Abstract
Due to their ability to present foreign antigens and prime naïve T cells, macrophages, and dendritic cells (DCs) are referred to as professional antigen-presenting cells (APCs). Although activated macrophages may function as APCs, these cells are particularly effective at directly engaging pathogens through phagocytosis, and production of antimicrobial compounds. On the other hand, DCs possess superb antigen-presenting and costimulatory capacity and they are essential for commencement and regulation of adaptive immune responses. In in vitro models, development of mature mammalian DCs from monocytes requires sequential exposure to growth factors (including GM-CSF and IL-4) and proinflammatory stimuli such as toll-like receptor (TLR) ligands. Currently, except for IL-4/13, neither orthologs nor functional analogs of the growth factors which are essential for the differentiation of mammalian DCs (including GM-CSF and FLT3) have been identified in teleosts and data about differentiation of piscine APCs is scant. In the present study, primary salmon mononuclear phagocytes (MPs) stimulated in vitro for 5–7 days with a B-class CpG oligodeoxynucleotides (ODN 2006PS) underwent morphological differentiation and developed “dendritic” morphology, characterized by long, branching pseudopodia. Transcriptional profiling showed that these cells expressed high levels of proinflammatory mediators characteristic for M1 polarized MPs. However, the cells treated with CpGs for 7 days downregulated their surface MHCII molecules as well as their capacity to endocytose ovalbumin and exhibited attenuated allostimulatory activity. This concurred with transcriptional downregulation of costimulatory CD80/86 and upregulation of inhibitory CD274 (B7-H1) genes. Despite their exhausted allostimulatory activity, these cells were still responsive to re-stimulation with gardiquimod (a TLR7/8 ligand) and further upregulated a wide array of immune genes including proinflammatory mediators such as intereukin-1 beta and tumor necrosis factor. Overall, the presented data highlight the disparate effects TLR ligands may have on the proinflammatory status of APCs, on one side, and their antigen-presenting/costimulatory functions, on the other. These findings also indicate that despite the poor phylogenetic conservation of the growth factors involved in the differentiation of DCs, some of the processes that orchestrate the development and the differentiation of professional APCs are conserved between teleosts in mammals.
Highlights
The mononuclear phagocyte (MP) system comprises circulating monocytes, tissue resident macrophages, and monocyte-derived DCs
When adherent salmon head kidney (HK) MPs were stimulated in vitro for >5 days with CpGs (2 μM) many of the cells developed relatively long, branching pseudopodia, a morphological feature manifested by DCs [9] and, in some cases, M1 macrophages [30] (Figure 1A)
Using a CellTraceTM Violet Cell Proliferation Kit we found that unlike autologous MPs, stimulators from other individuals incubated with responder spleen lymphocytes for 2 weeks induced modest spleen cell proliferation of the total population as indicated by the increased percentage of responders with reduced amount of dye
Summary
The mononuclear phagocyte (MP) system comprises circulating monocytes, tissue resident macrophages, and monocyte-derived DCs. Macrophages are mainly engaged in direct elimination of pathogens through endocytosis and production of antibacterial agents, they are capable of presenting foreign antigens and priming naïve T cells [6]. These cells have been studied extensively in fishes and the specifics of their development and functional diversity (including development of M1 and M2 functional phenotypes) within teleosts have recently been covered in review articles [7, 8]
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