Induced overexpression of MARCH-1 in human macrophages altered to M2 phenotype for suppressing inflammation process

(2022) Induced overexpression of MARCH-1 in human macrophages altered to M2 phenotype for suppressing inflammation process. IRANIAN JOURNAL OF BASIC MEDICAL SCIENCES. pp. 474-482. ISSN 2008-3866 2008-3874 J9 - IRAN J BASIC MED SCI

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Abstract

Objective(s): The M1 macrophage is characterized by enhanced pro-inflammatory cytokines production, whereas macrophage (M2) has anti-inflammatory features. Macrophage polarization as a therapeutic target for controlling immune responses could be performed by gene transduction to control the regulation of exaggerated innate/adaptive immune responses. Materials and Methods: Macrophages were prepared from THP-1 cell line and human monocytes that were transduced with (Membrane-Associated RING-CH-type finger) MARCH-1 viral lentivector produced in HEK-293T cells. RT-PCR and Western blotting confirmed MARCH-1 gene transduction. Cytokine production, CD markers assay, macrophage phagocytosis potential activity and mixed leukocyte reaction (MLR) with CFSE were performed for M1/M2 plasticity. Results: The mean fluorescent intensity of HLA-DR and CD64 expression reduced in MARCH-1+ transduced macrophage population. However, CD206 and CD163 expression increased in these macrophages. The concentrations of IL-6, TNF-?? and iNOS were decreased in MARCH-1 transduced cells, and TGF-?? production showed an augmentation in concentration. Western blotting and realtime PCR measurement confirmed that the expression levels of MARCH-1 protein and arginase-1 enzyme were increased in transduced macrophages. Conclusion: The anti-inflammatory features of MARCH-1 revealed the reduced levels of proinflammatory factors and maintained M2 phenotype characterized by high levels of scavenger receptors. Therefore, targeting MARCH-1 in monocytes/macrophages could represent a new autologous cell-based therapies strategy for inflammatory conditions.

Item Type: Article
Keywords: iNOS Macrophage MARCH-1 Polarization TGF-beta CELLS
Page Range: pp. 474-482
Journal or Publication Title: IRANIAN JOURNAL OF BASIC MEDICAL SCIENCES
Journal Index: ISI
Volume: 25
Number: 4
Identification Number: https://doi.org/10.22038/IJBMS.2022.62893.13902
ISSN: 2008-3866 2008-3874 J9 - IRAN J BASIC MED SCI
Depositing User: Zahra Otroj
URI: http://eprints.mui.ac.ir/id/eprint/15725

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