent inhibitory effect on T cell proliferation that could be partially reversed by TREM-2 blockage. Moreover, spleen tyrosine kinase (Syk) inhibitor restrained IL-10 production of TREM-2+DC. Remarkably, IL-10 neutralizing antibody and Syk inhibitor both lowered the suppressive potential of TREM-2+DCs in T cell proliferation. Also, adoptive transfer of this TREM-2+DCs accelerated the tumor growth rather than jeopardized survival in lung cancer-bearing mice. In conclusion, these results indicate that TREM-2 might act as a negative immuno-regulatory molecule through Syk pathway in an IL-10 dependent manner and partially predicts prognosis in lung cancer patients.
- Published
- 2016