Macrophage-specific nanotechnology-driven CD163 overexpression in human macrophages results in an M2 phenotype under inflammatory conditions

Alvarado-Vázquez, Perla Abigail; Bernal, Laura; Paige, Candler; Grosick, Rachel L.; Vilrriales, Carolina Moracho; Ferreira, David Wilson; Ulecia-Morón, Cristina; Romero‐Sandoval, E. Alfonso

doi:10.1016/j.imbio.2017.05.011

Cited by 85 publications

(54 citation statements)

References 60 publications

(83 reference statements)

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“…Macrophages participate in this process by maintaining the in ammatory and brogenic environment (41). CD163 promotes the transformation of macrophages from M1 to M2 phenotype and releases antiin ammatory factors to solve in ammation (42). In our analysis, CD163 was down regulated in HCM, which may be a key factor in the persistent in ammatory environment of HCM.…”

Section: Discussionmentioning

confidence: 57%

Dysfunctional network and mutation genes of hypertrophic cardiomyopathy

Cui

Liu

Liang

2020

Preprint

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Background Hypertrophic cardiomyopathy (HCM) is a group of heterogeneous diseases that affect the myocardium. It is also a common familial disease. The symptoms are not common and easy to find. Methods In this study, gene expression profiles of 37 samples (GSE130036) were downloaded from GEO database. Differential analysis was used to identify the related dysregulated genes in patients with HCM. Enrichment analysis identified the biological function and signal pathway of these differentially expressed genes. Then, we build PPI network and verify it in GSE36961 dataset. Finally, the gene of single nuclear variants (SNVs) in HCM samples was screened by means of maftools. Results Herein, we obtained 920 differentially expressed genes, and found that these genes are mainly related to metabolic related signaling pathways. 187 interacting genes were identified by PPI network analysis, and the expression trends of C1QB, F13A1, CD163, FCN3, PLA2G2A and CHRDL2 were verified by another dataset. ROC curve analysis showed that they had certain clinical diagnostic ability, and they were the potential key dysfunctional genes of HCM. In addition, we found that PRMT5 mutation was the most frequent in HCM samples, which may affect the pathogenesis of HCM. Conclusions Therefore, the key genes and enrichment results identified by our analysis may provide a reference for the occurrence and development mechanism of HCM. In addition, mutations in PRMT5 may be a useful therapeutic and diagnostic target for HCM.

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Section: Discussionmentioning

confidence: 57%

Dysfunctional network and mutation genes of hypertrophic cardiomyopathy

Cui

Liu

Liang

2020

Preprint

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“…The present results establish that a tolerogenic vaccine able to mitigate EAE in inbred SPF mice through MOG-targeting to peripheral DC and induction of FOXP3+ suppressor Tregs (Idoyaga et al , 2013; Ring et al , 2013) also applies to outbred adult primates with a trained immune system. In mice, tolerogenic priming relied on the ability of particular DC subsets to produce TGF β (Idoyaga et al , 2013; Ring et al , 2013; Yamazaki et al , 2008), a cytokine also produced by CD163+ M2 macrophages (Zaba et al , 2007; Alvarado-Vazquez et al , 2017). These CD163+ macaque’s skin macrophage have migratory properties as they are also retrieved in lymph nodes (Adam et al , 2015).…”

Section: Discussionmentioning

confidence: 99%

Targeting MOG to skin macrophages prevents EAE in macaques through TGFβ-induced peripheral tolerance

Fovet

Stimmer

Contreras

et al. 2019

Preprint

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To study the effect of vaccination on tolerization to the myelin antigen MOG we used 26 a macaque model of experimental autoimmune encephalitis (EAE) in which immunization with 27 recombinant human myelin oligodendrocyte glycoprotein (rhMOG) elicits brain inflammation 28 and demyelination mediated by MOG-specific autoreactive CD4+ T lymphocytes and anti-MOG 29IgG. For antigen targeting to tolerizing antigen presenting cells, we used a recombinant antibody 30 directed to the Dendritic Cells (DC)-Asialoglycoprotein receptor (DC-ASGPR). The intradermal 31 administration of an anti-DC-ASGPR-MOG fusion protein, but not a control anti-DC-ASGPR-32 PSA (prostate specific antigen) protein, protected monkeys committed to develop EAE. 33Although effective treatment did not modify anti-MOG IgG production, it prevented the CD4+ T 34 lymphocyte activation and pro-inflammatory cytokine production. Moreover, animals treated 35 with anti-DC-ASGPR-MOG experienced a rise of MOG-specific CD4+CD25+FOXP3+CD39+ 36 regulatory T cells as well as a TGFb1, TGFb2 and IL-8 upsurge after rhMOG re-immunization. 37Our results indicate that the pathogenicity of autoantibodies directed to MOG is mitigated in the 38 presence of MOG-specific regulatory lymphocytes. This vaccination scheme appears suitable to 39 treat relapsing autoimmune diseases with identified autoantigens such as that harboring anti-40 MOG or anti-AQP4 autoantibodies. 41 42

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“…23,24 Interestingly, CD163overexpressing macrophages inhibit LPS-induced inflammation in vitro. 25 Furuhashi et al. also found that CD163-expressing macrophages are associated with IL-10 production as an anti-inflammatory cytokine in anti-GBM glomerulonephritis rat.…”

Section: Introductionmentioning

confidence: 95%

α1-Acid Glycoprotein Attenuates Adriamycin-Induced Nephropathy via CD163 Expressing Macrophage Induction

et al. 2020

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Background: Recent clinical studies have shown that proteinuria is a critical factor in the progression of chronic kidney disease (CKD) and onset of cardiovascular disease (CVD). Inflammation and infiltration of macrophages into renal tissue are implicated as a cause of proteinuria. α1-acid glycoprotein (AGP), an acute phase plasma protein, is leaked into the urine in the patients with proteinuria. However, the relationship among the urinary leakage of AGP, renal inflammation and proteinuria remains unclear. Methods: Human AGP (hAGP) was exogenously administrated for five consecutive days to adriamycin-induced nephropathy model mice. Results: Adriamycin treatment increased urinary AGP accompanied by decreasing plasma AGP in mice. Exogenous hAGP administration to adriamycin-treated mice suppressed proteinuria, renal histological injury and inflammation. Then, hAGP administration increased renal CD163 expression, a marker of anti-inflammatory macrophages. Similar changes was observed in phorbol 12-myristate 13-acetatedifferentiated THP-1 cells treated with hAGP. Even in the presence of lipopolysaccharide, hAGP treatment increased CD163/IL-10 expression in differentiated THP-1 cells. Conclusions: AGP alleviates proteinuria and renal injury in mice with proteinuric kidney disease via induction of CD163-expressing macrophages with anti-inflammatory function. The results demonstrate that endogenous AGP could work to protect against glomerulus disease. Thus, AGP supplementation could be a possible new therapeutic intervention for patients with glomerular disease.

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Macrophage-specific nanotechnology-driven CD163 overexpression in human macrophages results in an M2 phenotype under inflammatory conditions

Cited by 85 publications

References 60 publications

Dysfunctional network and mutation genes of hypertrophic cardiomyopathy

Dysfunctional network and mutation genes of hypertrophic cardiomyopathy

Targeting MOG to skin macrophages prevents EAE in macaques through TGFβ-induced peripheral tolerance

α1-Acid Glycoprotein Attenuates Adriamycin-Induced Nephropathy via CD163 Expressing Macrophage Induction

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