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CXCR3.1 and CXCR3.2 Differentially Contribute to Macrophage Polarization in Teleost Fish
Author(s) -
XinJiang Lu,
Qiang Chen,
Ye-Jing Rong,
Feng Chen,
Jiong Chen
Publication year - 2017
Publication title -
the journal of immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.737
H-Index - 372
eISSN - 1550-6606
pISSN - 0022-1767
DOI - 10.4049/jimmunol.1700101
Subject(s) - cxcr3 , plecoglossus altivelis , biology , cxcl9 , gene , macrophage polarization , chemokine , immune system , phenotype , cxcl10 , microbiology and biotechnology , immunology , chemokine receptor , genetics , fish <actinopterygii> , fishery
The study of multiple copies of chemokine receptor genes in various teleosts has long appealed to investigators seeking to understand the evolution of the immune system. The CXCR CXCR3 gene has two isoforms, CXCR3.1 and CXCR3.2, which are both expressed in macrophages. The distinct roles of teleost CXCR3s have not been identified previously. In this article, we found that CXCR3.1 and CXCR3.2 differentially contributed to macrophage polarization in the teleosts: ayu ( Plecoglossus altivelis ), grass carp ( Ctenopharyngodon idella ), and spotted green pufferfish ( Tetraodon nigroviridis ). In ayu macrophages, the P. altivelis CXCR3.1 (PaCXCR3.1) gene was constitutively expressed, whereas the P. altivelis CXCR3.2 (PaCXCR3.2) gene was induced postinfection with Escherichia coli Upon E. coli infection, PaCXCR3.1 + and PaCXCR3.2 + macrophages showed an M1 and an M2 phenotype, respectively. CXCL9-11-like proteins mediated M1 and M2 polarization by interacting with the PaCXCR3.1 and PaCXCR3.2 proteins on macrophages, respectively. The transcription factors P. altivelis STAT1 and P. altivelis STAT3 were activated in PaCXCR3.1 + and PaCXCR3.2 + macrophages, respectively. Furthermore, the prognosis of septic ayu adoptively transferred with PaCXCR3.2 + macrophages was improved. Our data reveal a previously unknown mechanism for macrophage polarization, suggesting that redundant genes may regulate crucial functions in the teleost immune system.

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