M2 Macrophages Serve as Critical Executor of Innate Immunity in Chronic Allograft Rejection

Zhang, Hanwen; Li, Zhuonan; Li, Wei

doi:10.3389/fimmu.2021.648539

Cited by 16 publications

(17 citation statements)

References 79 publications

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“…Their role in kidney transplantation is still unclear. M1 macrophages could produce pro-inflammatory cytokines, which were involved in allograft rejection and result in tissue damage and poor graft survival (37).…”

Section: Discussionmentioning

confidence: 99%

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Immune-Related Genes for Predicting Future Kidney Graft Loss: A Study Based on GEO Database

et al. 2022

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ObjectiveWe aimed to identify feature immune-related genes that correlated with graft rejection and to develop a prognostic model based on immune-related genes in kidney transplantation.MethodsGene expression profiles were obtained from the GEO database. The GSE36059 dataset was used as a discovery cohort. Then, differential expression analysis and a machine learning method were performed to select feature immune-related genes. After that, univariate and multivariate Cox regression analyses were used to identify prognosis-related genes. A novel Riskscore model was built based on the results of multivariate regression. The levels of these feature genes were also confirmed in an independent single-cell dataset and other GEO datasets.Results15 immune-related genes were expressed differently between non-rejection and rejection kidney allografts. Those differentially expressed immune-related genes (DE-IRGs) were mainly associated with immune-related biological processes and pathways. Subsequently, a 5-immune-gene signature was constructed and showed favorable predictive results in the GSE21374 dataset. Recipients were divided into the high-risk and low-risk groups according to the median value of RiskScore. The GO and KEGG analysis indicated that the differentially expressed genes (DEGs) between high-risk and low-risk groups were mainly involved in inflammatory pathways, chemokine-related pathways, and rejection-related pathways. Immune infiltration analysis demonstrated that RiskScore was potentially related to immune infiltration. Kaplan-Meier survival analysis suggested that recipients in the high-risk group had poor graft survival. AUC values of 1- and 3-year graft survival were 0.804 and 0.793, respectively.ConclusionOur data suggest that this immune-related prognostic model had good sensitivity and specificity in predicting the 1- and 3-year kidney graft survival and might act as a useful tool for predicting kidney graft loss.

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Section: Discussionmentioning

confidence: 99%

“…M2 macrophages play important roles in anti-inflammation in allograft rejection. However, M2 macrophages are reported to contribute to fibrosis, leading to poor long-term graft survival (37). Moreover, macrophages are associated with graft vasculopathy, but the phenotypes remain unidentified (38).…”

Section: Discussionmentioning

confidence: 99%

Immune-Related Genes for Predicting Future Kidney Graft Loss: A Study Based on GEO Database

et al. 2022

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“…While both M1 and M2 can clear dead cells, proinflammatory macrophages are crucial for clearing dead cell debris at the early stage of heart injury (14). In contrast, antiinflammatory macrophages facilitate the resolution of inflammation and boost the repairing of injured cardiac tissue (15). As a matter of fact, recent studies have revealed that proinflammatory M1-like polarization is enhanced, whereas antiinflammatory M2-like response is inhibited in diabetic hearts, resulting in cardiac inflammation and contractile dysfunction (16).…”

Section: Introductionmentioning

confidence: 99%

Loss of Lipocalin 10 Exacerbates Diabetes-Induced Cardiomyopathy via Disruption of Nr4a1-Mediated Anti-Inflammatory Response in Macrophages

Li²,

Huang³

et al. 2022

Front. Immunol.

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Metabolic disorders (i.e., hyperglycemia, hyperlipidemia, and hyperinsulinemia) cause increased secretion of inflammatory cytokines/chemokines, leading to gradual loss of cardiac resident macrophage population and increased accumulation of inflammatory monocytes/macrophages in the heart. Such self-perpetuating effect may contribute to the development of cardiomyopathy during diabetes. Recent meta-analysis data reveal that lipocalin 10 (Lcn10) is significantly downregulated in cardiac tissue of patients with heart failure but is increased in the blood of septic patients. However, the functional role of Lcn10 in cardiac inflammation triggered by metabolic disorders has never been investigated. In this study, we demonstrate that the expression of Lcn10 in macrophages was significantly decreased under multiple metabolic stress conditions. Furthermore, Lcn10-null macrophages exhibited pro-inflammatory phenotype in response to inflammation stimuli. Next, using a global Lcn10-knockout (KO) mouse model to induce type-2 diabetes (T2D), we observed that loss of Lcn10 promoted more pro-inflammatory macrophage infiltration into the heart, compared to controls, leading to aggravated insulin resistance and impaired cardiac function. Similarly, adoptive transfer of Lcn10-KO bone marrow cells into X-ray irradiated mice displayed higher ratio of pro-/anti-inflammatory macrophages in the heart and worsened cardiac function than those mice received wild-type (WT) bone marrows upon T2D conditions. Mechanistically, RNA-sequencing analysis showed that Nr4a1, a nuclear receptor known to have potent anti-inflammatory effects, is involved in Lcn10-mediated macrophage activation. Indeed, we found that nuclear translocation of Nr4a1 was disrupted in Lcn10-KO macrophages upon stimulation with LPS + IFNγ. Accordingly, treatment with Cytosporone B (CsnB), an agonist of Nr4a1, attenuated the pro-inflammatory response in Lcn10-null macrophages and partially improved cardiac function in Lcn10-KO diabetic mice. Together, these findings indicate that loss of Lcn10 skews macrophage polarization to pro-inflammatory phenotype and aggravates cardiac dysfunction during type-2 diabetes through the disruption of Nr4a1-mediated anti-inflammatory signaling pathway in macrophages. Therefore, reduction of Lcn10 expression observed in diabetic macrophages may be responsible for the pathogenesis of diabetes-induced cardiac dysfunction. It suggests that Lcn10 might be a potential therapeutic factor for diabetic heart failure.

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“…Conservative treatment and surgical resection are no longer therapeutic options for many patients with end-stage and acute liver disease, and liver transplantation provides the only remaining opportunity. However, ischaemia-reperfusion injury (IRI) during surgery not only limits the utilization of many donor livers, but also severely restricts the prognosis of liver transplant patients (1)(2)(3). IRI is caused by the accumulation of inflammatory cytokines in the donor liver due to ischemia and hypoxia during perfusion Original Article Itaconic acid facilitates inflammation abatement and alleviates liver ischemia-reperfusion injury by inhibiting NF-κB/NLRP3/ caspase-1 inflammasome axis via organ preservation fluid after isolation.…”

Section: Introductionmentioning

confidence: 99%

“…Currently, emphasis in research on inflammatory diseases is shifting to the receding phase of inflammation. Studies have shown impaired inflammatory regression is the basis for the pathogenesis of many immune diseases and promoting regression can facilitate the restoration of immune homeostasis and mitigate the progression of inflammatory disease, providing better results than traditional "anti-inflammatory" treatment (3,9,11).…”

Section: Introductionmentioning

confidence: 99%

Itaconic acid facilitates inflammation abatement and alleviates liver ischemia-reperfusion injury by inhibiting NF-κB/NLRP3/caspase-1 inflammasome axis

Ma¹,

Xing²,

Pei³

et al. 2022

Ann Transl Med

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Background: Ischemia-reperfusion injury (IRI) severely limits the efficacy and donor source of liver transplantation, and the crucial step in alleviating it is to control inflammation. Itaconic acid is a metabolite produced by intrinsic immune cells (especially macrophages) in the inflammatory state and can promote inflammation subsidence. However, its role in liver ischemia-reperfusion is insufficiently clarified.Methods: A mouse liver ischemia-reperfusion model was constructed, and blood and liver tissue samples were collected by sequential euthanasia of mice at pre-set time points. Liver function and inflammatory factor concentrations were measured, and HE staining was conducted. In the hypoxia-reoxygenation model, proteins were collected at pre-set time points, and the expression of NF-κB pathway-associated protein and its downstream inflammation-associated protein NLRP3 and caspase-1 were detected by Western blot, immunohistochemistry, and immunofluorescence. The level of P-P65 in the nucleus was detected by immunofluorescence.Results: In the liver ischemia-reperfusion model, liver function and inflammatory factors were dynamically varied with reperfusion time in mice, and itaconic acid significantly modified liver function and inflammatory status during this process. NF-κB pathway activity was dynamically varied during hypoxia-reoxygenation, and itaconic acid significantly inhibited the activity of the pathway and significantly suppressed the expression of its downstream inflammation-related proteins.Conclusions: Itaconic acid inhibits NF-κB pathway activation and reduces the accumulation of P-P65 in the nucleus. In turn, this reduces NLRP3 and caspase-1 expression of downstream inflammation-related proteins, promotes inflammation regression, and attenuates liver IRI.

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M2 Macrophages Serve as Critical Executor of Innate Immunity in Chronic Allograft Rejection

Cited by 16 publications

References 79 publications

Immune-Related Genes for Predicting Future Kidney Graft Loss: A Study Based on GEO Database

Immune-Related Genes for Predicting Future Kidney Graft Loss: A Study Based on GEO Database

Loss of Lipocalin 10 Exacerbates Diabetes-Induced Cardiomyopathy via Disruption of Nr4a1-Mediated Anti-Inflammatory Response in Macrophages

Itaconic acid facilitates inflammation abatement and alleviates liver ischemia-reperfusion injury by inhibiting NF-κB/NLRP3/caspase-1 inflammasome axis

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