Macrophage Polarization and Its Role in Liver Disease

Wang, Cheng; Ma, Cheng; Gong, Lihong; Guo, Yuqin; Fu, Ke; Zhang, Yafang; Zhou, Honglin; Li, Yunxia

doi:10.3389/fimmu.2021.803037

Cited by 265 publications

(228 citation statements)

References 295 publications

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“…The production of another nine chemokines, including CCL1, CCL7, CCL17 and others, was decreased once N-SREBP was overexpressed ( Figure 4H ). However, the production of IFNγ, IL-4 and IL-10, which are canonical cytokines that stimulate M1 or M2 polarization ( Wang et al, 2021 ), as well as 10 other kinds of cytokines, showed no significant conversion between the eGFP- and N-SREBP-overexpressing groups ( Figure 4I ). These data clarified that SREBP could promote the secretion of various inflammatory cytokines in macrophages to fight HTNV infection.…”

Section: Resultsmentioning

confidence: 99%

“…The classical inflammatory activation pattern of macrophages (M1 polarization) or monocytes (M1-like monocytes), which is stimulated by host Th1-type cytokines (such as interferon-γ/IFNγ and tumor necrosis factor-α/TNFα) or pathogen-associated molecular patterns (PAMPs) via JAK/STAT, NF-κB or pattern-recognition receptor (PRR)-mediated signaling, maintains the potential ability of the immune system to restrict viral infection and promote virus clearance by initiating a robust interferon-centered inflammation response, the dysregulation of which triggers a cytokine storm and aggravates host immunopathological injury ( McNab et al, 2015 ; Merad and Martin, 2020 ; McGonagle et al, 2021 ). Alternatively, macrophages can be M2-polarized by Th2-type cytokines (such as IL-4 and IL-10), which promote the resolution of inflammatory responses and assist in tissue repair ( Wang et al, 2021 ). It has been reported that hantavirus (strain no.…”

Section: Introductionmentioning

confidence: 99%

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LncRNA NEAT1 Potentiates SREBP2 Activity to Promote Inflammatory Macrophage Activation and Limit Hantaan Virus Propagation

Yang

Yong

et al. 2022

Front. Microbiol.

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As the global prototypical zoonotic hantavirus, Hantaan virus (HTNV) is prevalent in Asia and is the leading causative agent of severe hemorrhagic fever with renal syndrome (HFRS), which has profound morbidity and mortality. Macrophages are crucial components of the host innate immune system and serve as the first line of defense against HTNV infection. Previous studies indicated that the viral replication efficiency in macrophages determines hantavirus pathogenicity, but it remains unknown which factor manipulates the macrophage activation pattern and the virus-host interaction process. Here, we performed the transcriptomic analysis of HTNV-infected mouse bone marrow-derived macrophages and identified the long noncoding RNA (lncRNA) nuclear enriched abundant transcript 1 (NEAT1), especially the isoform NEAT1-2, as one of the lncRNAs that is differentially expressed at the early phase. Based on coculture experiments, we revealed that silencing NEAT1-2 hinders inflammatory macrophage activation and facilitates HTNV propagation, while enhancing NEAT1-2 transcription effectively restrains viral replication. Furthermore, sterol response element binding factor-2 (SREBP2), which controls the cholesterol metabolism process, was found to stimulate macrophages by promoting the production of multiple inflammatory cytokines upon HTNV infection. NEAT1-2 could potentiate SREBP2 activity by upregulating Srebf1 expression and interacting with SREBP2, thus stimulating inflammatory macrophages and limiting HTNV propagation. More importantly, we demonstrated that the NEAT1-2 expression level in patient monocytes was negatively correlated with viral load and HFRS disease progression. Our results identified a function and mechanism of action for the lncRNA NEAT1 in heightening SREBP2-mediated macrophage activation to restrain hantaviral propagation and revealed the association of NEAT1 with HFRS severity.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

LncRNA NEAT1 Potentiates SREBP2 Activity to Promote Inflammatory Macrophage Activation and Limit Hantaan Virus Propagation

Yang

Yong

et al. 2022

Front. Microbiol.

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“…Clinical relevance analysis also indicated that high expression of CCL15 or the M2-like macrophage marker CD163 predict a poor prognosis of HCC and the combined predictive value of CCL15 and CD163 in the prognosis is superior to that using either marker alone. Currently, macrophage polarization involves a variety of molecular mechanisms, including TLR4/NF-κB, JAK/STATS, TGF-β/SMADS, PPARγ, NOTCH and microRNA signaling pathways 56 , however, the detailed mechanism driving M2-like macrophages by CCL15 will be our future work.…”

Section: Discussionmentioning

confidence: 99%

Spatial maps of hepatocellular carcinoma transcriptomes reveal spatial expression patterns in tumor immune microenvironment

Wang¹,

Yuan²,

Jiang³

et al. 2022

Theranostics

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Rationale: Hepatocellular carcinoma (HCC) is a highly heterogeneous and malignant disease with the complex immune microenvironment, which ultimately influence clinic outcomes of patients. However, the spatial expression patterns of diverse immune cells among tumor microenvironment remain to be further deciphered. Methods: Spatial transcriptomics sequencing (ST) was implemented on two portions of HCC specimens. Differentially expressed genes, cell cycle phases, epithelial-mesenchymal features, pseudo-time and immune infiltration analysis were applied to demonstrate the intratumor heterogeneity and define the specific immune-related regions, and the results were further validated by a second analysis on another ST study. In vitro and in vivo experiments were conducted to confirm the functional mechanisms of key molecules such as CCL15, CCL19 and CCL21. Clinical tissue samples were used to assess their potential prognostic and therapeutic values. Results: Totally, 7553 spots were categorized into 15 subsets by hierarchical clustering, and malignant subsets with intratumor heterogeneity phenotypes were identified. Spatial heterogeneity from distinct sectors highlights specific chemokines: CCL15 is remarkable in the core region of the carcinoma sector and facilitates the immunosuppressive microenvironment by recruiting and polarizing M2-like macrophages in vitro and in vivo ; High expression of CCL15 and CD163 respectively predicts poor prognosis of HCC patients, and the combined application of them has better predictive value. CCL19 and CCL21, sharing similar spatial expression patterns, are highly-correlated and prominent in the immune infiltration enrichment and recruit CD3 + T cells and CD20 + B cells to inhibit the growth of HCC, indicating a good prognosis of HCC patients. Conclusions: Taken together, our studies preliminarily reveal intratumor heterogeneity of HCC based on ST techniques and unravel the previously unexplored spatial expression patterns in the immune microenvironment. We also highlight the clinical significance and spatial discrepancy of key molecules, providing novel insight for further developing therapeutic strategies in HCC.

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“…For example, KCs are activated into M1 phenotype by lipopolysaccharide (LPS), IFN-gamma or M-CSF, characterizing by highly expressing pro-inflammatory genes IL1B, TNFα and iNOS ( 36 ). While IL4 or GM-CSF may polarize KCs into M2 type that highly express ARG1, IL10 and MRC1 ( 27 , 28 ). However, later studies found that M1-M2 dichotomy is insufficient to classify KCs, especially in liver injury ( 37 , 38 ).…”

Section: Kc In Homeostasismentioning

confidence: 99%

Heterogeneity and Function of Kupffer Cells in Liver Injury

Chang

2022

Front. Immunol.

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Kupffer cells (KCs) are key regulators of liver immunity composing the principal part of hepatic macrophages even body tissue macrophages. They reside in liver sinusoids towards portal vein. The micro-environment shapes KCs unique immunosuppressive features and functions. KCs express specific surface markers that distinguish from other liver macrophages. By engulfing gut-derived foreign products and apoptotic cells without triggering excessive inflammation, KCs maintain homeostasis of liver and body. Heterogeneity of KCs has been identified in different studies. In terms of the origin, adult KCs are derived from progenitors of both embryo and adult bone marrow. Embryo-derived KCs compose the majority of KCs in healthy and maintain by self-renewal. Bone marrow monocytes replenish massively when embryo-derived KC proliferation are impaired. The phenotype of KCs is also beyond the traditional dogma of M1-M2. Functionally, KCs play central roles in pathogenesis of acute and chronic liver injury. They contribute to each pathological stage of liver disease. By initiating inflammation, regulating fibrosis, cirrhosis and tumor cell proliferation, KCs contribute to the resolution of liver injury and restoration of tissue architecture. The underlying mechanism varied by damage factors and pathology. Understanding the characteristics and functions of KCs may provide opportunities for the therapy of liver injury. Herein, we attempt to afford insights on heterogeneity and functions of KCs in liver injury using the existing findings.

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Macrophage Polarization and Its Role in Liver Disease

Cited by 265 publications

References 295 publications

LncRNA NEAT1 Potentiates SREBP2 Activity to Promote Inflammatory Macrophage Activation and Limit Hantaan Virus Propagation

LncRNA NEAT1 Potentiates SREBP2 Activity to Promote Inflammatory Macrophage Activation and Limit Hantaan Virus Propagation

Spatial maps of hepatocellular carcinoma transcriptomes reveal spatial expression patterns in tumor immune microenvironment

Heterogeneity and Function of Kupffer Cells in Liver Injury

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