Your search keyword '"monocyte-derived macrophages"' showing total 828 results

1. Transcriptomic identification of genes associated with thrombosis and coagulation in lipopolysaccharideexposed bovine monocyte-derived macrophages.

Author

Cohen, Hannah R., DeCourcey, Michelle A., Davis, William C., and de Souza, Cleverson

Abstract

OBJECTIVE: The OBJECTIVE: of this study was to investigate the differential expression of genes associated with coagulation in bovine monocyte-derived macrophages (MoMF) exposed to lipopolysaccharide (LPS) in vitro. We hypothesized that MoMF stimulated with LPS would have upregulation of procoagulant genes and downregulation of genes protecting against coagulation. METHODS: MoMF were isolated from Holstein steers and exposed to Escherichia coli-derived LPS or a control for 3 hours. We used transcriptomics (RNA sequencing) to characterize the differential expression of genes associated with coagulation in the LPS-exposed MoMF relative to the control group. 1,602 genes were upregulated and 1,209 genes downregulated 3 hours after exposure to LPS. Monocyte-derived macrophages exposed to LPS displayed statistically significant upregulation of 4 proinflammatory genes, 2 antiinflammatory genes, 8 genes involved in promoting coagulation, and 5 genes considered protective against coagulation. There was significant downregulation of 1 gene involved in the promotion of coagulation. CONCLUSIONS Our RESULTS: showed increased expression of most genes investigated promoting and protecting against coagulation and increased expression of proinflammatory and anti-inflammatory genes. These findings suggest that MoMF exhibit a multifaceted response in the early response to LPS, promoting and protecting against excessive coagulation. This multifaceted response highlights the interplay between different pathways involved in early sepsis. CLINICAL RELEVANCE: Our data demonstrate the utility of using MoMF as a model system to investigate sepsis-associated coagulopathies. These insights into the early transcriptomic changes in response to LPS may help guide future research on the development of treatment modalities or diagnostic tests for patients with sepsis. [ABSTRACT FROM AUTHOR]

Published

2024

2. Single-Cell RNA Sequencing Reveals Monocyte-Derived Interstitial Macrophages with a Pro-Fibrotic Phenotype in Bleomycin-Induced Pulmonary Fibrosis.

Author

Wang, Shunli, Li, Jie, Wu, Caixia, Lei, Zhengyao, Wang, Tong, Huang, Xinxin, Zhang, Suxia, Liu, Yuting, Bi, Xiaohan, Zheng, Fanshuo, Zhu, Xuyou, Huang, Ziling, and Yi, Xianghua

Subjects

*IDIOPATHIC pulmonary fibrosis, *PLATELET-derived growth factor, *PULMONARY fibrosis, *EXTRACELLULAR matrix, *GENE expression profiling

Abstract

Idiopathic pulmonary fibrosis (IPF) is a chronic, progressive lung disease with limited effective therapies. Interstitial macrophages (IMs), especially those derived from monocytes, play an unknown role in IPF pathogenesis. By using single-cell RNA sequencing (scRNA-seq), bleomycin (BLM)-induced pulmonary fibrosis mouse lungs were analyzed to characterize the cellular landscape and heterogeneity of macrophages in this model. scRNA-seq was used to identify distinct interstitial macrophage subpopulations in fibrotic lungs, with monocyte-derived macrophages exhibiting a pro-fibrotic gene expression profile enriched in wound healing, extracellular matrix (ECM) remodeling, and pro-fibrotic cytokine production functions. A pseudotime analysis revealed that IMs originated from monocytes and differentiated along a specific trajectory. A cell–cell communication analysis demonstrated strong interactions between monocyte-derived interstitial macrophages (Mo-IMs) and fibroblasts through the transforming growth factor beta (TGFβ), secreted phosphoprotein 1 (SPP1), and platelet-derived growth factor (PDGF) signaling pathways. Flow cytometry validated the presence and expansion of Mo-IMs subpopulations in BLM-treated mice. This study reveals the cellular heterogeneity and developmental trajectory of lung macrophages in early BLM-induced pulmonary fibrosis, highlighting the crucial role of Mo-IMs with a pro-fibrotic phenotype in IPF pathogenesis via interactions with fibroblasts. Targeting these specific macrophage subpopulations and associated signaling pathways may provide novel therapeutic strategies for IPF. [ABSTRACT FROM AUTHOR]

Published

2024

3. The Therapeutic Potential of Exosomes vs. Matrix-Bound Nanovesicles from Human Umbilical Cord Mesenchymal Stromal Cells in Osteoarthritis Treatment.

Author

Klyucherev, Timofey O., Peshkova, Maria A., Revokatova, Daria P., Serejnikova, Natalia B., Fayzullina, Nafisa M., Fayzullin, Alexey L., Ershov, Boris P., Khristidis, Yana I., Vlasova, Irina I., Kosheleva, Nastasia V., Svistunov, Andrey A., and Timashev, Peter S.

Subjects

*OSTEOARTHRITIS, *KNEE osteoarthritis, *EXTRACELLULAR matrix, *LABORATORY rats, *EXTRACELLULAR vesicles

Abstract

Osteoarthritis (OA) is a degenerative joint disease with limited therapeutic options, where inflammation plays a critical role in disease progression. Extracellular vesicles (EV) derived from mesenchymal stromal cells (MSC) have shown potential as a therapeutic approach for OA by modulating inflammation and alleviating degenerative processes in the joint. This study evaluated the therapeutic effects for the treatment of OA of two types of EV—exosomes and matrix-bound nanovesicles (MBV)—both derived from the human umbilical cord MSC (UC-MSC) via differential ultracentrifugation. Different phenotypes of human monocyte-derived macrophages (MDM) were used to study the anti-inflammatory properties of EV in vitro, and the medial meniscectomy-induced rat model of knee osteoarthritis (MMx) was used in vivo. The study found that both EV reduced pro-inflammatory cytokines IL-6 and TNF-α in MDM. However, exosomes showed superior results, preserving the extracellular matrix (ECM) of hyaline cartilage, and reducing synovitis more effectively than MBVs. Additionally, exosomes downregulated inflammatory markers (TNF-α, iNOS) and increased Arg-1 expression in macrophages and synovial fibroblasts, indicating a stronger anti-inflammatory effect. These results suggest UC-MSC exosomes as a promising therapeutic option for OA, with the potential for modulating inflammation and promoting joint tissue regeneration. [ABSTRACT FROM AUTHOR]

Published

2024

4. Induction of the antiviral factors APOBEC3A and RSAD2 upon CCL2 neutralization in primary human macrophages involves NF-κB, JAK/STAT, and gp130 signaling.

Author

Covino, Daniela Angela, Farina, Iole, Catapano, Laura, Sozzi, Silvia, Spadaro, Francesca, Cecchetti, Serena, Purificato, Cristina, Gauzzi, Maria Cristina, and Fantuzzi, Laura

Subjects

REVERSE transcriptase polymerase chain reaction, NATURAL immunity, LIFE cycles (Biology), CELLULAR signal transduction, WESTERN immunoblotting

Abstract

The CCL2/CC chemokine receptor 2 axis plays key roles in the pathogenesis of HIV-1 infection. We previously reported that exposure of monocyte-derived macrophages to CCL2 neutralizing antibody (αCCL2 Ab) restricted HIV-1 replication at postentry steps of the viral life cycle. This effect was associated with induction of transcripts coding for innate antiviral proteins, including APOBEC3A and RSAD2. This study aimed at identifying the signaling pathways involved in induction of these factors by CCL2 blocking in monocyte-derived macrophages. Through a combination of pharmacologic inhibition, quantitative reverse transcription polymerase chain reaction, Western blotting, and confocal laser-scanning microscopy, we demonstrated that CCL2 neutralization activates the canonical NF-κB and JAK/STAT pathways, as assessed by time-dependent phosphorylation of IκB, STAT1, and STAT3 and p65 nuclear translocation. Furthermore, pharmacologic inhibition of IκB kinase and JAKs strongly reduced APOBEC3A and RSAD2 transcript accumulation elicited by αCCL2 Ab treatment. Interestingly, exposure of monocyte-derived macrophages to αCCL2 Ab resulted in induction of IL-6 family cytokines, and interference with glycoprotein 130, the common signal-transducing receptor subunit shared by these cytokines, inhibited APOBEC3A and RSAD2 upregulation triggered by CCL2 neutralization. These results provide novel insights into the signal transduction pathways underlying the activation of innate responses triggered by CCL2 neutralization in macrophages. Since this response was found to be associated with protective antiviral effects, the new findings may help design innovative therapeutic approaches targeting CCL2 to strengthen host innate immunity. [ABSTRACT FROM AUTHOR]

Published

2024

5. From monocyte‐derived macrophages to resident macrophages—how metabolism leads their way in cancer

Author

Ummi Ammarah, Andreia Pereira‐Nunes, Marcello Delfini, and Massimiliano Mazzone

Subjects

cancer metabolism, immunometabolism, monocyte‐derived macrophages, tissue‐resident macrophages, tumor microenvironment, tumor‐associated macrophages, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Macrophages are innate immune cells that play key roles during both homeostasis and disease. Depending on the microenvironmental cues sensed in different tissues, macrophages are known to acquire specific phenotypes and exhibit unique features that, ultimately, orchestrate tissue homeostasis, defense, and repair. Within the tumor microenvironment, macrophages are referred to as tumor‐associated macrophages (TAMs) and constitute a heterogeneous population. Like their tissue resident counterpart, TAMs are plastic and can switch function and phenotype according to the niche‐derived stimuli sensed. While changes in TAM phenotype are known to be accompanied by adaptive alterations in their cell metabolism, it is reported that metabolic reprogramming of macrophages can dictate their activation state and function. In line with these observations, recent research efforts have been focused on defining the metabolic traits of TAM subsets in different tumor malignancies and understanding their role in cancer progression and metastasis formation. This knowledge will pave the way to novel therapeutic strategies tailored to cancer subtype‐specific metabolic landscapes. This review outlines the metabolic characteristics of distinct TAM subsets and their implications in tumorigenesis across multiple cancer types.

Published

2024

6. Spatial and phenotypic heterogeneity of resident and monocyte-derived macrophages during inflammatory exacerbations leading to pulmonary fibrosis.

Author

Moos, Philip J., Cheminant, Jenna R., Cowman, Sophie, Noll, Jessica, Qiuming Wang, Musci, Teresa, and Venosa, Alessandro

Subjects

ALVEOLAR macrophages, PULMONARY fibrosis, DISEASE exacerbation, EXTRACELLULAR matrix, INTERSTITIAL lung diseases

Abstract

Introduction: Genetic mutations in critical nodes of pulmonary epithelial function are linked to the pathogenesis of pulmonary fibrosis (PF) and other interstitial lung diseases. The slow progression of these pathologies is often intermitted and accelerated by acute exacerbations, complex non-resolving cycles of inflammation and parenchymal damage, resulting in lung function decline and death. Excess monocyte mobilization during the initial phase of an acute exacerbation, and their long-term persistence in the lung, is linked to poor disease outcome. Methods: The present work leverages a clinical idiopathic PF dataset and a murine model of acute inflammatory exacerbations triggered by mutation in the alveolar type-2 cell-restricted Surfactant Protein-C [SP-C] gene to spatially and phenotypically define monocyte/macrophage changes in the fibrosing lung. Results: SP-C mutation triggered heterogeneous CD68+ macrophage activation, with highly active peri-injured cells relative to those sampled from fully remodeled and healthy regions. Ingenuity pathway analysis of sorted CD11b-SigF+CD11c+ alveolar macrophages defined asynchronous activation of extracellular matrix reorganization, cellular mobilization, and Apolipoprotein E (Apoe) signaling in the fibrosing lung. Cell-cell communication analysis of single cell sequencing datasets predicted pro-fibrogenic signaling (fibronectin/Fn1, osteopontin/Spp1, and Tgfb1) emanating fromTrem2/TREM2+ interstitial macrophages. These cells also produced a distinct lipid signature from alveolar macrophages and monocytes, characterized by Apoe expression. Mono- and di-allelic genetic deletion of ApoE in SP-C mutant mice had limited impact on inflammation and mortality up to 42 day after injury. Discussion: Together, these results provide a detailed spatio-temporal picture of resident, interstitial, and monocyte-derived macrophages during SP-C induced inflammatory exacerbations and end-stage clinical PF, and propose ApoE as a biomarker to identify activated macrophages involved in tissue remodeling. [ABSTRACT FROM AUTHOR]

Published

2024

7. From monocyte‐derived macrophages to resident macrophages—how metabolism leads their way in cancer.

Author

Ammarah, Ummi, Pereira‐Nunes, Andreia, Delfini, Marcello, and Mazzone, Massimiliano

Abstract

Macrophages are innate immune cells that play key roles during both homeostasis and disease. Depending on the microenvironmental cues sensed in different tissues, macrophages are known to acquire specific phenotypes and exhibit unique features that, ultimately, orchestrate tissue homeostasis, defense, and repair. Within the tumor microenvironment, macrophages are referred to as tumor‐associated macrophages (TAMs) and constitute a heterogeneous population. Like their tissue resident counterpart, TAMs are plastic and can switch function and phenotype according to the niche‐derived stimuli sensed. While changes in TAM phenotype are known to be accompanied by adaptive alterations in their cell metabolism, it is reported that metabolic reprogramming of macrophages can dictate their activation state and function. In line with these observations, recent research efforts have been focused on defining the metabolic traits of TAM subsets in different tumor malignancies and understanding their role in cancer progression and metastasis formation. This knowledge will pave the way to novel therapeutic strategies tailored to cancer subtype‐specific metabolic landscapes. This review outlines the metabolic characteristics of distinct TAM subsets and their implications in tumorigenesis across multiple cancer types. [ABSTRACT FROM AUTHOR]

Published

2024

8. Effects of carbon black particles on human monocyte-derived macrophages: type-dependent pro-inflammatory activation in vitro

Author

Pajarskienė, Justina, Vailionytė, Agnė, Uogintė, Ieva, Byčenkienė, Steigvilė, Jonavičė, Ugnė, Uzielienė, Ilona, Bagdonas, Edvardas, and Aldonytė, Rūta

Published

2024

9. Effects of Akt Activator SC79 on Human M0 Macrophage Phagocytosis and Cytokine Production.

Author

Lee, Robert J., Adappa, Nithin D., and Palmer, James N.

Subjects

*BITTERNESS (Taste), *PATTERN perception receptors, *PHAGOCYTOSIS, *SMALL molecules, *EPITHELIAL cells, *MACROPHAGES, *FLUORESCENT probes, *COMPLEMENT receptors

Abstract

Akt is an important kinase in metabolism. Akt also phosphorylates and activates endothelial and neuronal nitric oxide (NO) synthases (eNOS and nNOS, respectively) expressed in M0 (unpolarized) macrophages. We showed that e/nNOS NO production downstream of bitter taste receptors enhances macrophage phagocytosis. In airway epithelial cells, we also showed that the activation of Akt by a small molecule (SC79) enhances NO production and increases levels of nuclear Nrf2, which reduces IL-8 transcription during concomitant stimulation with Toll-like receptor (TLR) 5 agonist flagellin. We hypothesized that SC79's production of NO in macrophages might likewise enhance phagocytosis and reduce the transcription of some pro-inflammatory cytokines. Using live cell imaging of fluorescent biosensors and indicator dyes, we found that SC79 induces Akt activation, NO production, and downstream cGMP production in primary human M0 macrophages. This was accompanied by a reduction in IL-6, IL-8, and IL-12 production during concomitant stimulation with bacterial lipopolysaccharide, an agonist of pattern recognition receptors including TLR4. Pharmacological inhibitors suggested that this effect was dependent on Akt and Nrf2. Together, these data suggest that several macrophage immune pathways are regulated by SC79 via Akt. A small-molecule Akt activator may be useful in some infection settings, warranting future in vivo studies. [ABSTRACT FROM AUTHOR]

Published

2024

10. Nano(bio)Materials Do Not Affect Macrophage Phenotype—A Study Conducted by the REFINE Project.

Author

David, Christopher A. W., Vermeulen, Jolanda P., Gioria, Sabrina, Vandebriel, Rob J., and Liptrott, Neill J.

Subjects

*NANOSCIENCE, *MACROPHAGES, *PHENOTYPES, *MEDICAL supplies, *STANDARD operating procedure

Abstract

Macrophages are well known for their involvement in the biocompatibility, as well as biodistribution, of nano(bio)materials. Although there are a number of rodent cell lines, they may not fully recapitulate primary cell responses, particularly those of human cells. Isolation of tissue-resident macrophages from humans is difficult and may result in insufficient cells with which to determine the possible interaction with nano(bio)materials. Isolation of primary human monocytes and differentiation to monocyte-derived macrophages may provide a useful tool with which to further study these interactions. To that end, we developed a standard operating procedure for this differentiation, as part of the Regulatory Science Framework for Nano(bio)material-based Medical Products and Devices (REFINE) project, and used it to measure the secretion of bioactive molecules from M1 and M2 differentiated monocytes in response to model nano(bio)materials, following an initial assessment of pyrogenic contamination, which may confound potential observations. The SOP was deployed in two partner institutions with broadly similar results. The work presented here shows the utility of this assay but highlights the relevance of donor variability in responses to nano(bio)materials. Whilst donor variability can provide some logistical challenges to the application of such assays, this variability is much closer to the heterogeneous cells that are present in vivo, compared to homogeneous non-human cell lines. [ABSTRACT FROM AUTHOR]

Published

2024

11. Monocyte to macrophage differentiation and changes in cellular redox homeostasis promote cell type-specific HIV latency reactivation.

Author

Blanco, Alexandra, Coronado, Robert A., Arun, Neha, Ma, Kelly, Dar, Roy D., and Kieffer, Collin

Subjects

*HIV-positive persons, *PROTEIN kinase C, *HIV, *CLONE cells, *HOMEOSTASIS, *MACROPHAGES, *CURCUMIN

Abstract

HIV latency regulation in monocytes and macrophages can vary according to signals directing differentiation, polarization, and function. To investigate these processes, we generated an HIV latency model in THP-1 monocytes and showed differential levels of HIV reactivation among clonal populations. Monocyte-to-macrophage differentiation of HIV-infected primary human CD14+ and THP-1 cells induced HIV reactivation and showed that virus production increased concomitant with macrophage differentiation. We applied the HIV-infected THP-1 monocyte-to-macrophage (MLat) model to assess the biological mechanisms regulating HIV latency dynamics during monocyte-to-macrophage differentiation. We pinpointed protein kinase C signaling pathway activation and Cyclin T1 upregulation as inherent differentiation mechanisms that regulate HIV latency reactivation. Macrophage polarization regulated latency, revealing proinflammatory M1 macrophages suppressed HIV reactivation while anti-inflammatory M2 macrophages promoted HIV reactivation. Because macrophages rely on reactive-oxygen species (ROS) to exert numerous cellular functions, we disrupted redox pathways and found that inhibitors of the thioredoxin (Trx) system acted as latency-promoting agents in T-cells and monocytes, but opposingly acted as latency-reversing agents in macrophages. We explored this mechanism with Auranofin, a clinical candidate for reducing HIV reservoirs, and demonstrated Trx reductase inhibition led to ROS induced NF-κB activity, which promoted HIV reactivation in macrophages, but not in T-cells and monocytes. Collectively, cell type-specific differences in HIV latency regulation could pose a barrier to HIV eradication strategies. [ABSTRACT FROM AUTHOR]

Published

2024

12. The abortive SARS‐CoV‐2 infection of osteoclast precursors promotes their differentiation into osteoclasts.

Author

Sviercz, Franco, Jarmoluk, Patricio, Godoy Coto, Joshua, Cevallos, Cintia, Freiberger, Rosa Nicole, López, Cinthya Alicia Marcela, Ennis, Irene Lucia, Delpino, M. Victoria, and Quarleri, Jorge

Subjects

SARS-CoV-2, BONE resorption, COVID-19, POST-acute COVID-19 syndrome, OSTEOCLASTS

Abstract

The Coronavirus Disease 2019 (COVID‐19) pandemic has resulted in the loss of millions of lives, although a majority of those infected have managed to survive. Consequently, a set of outcomes, identified as long COVID, is now emerging. While the primary target of severe acute respiratory syndrome coronavirus 2 (SARS‐CoV‐2) is the respiratory system, the impact of COVID‐19 extends to various body parts, including the bone. This study aims to investigate the effects of acute SARS‐CoV‐2 infection on osteoclastogenesis, utilizing both ancestral and Omicron viral strains. Monocyte‐derived macrophages, which serve as precursors to osteoclasts, were exposed to both viral variants. However, the infection proved abortive, even though ACE2 receptor expression increased postinfection, with no significant impact on cellular viability and redox balance. Both SARS‐CoV‐2 strains heightened osteoclast formation in a dose‐dependent manner, as well as CD51/61 expression and bone resorptive ability. Notably, SARS‐CoV‐2 induced early pro‐inflammatory M1 macrophage polarization, shifting toward an M2‐like profile. Osteoclastogenesis‐related genes (RANK, NFATc1, DC‐STAMP, MMP9) were upregulated, and surprisingly, SARS‐CoV‐2 variants promoted RANKL‐independent osteoclast formation. This thorough investigation illuminates the intricate interplay between SARS‐CoV‐2 and osteoclast precursors, suggesting potential implications for bone homeostasis and opening new avenues for therapeutic exploration in COVID‐19. [ABSTRACT FROM AUTHOR]

Published

2024

13. Spatial and phenotypic heterogeneity of resident and monocyte-derived macrophages during inflammatory exacerbations leading to pulmonary fibrosis

Author

Philip J. Moos, Jenna R. Cheminant, Sophie Cowman, Jessica Noll, Qiuming Wang, Teresa Musci, and Alessandro Venosa

Subjects

alveolar type-2 cell, surfactant protein-C I73T mutant, pulmonary fibrosis, alveolar macrophages, monocyte-derived macrophages, apolipoprotein-E, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionGenetic mutations in critical nodes of pulmonary epithelial function are linked to the pathogenesis of pulmonary fibrosis (PF) and other interstitial lung diseases. The slow progression of these pathologies is often intermitted and accelerated by acute exacerbations, complex non-resolving cycles of inflammation and parenchymal damage, resulting in lung function decline and death. Excess monocyte mobilization during the initial phase of an acute exacerbation, and their long-term persistence in the lung, is linked to poor disease outcome.MethodsThe present work leverages a clinical idiopathic PF dataset and a murine model of acute inflammatory exacerbations triggered by mutation in the alveolar type-2 cell-restricted Surfactant Protein-C [SP-C] gene to spatially and phenotypically define monocyte/macrophage changes in the fibrosing lung.ResultsSP-C mutation triggered heterogeneous CD68+ macrophage activation, with highly active peri-injured cells relative to those sampled from fully remodeled and healthy regions. Ingenuity pathway analysis of sorted CD11b-SigF+CD11c+ alveolar macrophages defined asynchronous activation of extracellular matrix re-organization, cellular mobilization, and Apolipoprotein E (Apoe) signaling in the fibrosing lung. Cell-cell communication analysis of single cell sequencing datasets predicted pro-fibrogenic signaling (fibronectin/Fn1, osteopontin/Spp1, and Tgfb1) emanating from Trem2/TREM2+ interstitial macrophages. These cells also produced a distinct lipid signature from alveolar macrophages and monocytes, characterized by Apoe expression. Mono- and di-allelic genetic deletion of ApoE in SP-C mutant mice had limited impact on inflammation and mortality up to 42 day after injury.DiscussionTogether, these results provide a detailed spatio-temporal picture of resident, interstitial, and monocyte-derived macrophages during SP-C induced inflammatory exacerbations and end-stage clinical PF, and propose ApoE as a biomarker to identify activated macrophages involved in tissue remodeling.

Published

2024

14. GRK2 inhibits Flt-1+ macrophage infiltration and its proangiogenic properties in rheumatoid arthritis

Author

Xuezhi Yang, Yingjie Zhao, Qi Wei, Xuemin Zhu, Luping Wang, Wankang Zhang, Xiaoyi Liu, Jiajie Kuai, Fengling Wang, and Wei Wei

Subjects

GRK2, Monocyte-derived macrophages, Rheumatoid arthritis, PPARγ, Flt-1, Therapeutics. Pharmacology, RM1-950

Abstract

Rheumatoid arthritis (RA) is an autoimmune disease with a complex etiology. Monocyte-derived macrophages (MDMs) infiltration are associated with RA severity. We have reported the deletion of G-protein-coupled receptor kinase 2 (GRK2) reprograms macrophages toward an anti-inflammatory phenotype by recovering G-protein-coupled receptor signaling. However, as more GRK2-interacting proteins were discovered, the GRK2 interactome mechanisms in RA have been understudied. Thus, in the collagen-induced arthritis mouse model, we performed genetic GRK2 deletion using GRK2f/fLyz2-Cre+/− mice. Synovial inflammation and M1 polarization were improved in GRK2f/fLyz2-Cre+/− mice. Supporting experiments with RNA-seq and dual-luciferase reporter assays identified peroxisome proliferator-activated receptor γ (PPARγ) as a new GRK2-interacting protein. We further confirmed that fms-related tyrosine kinase 1 (Flt-1), which promoted macrophage migration to induce angiogenesis, was inhibited by GRK2-PPARγ signaling. Mechanistically, excess GRK2 membrane recruitment in CIA MDMs reduced the activation of PPARγ ligand-binding domain and enhanced Flt-1 transcription. Furthermore, the treatment of mice with GRK2 activity inhibitor resulted in significantly diminished CIA pathology, Flt-1+ macrophages induced-synovial inflammation, and angiogenesis. Altogether, we anticipate to facilitate the elucidation of previously unappreciated details of GRK2-specific intracellular signaling. Targeting GRK2 activity is a viable strategy to inhibit MDMs infiltration, affording a distinct way to control joint inflammation and angiogenesis of RA.

Published

2024

15. SGK3 deficiency in macrophages suppresses angiotensin II–induced cardiac remodeling via regulating Ndufa13–mediated mitochondrial oxidative stress

Author

Ren, Jiayu, Che, Yilin, Li, Heyu, Gao, Haijun, Wang, Yue, Wang, Ying, Su, Hongtong, Li, Zhihan, Li, Jing, and Qu, Peng

Published

2024

16. TNFα: TNFR1 signaling inhibits maturation and maintains the pro-inflammatory programming of monocyte-derived macrophages in murine chronic granulomatous disease.

Author

Gibbings, Sophie L., Haist, Kelsey C., Redente, Elizabeth F., Henson, Peter M., and Bratton, Donna L.

Subjects

CHRONIC granulomatous disease, MACROPHAGES, TUMOR necrosis factors, NADPH oxidase

Abstract

Introduction: Loss of NADPH oxidase activity results in proinflammatory macrophages that contribute to hyperinflammation in Chronic Granulomatous Disease (CGD). Previously, it was shown in a zymosan-induced peritonitis model that gp91phox-/- (CGD) monocyte-derived macrophages (MoMacs) fail to phenotypically mature into pro-resolving MoMacs characteristic of wild type (WT) but retain the ability to do so when placed in the WT milieu. Accordingly, it was hypothesized that soluble factor(s) in the CGD milieu thwart appropriate programming. Methods: We sought to identify key constituents using ex vivo culture of peritoneal inflammatory leukocytes and their conditioned media. MoMac phenotyping was performed via flow cytometry, measurement of efferocytic capacity and multiplex analysis of secreted cytokines. Addition of exogenous TNFa, TNFa neutralizing antibody and TNFR1-/- MoMacs were used to study the role of TNFa: TNFR1 signaling in MoMac maturation. Results: More extensive phenotyping defined normal MoMac maturation and demonstrated failure of maturation of CGD MoMacs both ex vivo and in vivo. Protein components, and specifically TNFa, produced and released by CGD neutrophils and MoMacs into conditioned media was identified as critical to preventing maturation. Exogenous addition of TNFa inhibited WT MoMac maturation, and its neutralization allowed maturation of cultured CGD MoMacs. TNFa neutralization also reduced production of IL-1b, IL-6 and CXCL1 by CGD cells though these cytokines played no role in MoMac programming. MoMacs lacking TNFR1 matured more normally in the CGD milieu both ex vivo and following adoptive transfer in vivo. Discussion: These data lend mechanistic insights into the utility of TNFa blockade in CGD and to other diseases where such therapy has been shown to be beneficial. [ABSTRACT FROM AUTHOR]

Published

2024

17. PEG–Lipid–PLGA Hybrid Particles for Targeted Delivery of Anti-Inflammatory Drugs.

Author

Ismail, Jana, Klepsch, Lea C., Dahlke, Philipp, Tsarenko, Ekaterina, Vollrath, Antje, Pretzel, David, Jordan, Paul M., Rezaei, Kourosh, Czaplewska, Justyna A., Stumpf, Steffi, Beringer-Siemers, Baerbel, Nischang, Ivo, Hoeppener, Stephanie, Werz, Oliver, and Schubert, Ulrich S.

Subjects

*TARGETED drug delivery, *DRUG delivery systems, *HIGH performance liquid chromatography, *ANTI-inflammatory agents, *SCANNING electron microscopy

Abstract

Hybrid nanoparticles (HNPs) were designed by combining a PLGA core with a lipid shell that incorporated PEG–Lipid conjugates with various functionalities (-RGD, -cRGD, -NH2, and -COOH) to create targeted drug delivery systems. Loaded with a neutral lipid orange dye, the HNPs were extensively characterized using various techniques and investigated for their uptake in human monocyte-derived macrophages (MDMs) using FC and CLSM. Moreover, the best-performing HNPs (i.e., HNP-COOH and HNP-RGD as well as HNP-RGD/COOH mixed) were loaded with the anti-inflammatory drug BRP-201 and prepared in two size ranges (dH ~140 nm and dH ~250 nm). The HNPs were examined further for their stability, degradation, MDM uptake, and drug delivery efficiency by studying the inhibition of 5-lipoxygenase (5-LOX) product formation, whereby HNP-COOH and HNP-RGD both exhibited superior uptake, and the HNP-COOH/RGD (2:1) displayed the highest inhibition. [ABSTRACT FROM AUTHOR]

Published

2024

18. Immunity in malignant brain tumors: Tumor entities, role of immunotherapy, and specific contribution of myeloid cells to the brain tumor microenvironment.

Author

Kienzler, Jenny C. and Becher, Burkhard

Subjects

MYELOID cells, TUMOR microenvironment, BRAIN tumors, IMMUNE checkpoint inhibitors, IMMUNITY, TUMOR growth, LIPOCALINS, IPILIMUMAB

Abstract

Malignant brain tumors lack effective treatment, that can improve their poor overall survival achieved with standard of care. Advancement in different cancer treatments has shifted the focus in brain tumor research and clinical trials toward immunotherapy‐based approaches. The investigation of the immune cell landscape revealed a dominance of myeloid cells in the tumor microenvironment. Their exact roles and functions are the subject of ongoing research. Current evidence suggests a complex interplay of tumor cells and myeloid cells with competing functions toward support vs. control of tumor growth. Here, we provide a brief overview of the three most abundant brain tumor entities: meningioma, glioma, and brain metastases. We also describe the field of ongoing immunotherapy trials and their results, including immune checkpoint inhibitors, vaccination studies, oncolytic viral therapy, and CAR‐T cells. Finally, we summarize the phenotypes of microglia, monocyte‐derived macrophages, border‐associated macrophages, neutrophils, and potential novel therapy targets. [ABSTRACT FROM AUTHOR]

Published

2024

19. Systemic Lipopolysaccharide Exposure Exacerbates Choroidal Neovascularization in Mice.

Author

Tsioti, Ioanna, Steiner, Beatrice L., Escher, Pascal, Zinkernagel, Martin S., Benz, Peter M., and Kokona, Despina

Subjects

*LIPOPOLYSACCHARIDES, *NEOVASCULARIZATION, *FLUORESCENCE angiography, *IN situ hybridization, *LABORATORY mice

Abstract

This study aims to investigate the effect of a systemic lipopolysaccharide (LPS) stimulus in the course of laser-induced choroidal neovascularization (CNV) in C57BL/6 J mice. A group of CNV-subjected mice received 1 mg/kg LPS via the tail vein immediately after CNV induction. Mouse eyes were monitored in vivo with fluorescein angiography for 2 weeks. In situ hybridization and flow cytometry were performed in the retina at different time points. LPS led to increased fluorescein leakage 3 days after CNV, correlated with a large influx of monocyte-derived macrophages and increase of pro-inflammatory microglia/macrophages in the retina. Additionally, LPS enhanced Vegfα mRNA expression by Glul-expressing cells but not Aif1 positive microglia/macrophages in the laser lesion. These findings suggest that systemic LPS exposure has transient detrimental effects in the course of CNV through activation of microglia/macrophages to a pro-inflammatory phenotype and supports the important role of these cells in the CNV course. [ABSTRACT FROM AUTHOR]

Published

2024

20. GRK2 inhibits Flt-1+ macrophage infiltration and its proangiogenic properties in rheumatoid arthritis.

Author

Yang, Xuezhi, Zhao, Yingjie, Wei, Qi, Zhu, Xuemin, Wang, Luping, Zhang, Wankang, Liu, Xiaoyi, Kuai, Jiajie, Wang, Fengling, and Wei, Wei

Subjects

RHEUMATOID arthritis, LUCIFERASES, PEROXISOME proliferator-activated receptors, MACROPHAGES, COLLAGEN-induced arthritis, PROTEIN-tyrosine kinases

Abstract

Rheumatoid arthritis (RA) is an autoimmune disease with a complex etiology. Monocyte-derived macrophages (MDMs) infiltration are associated with RA severity. We have reported the deletion of G-protein-coupled receptor kinase 2 (GRK2) reprograms macrophages toward an anti-inflammatory phenotype by recovering G-protein-coupled receptor signaling. However, as more GRK2-interacting proteins were discovered, the GRK2 interactome mechanisms in RA have been understudied. Thus, in the collagen-induced arthritis mouse model, we performed genetic GRK2 deletion using GRK2 f/f Lyz2 -Cre+/− mice. Synovial inflammation and M1 polarization were improved in GRK2 f/f Lyz2 -Cre+/− mice. Supporting experiments with RNA-seq and dual-luciferase reporter assays identified peroxisome proliferator-activated receptor γ (PPAR γ) as a new GRK2-interacting protein. We further confirmed that fms-related tyrosine kinase 1 (Flt-1), which promoted macrophage migration to induce angiogenesis, was inhibited by GRK2-PPAR γ signaling. Mechanistically, excess GRK2 membrane recruitment in CIA MDMs reduced the activation of PPAR γ ligand-binding domain and enhanced Flt-1 transcription. Furthermore, the treatment of mice with GRK2 activity inhibitor resulted in significantly diminished CIA pathology, Flt-1+ macrophages induced-synovial inflammation, and angiogenesis. Altogether, we anticipate to facilitate the elucidation of previously unappreciated details of GRK2-specific intracellular signaling. Targeting GRK2 activity is a viable strategy to inhibit MDMs infiltration, affording a distinct way to control joint inflammation and angiogenesis of RA. The recruitment of GRK2 to the membrane inhibits PPAR γ -Tyr473 activation, consequently leading to synovial Flt-1+ macrophages infiltration, ultimately aggravating synovial inflammation and angiogenesis in rheumatoid arthritis. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

21. Effects of autologous serum on TREM2 and APOE in a personalized monocyte-derived macrophage assay of late-onset Alzheimer’s patients

Author

Neriman Eren, Susanna Gerike, Berk Üsekes, Oliver Peters, Nicoleta-Carmen Cosma, and Julian Hellmann-Regen

Subjects

Late-onset Alzheimer's disease, TREM2, APOE, Monocyte-derived macrophages, Amyloid-beta uptake, Sex differences, Immunologic diseases. Allergy, RC581-607, Geriatrics, RC952-954.6

Abstract

Abstract Background Age-associated deterioration of the immune system contributes to a chronic low-grade inflammatory state known as “inflammaging” and is implicated in the pathogenesis of late-onset Alzheimer's disease (LOAD). Whether changes in the tissue environment caused by circulatory factors associated with aging may alter the innate immune response is unknown. Monocyte-derived macrophages (Mo-MФs) infiltrating the brain alongside microglia are postulated to play a modulatory role in LOAD and both express triggering receptor expressed on myeloid cells 2 (TREM2). Apolipoprotein E (APOE) acts as a ligand for TREM2, and their role in amyloid beta (Aβ) clearance highlights their importance in LOAD. However, the influence of the patient's own milieu (autologous serum) on the synthesis of TREM2 and APOE in infiltrating macrophages remains unknown. Objectives To functionally assess patient-specific TREM2 and APOE synthesis, we designed a personalized assay based on Mo-MФs using monocytes from LOAD patients and matched controls (CO). We assessed the influence of each participant’s own milieu, by examining the effect of short- (1 day) and long- (10 days) term differentiation of the cells in the presence of the donor´s autologous serum (AS) into M1-, M2- or M0-macrophages. Additionally, sex differences and Aβ-uptake ability in short- and long-term differentiated Mo-MФs were assessed. Results We showed a time-dependent increase in TREM2 and APOE protein levels in LOAD- and CO-derived cells. While AS did not differentially modulate TREM2 compared to standard fetal calf serum (FCS), AS decreased APOE levels in M2 macrophages but increased levels in M1 macrophages. Interestingly, higher levels of TREM2 and lower levels of APOE were detected in female- than in male- LOAD patients. Finally, we report decreased Aβ-uptake in long-term differentiated CO- and LOAD-derived cells, particularly in APOEε4(+) carriers. Conclusions We demonstrate for the first time the suitability of a personalized Mo-MФ cell culture-based assay for studying functional TREM2 and APOE synthesis in a patient's own aged milieu. Our strategy may thus provide a useful tool for future research on diagnostic and therapeutic aspects of personalized medicine.

Published

2023

22. TNFα: TNFR1 signaling inhibits maturation and maintains the pro-inflammatory programming of monocyte-derived macrophages in murine chronic granulomatous disease

Author

Sophie L. Gibbings, Kelsey C. Haist, Elizabeth F. Redente, Peter M. Henson, and Donna L. Bratton

Subjects

tumor necrosis factor, monocyte-derived macrophages, hyperinflammation, chronic granulomatous disease (CGD), TNF inhibitor, macrophage programming, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionLoss of NADPH oxidase activity results in proinflammatory macrophages that contribute to hyperinflammation in Chronic Granulomatous Disease (CGD). Previously, it was shown in a zymosan-induced peritonitis model that gp91phox-/- (CGD) monocyte-derived macrophages (MoMacs) fail to phenotypically mature into pro-resolving MoMacs characteristic of wild type (WT) but retain the ability to do so when placed in the WT milieu. Accordingly, it was hypothesized that soluble factor(s) in the CGD milieu thwart appropriate programming.MethodsWe sought to identify key constituents using ex vivo culture of peritoneal inflammatory leukocytes and their conditioned media. MoMac phenotyping was performed via flow cytometry, measurement of efferocytic capacity and multiplex analysis of secreted cytokines. Addition of exogenous TNFα, TNFα neutralizing antibody and TNFR1-/- MoMacs were used to study the role of TNFα: TNFR1 signaling in MoMac maturation.ResultsMore extensive phenotyping defined normal MoMac maturation and demonstrated failure of maturation of CGD MoMacs both ex vivo and in vivo. Protein components, and specifically TNFα, produced and released by CGD neutrophils and MoMacs into conditioned media was identified as critical to preventing maturation. Exogenous addition of TNFα inhibited WT MoMac maturation, and its neutralization allowed maturation of cultured CGD MoMacs. TNFα neutralization also reduced production of IL-1β, IL-6 and CXCL1 by CGD cells though these cytokines played no role in MoMac programming. MoMacs lacking TNFR1 matured more normally in the CGD milieu both ex vivo and following adoptive transfer in vivo.DiscussionThese data lend mechanistic insights into the utility of TNFα blockade in CGD and to other diseases where such therapy has been shown to be beneficial.

Published

2024

23. Novel phenotypical and functional sub‐classification of liver macrophages highlights changes in population dynamics in experimental mouse models.

Author

Nakashima, Hiroyuki, Kearney, Bradley M., Kato, Azusa, Miyazaki, Hiromi, Ito, Seigo, Nakashima, Masahiro, and Kinoshita, Manabu

Abstract

Liver macrophages are critical components of systemic immune system defense mechanisms. F4/80high Kupffer cells (KCs) are the predominant liver‐resident macrophages and the first immune cells to contact pathogens entering the liver. F4/80low monocyte‐derived macrophages (MoMφs) are essential macrophages that modulate liver immune functions. Here we report a novel method of identifying subpopulations of these two populations using traditional flow cytometry and examine each subpopulation for its putative roles in the pathogenesis of an experimental non‐alcoholic steatohepatitis model. Using male C57BL/6 mice, we isolated and analyzed liver non‐parenchymal cells by flow cytometry. We identified F4/80high and F4/80low macrophage populations and characterized subpopulations using uniform manifold approximation and projection. We identified three subpopulations in F4/80high macrophages: CD163(+) KCs, CD163(−) KCs, and liver capsular macrophages. CD163(+) KCs had higher phagocytic and bactericidal activities and more complex cellular structures than CD163(−) KCs. We also identified four subpopulations of F4/80low MoMφs based on Ly6C and MHC class II expression: infiltrating monocytes, pro‐inflammatory MoMφs, Ly6C(−) monocytes, and conventional dendritic cells. CCR2 knock‐out mice expressed lower levels of these monocyte‐derived cells, and the count varied by subpopulation. In high‐fat‐ and cholesterol‐diet‐fed mice, only one subpopulation, pro‐inflammatory MoMφs, significantly increased in count. This indicates that changes to this subpopulation is the first step in the progression to non‐alcoholic steatohepatitis. The community can use our novel subpopulation and gating strategy to better understand complex immunological mechanisms in various liver disorders through detailed analysis of these subpopulations. [ABSTRACT FROM AUTHOR]

Published

2023

24. Effects of autologous serum on TREM2 and APOE in a personalized monocyte-derived macrophage assay of late-onset Alzheimer's patients.

Author

Eren, Neriman, Gerike, Susanna, Üsekes, Berk, Peters, Oliver, Cosma, Nicoleta-Carmen, and Hellmann-Regen, Julian

Subjects

*ALZHEIMER'S patients, *APOLIPOPROTEIN E, *MACROPHAGES, *ALZHEIMER'S disease, *MYELOID cells, *CELL differentiation

Abstract

Background: Age-associated deterioration of the immune system contributes to a chronic low-grade inflammatory state known as "inflammaging" and is implicated in the pathogenesis of late-onset Alzheimer's disease (LOAD). Whether changes in the tissue environment caused by circulatory factors associated with aging may alter the innate immune response is unknown. Monocyte-derived macrophages (Mo-MФs) infiltrating the brain alongside microglia are postulated to play a modulatory role in LOAD and both express triggering receptor expressed on myeloid cells 2 (TREM2). Apolipoprotein E (APOE) acts as a ligand for TREM2, and their role in amyloid beta (Aβ) clearance highlights their importance in LOAD. However, the influence of the patient's own milieu (autologous serum) on the synthesis of TREM2 and APOE in infiltrating macrophages remains unknown. Objectives: To functionally assess patient-specific TREM2 and APOE synthesis, we designed a personalized assay based on Mo-MФs using monocytes from LOAD patients and matched controls (CO). We assessed the influence of each participant's own milieu, by examining the effect of short- (1 day) and long- (10 days) term differentiation of the cells in the presence of the donor´s autologous serum (AS) into M1-, M2- or M0-macrophages. Additionally, sex differences and Aβ-uptake ability in short- and long-term differentiated Mo-MФs were assessed. Results: We showed a time-dependent increase in TREM2 and APOE protein levels in LOAD- and CO-derived cells. While AS did not differentially modulate TREM2 compared to standard fetal calf serum (FCS), AS decreased APOE levels in M2 macrophages but increased levels in M1 macrophages. Interestingly, higher levels of TREM2 and lower levels of APOE were detected in female- than in male- LOAD patients. Finally, we report decreased Aβ-uptake in long-term differentiated CO- and LOAD-derived cells, particularly in APOEε4(+) carriers. Conclusions: We demonstrate for the first time the suitability of a personalized Mo-MФ cell culture-based assay for studying functional TREM2 and APOE synthesis in a patient's own aged milieu. Our strategy may thus provide a useful tool for future research on diagnostic and therapeutic aspects of personalized medicine. [ABSTRACT FROM AUTHOR]

Published

2023

25. Celastrol attenuates interleukin-8 release from LPS-activated human monocytes and monocyte-derived macrophages by inhibiting the NF-κB signalling pathway.

Author

Malisorn, Nipapan, Bootkotr, Wannapa, Thassapong Khamkhai, Chaikan, Ammara, and Seubsasana, Supawadee

Subjects

*MONOCYTES, *CELLULAR signal transduction, *INTERLEUKIN-8, *MACROPHAGES, *TRANSCRIPTION factors

Abstract

Interleukin-8 (IL-8), a potent neutrophil chemotactic factor, plays a critical role during inflammation. IL-8 is produced primarily by several immune cell types upon lipopolysaccharide (LPS) stimulation by activating the nuclear factor-κB (NF-κB) signalling pathway. NF-κB is an important transcription factor implicated in the inflammatory response, and the NF-κB signalling pathway is a potential target for inhibition by anti-inflammatory compounds. Celastrol has been shown to have therapeutic potential in treating many inflammatory diseases; however, there is little information on its ability to attenuate IL-8 production in human monocytes and macrophages. Here, we determined the effects of celastrol on LPS-induced IL-8 release and its molecular mechanism. Celastrol treatment significantly reduced IL-8 release from LPS-activated human monocytes and monocyte-derived macrophages with IC50 values of 3.13 ± 0.03 µM and 3.18 ± 0.05 µM, respectively. Additionally, the inhibitory effect of celastrol on the production of IL-8 was related to the modulation of IL-8 mRNA levels. Pre-treatment with celastrol significantly inhibited IKK, IκBα, and p65 phosphorylation and also prevented IκBα degradation due to LPS activation. Collectively, these results demonstrate that celastrol attenuates the release of IL-8 from LPS-activated human monocytes and monocyte-derived macrophages and suggest that inhibition of NF-κB signalling activation is likely a mechanism for the attenuation. This anti-inflammatory effect further highlights the therapeutic potential of celastrol. [ABSTRACT FROM AUTHOR]

Published

2023

26. Origin and maintenance of Kupffer Cells in homeostasis and liver injury

Author

Hawley, Catherine Alice, Jenkins, Stephen, and Dransfield, Ian

Subjects

616.3, macrophages, Kupffer Cells, foetal liver monocytes, CSF1, liver injury, monocyte-derived macrophages, KC population

Abstract

Evaluation of liver resident Kupffer Cells (KC) has shown that in mouse these cells derive from a population of foetal liver monocytes that seed the tissues during embryogenesis and maintain themselves in steady state conditions independently of circulating monocytes, via local proliferation. The factors which regulate this KC autonomy have not yet been determined, but likely comprise both biochemical and physical factors which form their ‘niche’. Furthermore, their regulation, and specifically whether they retain total autonomy from monocyte-derived macrophages following liver injury has not been extensively studied. In this thesis I aimed to address the role of availability of the macrophage growth factor CSF1 in maintenance of KC and their autonomy from monocytes in homeostasis, and the roles and long-term fate of KC and monocyte-derived macrophages following acute and chronic liver injury. An optimal method for isolation and identification of F4/80hiCD11blo KC for flow cytometric analysis was first established. To explore the role of CSF1 in maintenance of KC, Csf1r-mApple mice were generated which revealed that KC expressed the highest levels of the csf1rmApple transgene compared with other leukocytes in the liver. In vivo administration of fluorescently-labelled CSF1-FcAF647 revealed that KC captured 10x more circulating CSF1 per cell than other myeloid cells in the liver and lung, suggesting efficient capture of CSF1 may be one mechanism that allows KC to regulate differentiation of monocytes in the liver. Delivery of CSF1-Fc to chimeric mice led to an increase in proliferation and accumulation of resident KC and a transient increase in the number of bone marrow-derived F4/80hiCD11blo cells in the liver, which were lost by 2 weeks following withdrawal of CSF1-Fc. These bone-marrow derived macrophages did not express the putative KC marker Tim4, indicating that they did not fully adopt a KC phenotype. Acute CCl4-driven liver injury resulted in a transient loss of approximately 50% of the resident KC population which recovered in number by 6 days post injury, through proliferation of the remaining KC. This was despite the fact that injury led to the massive recruitment of monocyte-derived macrophages some of which matured into an F4/80hiCD11blo population, but which also lacked Tim4 expression. These cells were spatially distinct from KC and were found clustered around blood vessels, presumed to be the region of necrotic damage. Comparison of gene expression was consistent with their involvement in tissue repair. Following CCl4-driven chronic liver injury, KC were depleted in number, but unlike in acute injury, the population did not return to normal numbers even 8 weeks following cessation of treatment. This time, the recruited macrophages these were not found in clusters but alongside resident KC in the parenchyma. However, in both acute and chronic injury, monocyte-derived macrophages could no longer be seen 8 weeks after injury, and did not mature into long-lived, self-renewing KC. In conclusion I found that CSF1 is one of the major limiting factors that dictates the size of the KC niche, but additional factors are required to fully support monocyte engraftment to the KC population. Following CCl4-driven acute liver injury, monocyte-derived macrophages do not contribute long-term to the KC population despite exhibiting a F4/80hiCD11blo phenotype during the latter stages of liver repair. KC are depleted long-term following CCl4- driven chronic liver injury, but monocyte-derived macrophages remain unable to replenish the population, indicating that damage to a physical component of the KC niche may have occurred.

Published

2020

27. Effects of Akt Activator SC79 on Human M0 Macrophage Phagocytosis and Cytokine Production

Author

Robert J. Lee, Nithin D. Adappa, and James N. Palmer

Subjects

signal transduction, live cell imaging, monocyte-derived macrophages, inflammation, innate immunity, Toll-like receptor, Cytology, QH573-671

Abstract

Akt is an important kinase in metabolism. Akt also phosphorylates and activates endothelial and neuronal nitric oxide (NO) synthases (eNOS and nNOS, respectively) expressed in M0 (unpolarized) macrophages. We showed that e/nNOS NO production downstream of bitter taste receptors enhances macrophage phagocytosis. In airway epithelial cells, we also showed that the activation of Akt by a small molecule (SC79) enhances NO production and increases levels of nuclear Nrf2, which reduces IL-8 transcription during concomitant stimulation with Toll-like receptor (TLR) 5 agonist flagellin. We hypothesized that SC79’s production of NO in macrophages might likewise enhance phagocytosis and reduce the transcription of some pro-inflammatory cytokines. Using live cell imaging of fluorescent biosensors and indicator dyes, we found that SC79 induces Akt activation, NO production, and downstream cGMP production in primary human M0 macrophages. This was accompanied by a reduction in IL-6, IL-8, and IL-12 production during concomitant stimulation with bacterial lipopolysaccharide, an agonist of pattern recognition receptors including TLR4. Pharmacological inhibitors suggested that this effect was dependent on Akt and Nrf2. Together, these data suggest that several macrophage immune pathways are regulated by SC79 via Akt. A small-molecule Akt activator may be useful in some infection settings, warranting future in vivo studies.

Published

2024

28. The diversity and dynamics of tumor-associated macrophages in recurrent glioblastoma.

Author

Lingyun Zhang, Yu Jiang, Gao Zhang, and Shiyou Wei

Subjects

MACROPHAGES, GLIOBLASTOMA multiforme, TUMOR growth, TUMOR microenvironment, IMMUNOSUPPRESSION

Abstract

Despite tremendous efforts to exploit effective therapeutic strategies, most glioblastoma (GBM) inevitably relapse and become resistant to therapies, including radiotherapy and immunotherapy. The tumor microenvironment (TME) of recurrent GBM (rGBM) is highly immunosuppressive, dominated by tumor-associated macrophages (TAMs). TAMs consist of tissue-resident microglia and monocyte-derived macrophages (MDMs), which are essential for favoring tumor growth, invasion, angiogenesis, immune suppression, and therapeutic resistance; however, restricted by the absence of potent methods, the heterogeneity and plasticity of TAMs in rGBM remain incompletely investigated. Recent application of single-cell technologies, such as single-cell RNA-sequencing has enabled us to decipher the unforeseen diversity and dynamics of TAMs and to identify new subsets of TAMs which regulate antitumor immunity. Here, we first review hallmarks of the TME, progress and challenges of immunotherapy, and the biology of TAMs in the context of rGBM, including their origins, categories, and functions. Next, from a singlecell perspective, we highlight recent findings regarding the distinctions between tissue-resident microglia and MDMs, the identification and characterization of specific TAM subsets, and the dynamic alterations of TAMs during tumor progression and treatment. Last, we briefly discuss the potential of TAMtargeted strategies for combination immunotherapy in rGBM. We anticipate the comprehensive understanding of the diversity and dynamics of TAMs in rGBM will shed light on further improvement of immunotherapeutic efficacy in rGBM. [ABSTRACT FROM AUTHOR]

Published

2023

29. Myeloid-specific blockade of notch signaling alleviates dopaminergic neurodegeneration in Parkinson's disease by dominantly regulating resident microglia activation through NF-κB signaling.

Author

Shi-Qian Liang, Peng-Hui Li, Yi-Yang Hu, Jun-Long Zhao, Fang-Ze Shao, Fang Kuang, Kai-Xi Ren, Tiao-Xia Wei, Fan Fan, Lei Feng, Hua Han, and Hong-Yan Qin

Subjects

PARKINSON'S disease, MICROGLIA, MAJOR histocompatibility complex, TYROSINE hydroxylase, NEURODEGENERATION

Abstract

Yolk sac-derived microglia and peripheral monocyte-derived macrophages play a key role during Parkinson's disease (PD) progression. However, the regulatory mechanism of microglia/macrophage activation and function in PD pathogenesis remains unclear. Recombination signal-binding protein Jκ (RBP-J)-mediated Notch signaling regulates macrophage development and activation. In this study, with an 1-Methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) hydrochloride-induced acute murine PD model, we found that Notch signaling was activated in amoeboid microglia accompanied by a decrease in tyrosine hydroxylase (TH)-positive neurons. Furthermore, using myeloid-specific RBP-J knockout (RBP-JcKO) mice combined with a PD model, our results showed that myeloid-specific disruption of RBP-J alleviated dopaminergic neurodegeneration and improved locomotor activity. Fluorescence-activated cell sorting (FACS) analysis showed that the number of infiltrated inflammatory macrophages and activated major histocompatibility complex (MHC) II+ microglia decreased in RBP-JcKO mice compared with control mice. Moreover, to block monocyte recruitment by using chemokine (C-C motif) receptor 2 (CCR2) knockout mice, the effect of RBP-J deficiency on dopaminergic neurodegeneration was not affected, indicating that Notch signaling might regulate neuroinflammation independent of CCR2+ monocyte infiltration. Notably, when microglia were depleted with the PLX5622 formulated diet, we found that myeloid-specific RBP-J knockout resulted in more TH+ neurons and fewer activated microglia. Ex vitro experiments demonstrated that RBP-J deficiency in microglia might reduce inflammatory factor secretion, TH+ neuron apoptosis, and p65 nuclear translocation. Collectively, our study first revealed that RBP-J-mediated Notch signaling might participate in PD progression by mainly regulating microglia activation through nuclear factor kappa-B (NF-κB) signaling. [ABSTRACT FROM AUTHOR]

Published

2023

30. Characteristics of activation of monocyte-derived macrophages versus microglia after mouse experimental intracerebral hemorrhage.

Author

Ye, Fenghui, Yang, Jinting, Holste, Katherine G, Koduri, Sravanthi, Hua, Ya, Keep, Richard F, Garton, Hugh JL, and Xi, Guohua

Abstract

Both monocyte-derived macrophages (MDMs) and brain resident microglia participate in hematoma resolution after intracerebral hemorrhage (ICH). Here, we utilized a transgenic mouse line with enhanced green fluorescent protein (EGFP) labeled microglia (Tmem119-EGFP mice) combined with a F4/80 immunohistochemistry (a pan-macrophage marker) to visualize changes in MDMs and microglia after ICH. A murine model of ICH was used in which autologous blood was stereotactically injected into the right basal ganglia. The autologous blood was co-injected with CD47 blocking antibodies to enhance phagocytosis or clodronate liposomes for phagocyte depletion. In addition, Tmem119-EGFP mice were injected with the blood components peroxiredoxin 2 (Prx2) or thrombin. MDMs entered the brain and formed a peri-hematoma cell layer by day 3 after ICH and giant phagocytes engulfed red blood cells were found. CD47 blocking antibody increased the number of MDMs around and inside the hematoma and extended MDM phagocytic activity to day 7. Both MDMs and microglia could be diminished by clodronate liposomes. Intracerebral injection of Prx2 but not thrombin attracted MDMs into brain parenchyma. In conclusion, MDMs play an important role in phagocytosis after ICH which can be enhanced by CD47 blocking antibody, suggesting the modulation of MDMs after ICH could be a future therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2023

31. Acute and Chronic Macrophage Differentiation Modulates TREM2 in a Personalized Alzheimer's Patient-Derived Assay.

Author

Cosma, Nicoleta-Carmen, Eren, Neriman, Üsekes, Berk, Gerike, Susanna, Heuser, Isabella, Peters, Oliver, and Hellmann-Regen, Julian

Subjects

*ALZHEIMER'S disease, *MACROPHAGES, *MYELOID cells, *PATHOLOGY, *INDIVIDUALIZED medicine

Abstract

Neuroinflammation plays a pivotal role in the pathogenesis of Alzheimer's disease (AD). Brain macrophage populations differentially modulate the immune response to AD pathology according to the disease stage. Triggering receptor expressed on myeloid cells 2 (TREM2) is known to play a protective role in AD and has been postulated as a putative therapeutic target. Whether, and to which extent TREM2 expression can be modulated in the aged macrophage population of the brain is unknown, emphasizing the need for a human, patient-specific model. Using cells from AD patients and matched controls (CO) we designed an assay based on monocyte-derived macrophages to mimic brain-infiltrating macrophages and to assess the individualized TREM2 synthesis in vitro. We systematically assessed the effects of short-term (acute—2 days) and long-term (chronic—10 days) M1- (LPS), M2- (IL-10, IL-4, TGF-β), and M0- (vehicle) macrophage differentiation on TREM2 synthesis. Moreover, the effects of retinoic acid (RA), a putative TREM2 modulator, on individualized TREM2 synthesis were assessed. We report increased TREM2 synthesis after acute M2- compared to M1-differentiation in CO- but not AD-derived cells. Chronic M2- and M0-differentiation however resulted in an increase of TREM2 synthesis in both AD- and CO-derived cells while chronic M1-differentiation increased TREM2 in AD-derived cells only. Moreover, chronic M2- and M0-differentiation improved the amyloid-β (Aβ) uptake of the CO-derived whereas M1-differentiation of the AD-derived cells. Interestingly, RA-treatment did not modulate TREM2. In the age of personalized medicine, our individualized model could be used to screen for potential drug-mediated treatment responses in vitro. Triggering receptor expressed on myeloid cells 2 (TREM2) has been postulated as a putative therapeutic target in Alzheimer's disease (AD). Using cells from AD patients and matched controls (CO), we designed a monocyte-derived macrophages (Mo-MФs) assay to assess the individualized TREM2 synthesis in vitro. We report increased TREM2 synthesis after acute M2- compared to M1- macrophage differentiation in CO- but not AD-derived cells. Chronic M2- and M0- differentiation however resulted in an increase of TREM2 synthesis in both AD- and CO-derived cells while chronic M1-differentiation increased TREM2 in AD-cells only [ABSTRACT FROM AUTHOR]

Published

2023

32. Cardiac macrophages undergo dynamic changes after coxsackievirus B3 infection and promote the progression of myocarditis.

Author

Dong, Jingwei, Lu, Jing, Cen, Zhihong, Tang, Quan, Li, Yong, Qin, Lin, Yan, Yuluan, Lu, Feiyu, and Wu, Weifeng

Subjects

COXSACKIEVIRUS diseases, MACROPHAGES, MYOCARDITIS, HEART cells, CHEMOKINE receptors

Abstract

Although most patients with acute viral myocarditis recover spontaneously, some patients progress to heart failure. Perturbations in innate immunity may partially explain the heterogeneity of clinical outcomes. As the most abundant immune cells in the heart, cardiac macrophages have heterogeneous origins, including embryonic‐derived resident macrophages (ResMϕs) and monocyte‐derived macrophages (MoMFs). However, the time course change and role of cardiac macrophage subsets has not been fully explored. In the present study, we found that BALB/c mice had prolonged MoMF accumulation and low proportions of ResMϕs that could not be restored to normal levels. MoMFs of BALB/c mice generally exhibit an M1‐dominant functional phenotype. Moreover, the preferential depletion of MoMF by a C‐C chemokine receptor type 2 (CCR2) inhibitor resulted in improved acute myocarditis and chronic fibrosis, as well as the recovery of ResMϕs number and reduced CD4+ T cell expansion. Hence, immunomodulatory therapy that targets the balance among cardiac macrophages and modulates their function is expected to prevent the progression of cardiac injury to overt heart failure and improve adverse outcomes. [ABSTRACT FROM AUTHOR]

Published

2023

33. iPS cell–derived model to study the interaction between tissue macrophage and HIV-1.

Author

Eltalkhawy, Youssef M, Takahashi, Naofumi, Ariumi, Yasuo, Shimizu, Jun, Miyazaki, Kazuo, Senju, Satoru, and Suzu, Shinya

Subjects

HIV, MACROPHAGES, YOLK sac, CELL motility, ANTIRETROVIRAL agents

Abstract

Despite effective antiretroviral therapy, HIV-1 persists in cells, including macrophages, which is an obstacle to cure. However, the precise role of macrophages in HIV-1 infection remains unclear because they reside in tissues that are not easily accessible. Monocyte-derived macrophages are widely used as a model in which peripheral blood monocytes are cultured and differentiated into macrophages. However, another model is needed because recent studies revealed that most macrophages in adult tissues originate from the yolk sac and fetal liver precursors rather than monocytes, and the embryonic macrophages possess a self-renewal (proliferating) capacity that monocyte-derived macrophages lack. Here, we show that human induced pluripotent stem cell–derived immortalized macrophage-like cells are a useful self-renewing macrophage model. They proliferate in a cytokine-dependent manner, retain macrophage functions, support HIV-1 replication, and exhibit infected monocyte-derived macrophage–like phenotypes, such as enhanced tunneling nanotube formation and cell motility, as well as resistance to a viral cytopathic effect. However, several differences are also observed between monocyte-derived macrophages and induced pluripotent stem cell–derived immortalized macrophage-like cells, most of which can be explained by the proliferation of induced pluripotent stem cell–derived immortalized macrophage-like cells. For instance, proviruses with large internal deletions, which increased over time in individuals receiving antiretroviral therapy, are enriched more rapidly in induced pluripotent stem cell–derived immortalized macrophage-like cells. Interestingly, inhibition of viral transcription by HIV-1–suppressing agents is more obvious in induced pluripotent stem cell–derived immortalized macrophage-like cells. Collectively, our present study proposes that the model of induced pluripotent stem cell–derived immortalized macrophage-like cells is suitable for mimicking the interplay between HIV-1 and self-renewing tissue macrophages, the newly recognized major population in most tissues that cannot be fully modeled by monocyte-derived macrophages alone. [ABSTRACT FROM AUTHOR]

Published

2023

34. Endothelial Toll-like receptor 4 is required for microglia activation in the murine retina after systemic lipopolysaccharide exposure

Author

Ioanna Tsioti, Beatrice L. Steiner, Pascal Escher, Martin S. Zinkernagel, Peter M. Benz, and Despina Kokona

Subjects

Retina, Microglia, Lipopolysaccharide, Toll-like receptor 4, Endothelial cells, Monocyte-derived macrophages, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Clustering of microglia around the vasculature has been reported in the retina and the brain after systemic administration of lipopolysaccharides (LPS) in mice. LPS acts via activation of Toll-like receptor 4 (TRL4), which is expressed in several cell types including microglia, monocytes and vascular endothelial cells. The purpose of this study was to investigate the effect of systemic LPS in the pigmented mouse retina and the involvement of endothelial TLR4 in LPS-induced retinal microglia activation. Methods C57BL/6J, conditional knockout mice that lack Tlr4 expression selectively on endothelial cells (TekCre−posTlr4loxP/loxP) and TekCre−negTlr4loxP/loxP mice were used. The mice were injected with 1 mg/kg LPS via the tail vein once per day for a total of 4 days. Prior to initiation of LPS injections and approximately 5 h after the last injection, in vivo imaging using fluorescein angiography and spectral-domain optical coherence tomography was performed. Immunohistochemistry, flow cytometry, electroretinography and transmission electron microscopy were utilized to investigate the role of endothelial TLR4 in LPS-induced microglia activation and retinal function. Results Activation of microglia, infiltration of monocyte-derived macrophages, impaired ribbon synapse organization and retinal dysfunction were observed after the LPS exposure in C57BL/6J and TekCre−negTlr4loxP/loxP mice. None of these effects were observed in the retinas of conditional Tlr4 knockout mice after the LPS challenge. Conclusions The findings of the present study suggest that systemic LPS exposure can have detrimental effects in the healthy retina and that TLR4 expressed on endothelial cells is essential for retinal microglia activation and retinal dysfunction upon systemic LPS challenge. This important finding provides new insights into the role of microglia–endothelial cell interaction in inflammatory retinal disease.

Published

2023

35. Expression of factor XIII originating from synovial fibroblasts and macrophages induced by interleukin-6 signaling

Author

Hirofumi Watanabe, Sho Mokuda, Tadahiro Tokunaga, Hiroki Kohno, Michinori Ishitoku, Kei Araki, Tomohiro Sugimoto, Yusuke Yoshida, Toshihiro Yamamoto, Mayuko Matsumoto, Junya Masumoto, Shintaro Hirata, and Eiji Sugiyama

Subjects

Rheumatoid arthritis, Blood coagulation factor XIII, Monocyte-derived macrophages, Fibroblast-like synoviocytes (FLS), Interleukin-6, Pathology, RB1-214

Abstract

Abstract Background Blood coagulation factor XIII (FXIII) promotes cross-linking between fibrin molecules at the final stage of the blood coagulation cascade. However, its expression in cells or tissues and function, particularly factor XIII subunit B (FXIII-B), remains controversial. Hemorrhagic FXIII deficiency following anti-interleukin-6 (IL-6) receptor antibody treatment has been reported in patients with rheumatoid arthritis (RA). Patients receiving this biologics have reduced FXIII activity when compared to the activity in those treated with other biologics. The relationship between pro-inflammatory cytokines and FXIII expression remains unknown. Methods To investigate the expression pattern of FXIII in synovial tissues, immunohistochemistry, RT-qPCR, and western blotting were performed. FXIII-A expressed monocyte-derived macrophages were treated with recombinant IL-6 and anti-IL-6 receptor antibody. RNA sequencing of FXIII-B-overexpressing cells was performed to clarify the function of FXIII-B. Results The immunohistochemical analysis of synovial tissues revealed that factor XIII subunit A (FXIII-A) was expressed in M2 macrophages, and FXIII-B was expressed in fibroblast-like synoviocytes. IL-6 stimulation upregulated FXIII-A expression in IL-4-induced monocyte-derived macrophages, and the anti-IL-6 receptor antibody suppressed FXIII-A expression. FXIII-B was more abundantly secreted in the supernatant of fibroblast-like synoviocytes compared with that of other cells. RNA sequencing showed that FXIII-B elevated the expression of genes associated with anti-apoptotic molecules and chemokines. Conclusions Our findings highlight that synovial tissue is one of the sources of FXIII production. We also have demonstrated IL-6-dependent FXIII-A expression and the novel potential functions of FXIII-B.

Published

2023

36. Endothelial cell CD36 mediates stroke-induced brain injury via BBB dysfunction and monocyte infiltration in normal and obese conditions.

Author

Kim, Il-doo, Ju, Hyunwoo, Minkler, Joseph, Jiang, Roselyn, Singh, Abhilasha, Sharma, Roopa, Febbraio, Maria, and Cho, Sunghee

Abstract

CD36 expressed in multiple cell types regulates inflammation, vascular function, and innate immunity. Specifically, CD36 in microvascular endothelial cells (ECs) signals to elicit inflammation and causes EC death. This study investigated roles for EC-CD36 on acute stroke pathology in normal and obese conditions. Obesity induced by a high-fat diet (HD) selectively increased CD36 expression in ECs, not in monocytes/macrophages, in the post-ischemic brain. Mice deficient CD36 in ECs (ECCD36−/−) showed reduced injury size and vascular permeability in normal conditions. While control mice fed a HD developed obesity and aggravated stroke injury, ECCD36−/− mice were resistant to develop an obesity phenotype. Subjecting ECCD36−/− mice to stroke resulted in reduced injury size and BBB disruption. Moreover, the mice had reduced MCP-1 and CCR2 gene expression, resulting in reduced monocyte trafficking with improved survival and acute motor function. Reduced MCP-1 and CCR2 expression was still evident in ECCD36−/− mice subjected to severe stroke, suggesting that monocyte trafficking is an infarct-independent metabolic effect associated with specific EC-CD36 deletion. Our findings demonstrate the importance of EC-CD36 in developing vascular comorbidities and suggest that targeting EC-CD36 is a potential preventative strategy to normalize vascular risk factors, leading to improved acute stroke outcomes. [ABSTRACT FROM AUTHOR]

Published

2023

37. The generation, activation, and polarization of monocyte-derived macrophages in human malignancies.

Author

Chaintreuil, Paul, Kerreneur, Emeline, Bourgoin, Maxence, Savy, Coline, Favreau, Cécile, Robert, Guillaume, Jacquel, Arnaud, and Auberger, Patrick

Subjects

MACROPHAGES, HEMATOLOGIC malignancies, PHAGOCYTOSIS, MACROPHAGE activation, EMBRYOLOGY

Abstract

Macrophages are immune cells that originate from embryogenesis or from the differentiation of monocytes. They can adopt numerous phenotypes depending on their origin, tissue distribution and in response to different stimuli and tissue environment. Thus, in vivo, macrophages are endowed with a continuum of phenotypes that are rarely strictly pro-inflammatory or anti-inflammatory and exhibit a broad expression profile that sweeps over the whole polarization spectrum. Schematically, three main macrophage subpopulations coexist in human tissues: naïve macrophages also called M0, pro-inflammatory macrophages referred as M1 macrophages, and anti-inflammatory macrophages also known as M2 macrophages. Naïve macrophages display phagocytic functions, recognize pathogenic agents, and rapidly undergo polarization towards pro or anti-inflammatory macrophages to acquire their full panel of functions. Pro-inflammatory macrophages are widely involved in inflammatory response, during which they exert anti-microbial and anti-tumoral functions. By contrast, anti-inflammatory macrophages are implicated in the resolution of inflammation, the phagocytosis of cell debris and tissue reparation following injuries. Macrophages also play important deleterious or beneficial roles in the initiation and progression of different pathophysiological settings including solid and hematopoietic cancers. A better understanding of the molecular mechanisms involved in the generation, activation and polarization of macrophages is a prerequisite for the development of new therapeutic strategies to modulate macrophages functions in pathological situations. [ABSTRACT FROM AUTHOR]

Published

2023

38. The Potential of Epigallocatechin-3-gallate (EGCG) as Complementary Medicine for the Treatment of Inflammatory Bowel Disease.

Author

Schnur, Sabrina, Hans, Fabian, Dehne, Annika, Osti, Janina, Schneemann, Malte-Ole, Schneider, Marc, and Hittinger, Marius

Subjects

*INFLAMMATORY bowel diseases, *ALTERNATIVE medicine, *EPIGALLOCATECHIN gallate, *THERAPEUTICS, *NATURAL products, *ADALIMUMAB, *VEDOLIZUMAB

Abstract

Complementary and alternative medicine has the potential to enrich conventional therapy to improve the treatment of various diseases. Patients that suffer from inflammatory bowel disease, which requires a constant need for medication, have to deal with the adverse effects of repeated application. Natural products such as Epigallocatechin-3-gallate (EGCG) possess the potential to improve symptoms of inflammatory diseases. We investigated the efficacy of EGCG on an inflamed co-culture model simulating IBD and compared it to the efficacies of four commonly applied active pharmaceutical ingredients. EGCG (200 µg/mL) strongly stabilized the TEER value of the inflamed epithelial barrier to 165.7 ± 4.6% after 4 h. Moreover, the full barrier integrity was maintained even after 48 h. This corresponds to the immunosuppressant 6-Mercaptopurin and the biological drug Infliximab. The EGCG treatment significantly decreased the release of the pro-inflammatory cytokines IL-6 (to 0%) and IL-8 (to 14.2%), similar to the effect of the corticosteroid Prednisolone. Therefore, EGCG has a high potential to be deployed as complementary medicine in IBD. In future studies, the improvement of EGCG stability is a key factor in increasing the bioavailability in vivo and fully harnessing the health-improving effects of EGCG. [ABSTRACT FROM AUTHOR]

Published

2023

39. Mouse Tissue‐Resident Peritoneal Macrophages in Homeostasis, Repair, Infection, and Tumor Metastasis.

Author

Ardavín, Carlos, Alvarez‐Ladrón, Natalia, Ferriz, Margarita, Gutiérrez‐González, Alejandra, and Vega‐Pérez, Adrián

Subjects

*PERITONEAL macrophages, *METASTASIS, *PERITONEUM, *PARASITIC diseases, *HOMEOSTASIS, *PHAGOCYTOSIS

Abstract

Large peritoneal macrophages (LPMs) are long‐lived, tissue‐resident macrophages, formed during embryonic life, developmentally and functionally confined to the peritoneal cavity. LPMs provide the first line of defense against life‐threatening pathologies of the peritoneal cavity, such as abdominal sepsis, peritoneal metastatic tumor growth, or peritoneal injuries caused by trauma, or abdominal surgery. Apart from their primary phagocytic function, reminiscent of primitive defense mechanisms sustained by coelomocytes in the coelomic cavity of invertebrates, LPMs fulfill an essential homeostatic function by achieving an efficient clearance of apoptotic, that is crucial for the maintenance of self‐tolerance. Research performed over the last few years, in mice, has unveiled the mechanisms by which LPMs fulfill a crucial role in repairing peritoneal injuries and controlling microbial and parasitic infections, reflecting that the GATA6‐driven LPM transcriptional program can be modulated by extracellular signals associated with pathological conditions. In contrast, recent experimental evidence supports that peritoneal tumors can subvert LPM metabolism and function, leading to the acquisition of a tumor‐promoting potential. The remarkable functional plasticity of LPMs can be nevertheless exploited to revert tumor‐induced LPM protumor potential, providing the basis for the development of novel immunotherapeutic approaches against peritoneal tumor metastasis based on macrophage reprogramming. [ABSTRACT FROM AUTHOR]

Published

2023

40. Early treatment with C-reactive protein-derived peptide reduces septic acute kidney injury in mice via controlled activation of kidney macrophages.

Author

Ito, Seigo, Goto, Hiroyasu, Tanoue, Keiko, Koiwai, Kazuki, Ishikiriyama, Takuya, Kearney, Bradley M, Mori, Kazuma, Nakashima, Masahiro, Nakashima, Hiroyuki, Kumagai, Hiroo, Seki, Shuhji, Kinoshita, Manabu, and Oshima, Naoki

Subjects

PEPTIDES, ACUTE kidney failure, MACROPHAGE activation, C-reactive protein

Abstract

The mortality rate for acute kidney injury (AKI) due to sepsis remains high, and effective therapies based on its pathogenesis remain elusive. Macrophages are crucial for clearing bacteria from vital organs, including the kidney, under septic conditions. Excessive macrophage activation results in organ injury. C-reactive protein (CRP) peptide (174-185), a functional product of proteolyzed CRP in vivo, effectively activates macrophages. We investigated the therapeutic efficacy of synthetic CRP peptide on septic AKI, focusing on effects on kidney macrophages. Mice underwent cecal ligation and puncture (CLP) to induce septic AKI and were intraperitoneally administered 20 mg/kg of synthetic CRP peptide 1 h post-CLP. Early CRP peptide treatment improved AKI while still clearing infection. Ly6C-negative kidney tissue-resident macrophages did not significantly increase at 3 h after CLP, while Ly6C-positive monocyte-derived macrophages significantly accumulated in the kidney 3 h post-CLP. CRP peptide augmented the phagocytic ROS production in both subtypes of kidney macrophage at 3 h. Interestingly, both subtypes of macrophage increased ROS production 24 h post-CLP compared to the control group, while CRP peptide treatment maintained ROS production at the same level seen 3 h post-CLP. Although bacterium-phagocytic kidney macrophages produced TNF-α, CRP peptide reduced bacterial propagation and tissue TNF-α levels in the septic kidney at 24 h. Although both subsets of kidney macrophages showed populations of M1 at 24 h post-CLP, CRP peptide therapy skewed the macrophages population toward M2 at 24 h. CRP peptide alleviated murine septic AKI via the controlled activation of kidney macrophages and is an excellent candidate for future human therapeutic studies. [ABSTRACT FROM AUTHOR]

Published

2023

41. Distinct spatiotemporal features of microglia and monocyte‐derived macrophages in glioma.

Author

Banerjee, Kaveri, Ratzabi, Avinoam, Caspit, Itai M, Ganon, Or, Blinder, Pablo, Jung, Steffen, and Stein, Reuven

Subjects

GLIOMAS, MICROGLIA, MACROPHAGES, BRAIN tumors, CANCER invasiveness

Abstract

Gliomas are the most frequent primary tumors of the brain. Glioma progression is regulated by the tumor microenvironment, which is mainly composed of tumor‐associated microglia (TA‐MG) and monocyte‐derived macrophages (MDM). Recent studies have highlighted the distinct properties of these cells in glioma progression. However, their spatiotemporal alteration during tumor progression has not been fully explored. Using a genetic lineage tracing approach, we show that TA‐MG and MDMs differ in their spatiotemporal distribution and interaction with other components of the glioma microenvironment. MDM were present only inside the tumor, whereas TA‐MG accumulated both outside and inside the tumor. However, TA‐MG was eliminated from the tumor mass as the tumor progressed. Depletion of MDM led to enhanced occupancy of TA‐MG in the tumor core, indicating that TA‐MG elimination was regulated by MDM. TA‐MG and MDM are heterogeneous cell populations whose compositions and properties can change during tumor progression. Finally, MG, TA‐MG and MDM were enriched in the perivascular area (PVA) compared to more distal blood vessel‐associated areas. However, inside the tumor, the MDM enrichment in PVA was higher than that in TA‐MG. Collectively, we established that TA‐MG and MDM exhibit different spatiotemporal features in glioma, suggesting distinctive roles during tumor progression. [ABSTRACT FROM AUTHOR]

Published

2023

42. The functional response of human monocyte-derived macrophages to serum amyloid A and Mycobacterium tuberculosis infection

Author

Malwina Kawka, Renata Płocińska, Przemysław Płociński, Jakub Pawełczyk, Marcin Słomka, Justyna Gatkowska, Katarzyna Dzitko, Bożena Dziadek, and Jarosław Dziadek

Subjects

tuberculosis, human serum amyloid A, monocyte-derived macrophages, immunological response, host-pathogen transcriptomics, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionIn the course of tuberculosis (TB), the level of major acute phase protein, namely serum amyloid A (hSAA-1), increases up to a hundredfold in the pleural fluids of infected individuals. Tubercle bacilli infecting the human host can be opsonized by hSAA-1, which affects bacterial entry into human macrophages and their intracellular multiplication.MethodsWe applied global RNA sequencing to evaluate the functional response of human monocyte-derived macrophages (MDMs), isolated from healthy blood donors, under elevated hSAA-1 conditions and during infection with nonopsonized and hSAA-1-opsonized Mycobacterium tuberculosis (Mtb). In the same infection model, we also examined the functional response of mycobacteria to the intracellular environment of macrophages in the presence and absence of hSAA-1. The RNASeq analysis was validated using qPCR. The functional response of MDMs to hSAA-1 and/or tubercle bacilli was also evaluated for selected cytokines at the protein level by applying the Milliplex system.FindingsTranscriptomes of MDMs cultured in the presence of hSAA-1 or infected with Mtb showed a high degree of similarity for both upregulated and downregulated genes involved mainly in processes related to cell division and immune response, respectively. Among the most induced genes, across both hSAA-1 and Mtb infection conditions, CXCL8, CCL15, CCL5, IL-1β, and receptors for IL-7 and IL-2 were identified. We also observed the same pattern of upregulated pro-inflammatory cytokines (TNFα, IL-6, IL-12, IL-18, IL-23, and IL-1) and downregulated anti-inflammatory cytokines (IL-10, TGFβ, and antimicrobial peptide cathelicidin) in the hSAA-1 treated-MDMs or the phagocytes infected with tubercle bacilli. At this early stage of infection, Mtb genes affected by the inside microenvironment of MDMs are strictly involved in iron scavenging, adaptation to hypoxia, low pH, and increasing levels of CO2. The genes for the synthesis and transport of virulence lipids, but not cholesterol/fatty acid degradation, were also upregulated.ConclusionElevated serum hSAA-1 levels in tuberculosis enhance the response of host phagocytes to infection, including macrophages that have not yet been in contact with mycobacteria. SAA induces antigen processing and presentation processes by professional phagocytes reversing the inhibition caused by Mtb infection.

Published

2023

43. PEG–Lipid–PLGA Hybrid Particles for Targeted Delivery of Anti-Inflammatory Drugs

Author

Jana Ismail, Lea C. Klepsch, Philipp Dahlke, Ekaterina Tsarenko, Antje Vollrath, David Pretzel, Paul M. Jordan, Kourosh Rezaei, Justyna A. Czaplewska, Steffi Stumpf, Baerbel Beringer-Siemers, Ivo Nischang, Stephanie Hoeppener, Oliver Werz, and Ulrich S. Schubert

Subjects

hybrid nanoparticles, targeted drug delivery, BRP-201, anti-inflammatory, monocyte-derived macrophages, 5-LOX inhibition, Pharmacy and materia medica, RS1-441

Abstract

Hybrid nanoparticles (HNPs) were designed by combining a PLGA core with a lipid shell that incorporated PEG–Lipid conjugates with various functionalities (-RGD, -cRGD, -NH2, and -COOH) to create targeted drug delivery systems. Loaded with a neutral lipid orange dye, the HNPs were extensively characterized using various techniques and investigated for their uptake in human monocyte-derived macrophages (MDMs) using FC and CLSM. Moreover, the best-performing HNPs (i.e., HNP-COOH and HNP-RGD as well as HNP-RGD/COOH mixed) were loaded with the anti-inflammatory drug BRP-201 and prepared in two size ranges (dH ~140 nm and dH ~250 nm). The HNPs were examined further for their stability, degradation, MDM uptake, and drug delivery efficiency by studying the inhibition of 5-lipoxygenase (5-LOX) product formation, whereby HNP-COOH and HNP-RGD both exhibited superior uptake, and the HNP-COOH/RGD (2:1) displayed the highest inhibition.

Published

2024

44. Phagocytosis converts infiltrated monocytes to microglia-like phenotype in experimental brain ischemia

Author

Hyunwoo Ju, Keun Woo Park, Il-doo Kim, John W. Cave, and Sunghee Cho

Subjects

Ischemic stroke, Phagocytes, Monocyte-derived macrophages, Microglia, Phagocytosis, Phenotype, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Monocyte-derived macrophages (MDMs) and microglia elicit neural inflammation and clear debris for subsequent tissue repair and remodeling. The role of infiltrating MDMs in the injured brain, however, has been controversial due to overlapping antigen expression with microglia. In this study, we define the origin and function of MDMs in cerebral ischemia. Methods Using adoptive transfer of GFP+ splenocytes into adult asplenic mice subjected to transient middle cerebral artery occlusion, we compared the role of CD11b + /CD45+/NK1.1 − /Ly6G − MDMs and microglia in the ischemic brain. The phagocytic activities of MDMs and microglia were measured by the uptake of fluorescent beads both in vivo with mice infused with GFP+ splenocytes and ex vivo with cultures of isolated brain immune cells. Results Stroke induced an infiltration of MDMs [GFP+] into the ipsilateral hemisphere at acute (3 days) and sub-acute phases (7 days) of post-stroke. At 7 days, the infiltrating MDMs contained both CD45High and CD45Low subsets. The CD45High MDMs in the injured hemisphere exhibited a significantly higher proliferation capacity (Ki-67 expression levels) as well as higher expression levels of CD11c when compared to CD45Low MDMs. The CD45High and CD45Low MDM subsets in the injured hemisphere were approximately equal populations, indicating that CD45High MDMs infiltrating the ischemic brain changes their phenotype to CD45Low microglia-like phenotype. Studies with fluorescent beads reveal high levels of MDM phagocytic activity in the post-stroke brain, but this phagocytic activity was exclusive to post-ischemic brain tissue and was not detected in circulating monocytes. By contrast, CD45Low microglia-like cells had low levels of phagocytic activity when compared to CD45High cells. Both in vivo and ex vivo studies also show that the phagocytic activity in CD45High MDMs is associated with an increase in the CD45Low/CD45High ratio, indicating that phagocytosis promotes MDM phenotype conversion. Conclusions This study demonstrates that MDMs are the predominant phagocytes in the post-ischemic brain, with the CD45High subset having the highest phagocytic activity levels. Upon phagocytosis, CD45High MDMs in the post-ischemic brain adopt a CD45Low phenotype that is microglia-like. Together, these studies reveal key roles for MDMs and their phagocytic function in tissue repair and remodeling following cerebral ischemia.

Published

2022

45. The generation, activation, and polarization of monocyte-derived macrophages in human malignancies

Author

Paul Chaintreuil, Emeline Kerreneur, Maxence Bourgoin, Coline Savy, Cécile Favreau, Guillaume Robert, Arnaud Jacquel, and Patrick Auberger

Subjects

monocyte-derived macrophages, CSF-1, differentiation, polarization, TAM, LAM, Immunologic diseases. Allergy, RC581-607

Abstract

Macrophages are immune cells that originate from embryogenesis or from the differentiation of monocytes. They can adopt numerous phenotypes depending on their origin, tissue distribution and in response to different stimuli and tissue environment. Thus, in vivo, macrophages are endowed with a continuum of phenotypes that are rarely strictly pro-inflammatory or anti-inflammatory and exhibit a broad expression profile that sweeps over the whole polarization spectrum. Schematically, three main macrophage subpopulations coexist in human tissues: naïve macrophages also called M0, pro-inflammatory macrophages referred as M1 macrophages, and anti-inflammatory macrophages also known as M2 macrophages. Naïve macrophages display phagocytic functions, recognize pathogenic agents, and rapidly undergo polarization towards pro or anti-inflammatory macrophages to acquire their full panel of functions. Pro-inflammatory macrophages are widely involved in inflammatory response, during which they exert anti-microbial and anti-tumoral functions. By contrast, anti-inflammatory macrophages are implicated in the resolution of inflammation, the phagocytosis of cell debris and tissue reparation following injuries. Macrophages also play important deleterious or beneficial roles in the initiation and progression of different pathophysiological settings including solid and hematopoietic cancers. A better understanding of the molecular mechanisms involved in the generation, activation and polarization of macrophages is a prerequisite for the development of new therapeutic strategies to modulate macrophages functions in pathological situations.

Published

2023

46. Mouse Tissue‐Resident Peritoneal Macrophages in Homeostasis, Repair, Infection, and Tumor Metastasis

Author

Carlos Ardavín, Natalia Alvarez‐Ladrón, Margarita Ferriz, Alejandra Gutiérrez‐González, and Adrián Vega‐Pérez

Subjects

macrophages, monocyte‐derived macrophages, peritoneal cavity, peritoneal injury, peritoneal metastasis, peritoneal sepsis, Science

Abstract

Abstract Large peritoneal macrophages (LPMs) are long‐lived, tissue‐resident macrophages, formed during embryonic life, developmentally and functionally confined to the peritoneal cavity. LPMs provide the first line of defense against life‐threatening pathologies of the peritoneal cavity, such as abdominal sepsis, peritoneal metastatic tumor growth, or peritoneal injuries caused by trauma, or abdominal surgery. Apart from their primary phagocytic function, reminiscent of primitive defense mechanisms sustained by coelomocytes in the coelomic cavity of invertebrates, LPMs fulfill an essential homeostatic function by achieving an efficient clearance of apoptotic, that is crucial for the maintenance of self‐tolerance. Research performed over the last few years, in mice, has unveiled the mechanisms by which LPMs fulfill a crucial role in repairing peritoneal injuries and controlling microbial and parasitic infections, reflecting that the GATA6‐driven LPM transcriptional program can be modulated by extracellular signals associated with pathological conditions. In contrast, recent experimental evidence supports that peritoneal tumors can subvert LPM metabolism and function, leading to the acquisition of a tumor‐promoting potential. The remarkable functional plasticity of LPMs can be nevertheless exploited to revert tumor‐induced LPM protumor potential, providing the basis for the development of novel immunotherapeutic approaches against peritoneal tumor metastasis based on macrophage reprogramming.

Published

2023

47. Endothelial Toll-like receptor 4 is required for microglia activation in the murine retina after systemic lipopolysaccharide exposure.

Author

Tsioti, Ioanna, Steiner, Beatrice L., Escher, Pascal, Zinkernagel, Martin S., Benz, Peter M., and Kokona, Despina

Subjects

*RETINAL injuries, *TOLL-like receptors, *MICROGLIA, *VASCULAR endothelial cells, *RETINA, *LIPOPOLYSACCHARIDES

Abstract

Background: Clustering of microglia around the vasculature has been reported in the retina and the brain after systemic administration of lipopolysaccharides (LPS) in mice. LPS acts via activation of Toll-like receptor 4 (TRL4), which is expressed in several cell types including microglia, monocytes and vascular endothelial cells. The purpose of this study was to investigate the effect of systemic LPS in the pigmented mouse retina and the involvement of endothelial TLR4 in LPS-induced retinal microglia activation. Methods: C57BL/6J, conditional knockout mice that lack Tlr4 expression selectively on endothelial cells (TekCre−posTlr4loxP/loxP) and TekCre−negTlr4loxP/loxP mice were used. The mice were injected with 1 mg/kg LPS via the tail vein once per day for a total of 4 days. Prior to initiation of LPS injections and approximately 5 h after the last injection, in vivo imaging using fluorescein angiography and spectral-domain optical coherence tomography was performed. Immunohistochemistry, flow cytometry, electroretinography and transmission electron microscopy were utilized to investigate the role of endothelial TLR4 in LPS-induced microglia activation and retinal function. Results: Activation of microglia, infiltration of monocyte-derived macrophages, impaired ribbon synapse organization and retinal dysfunction were observed after the LPS exposure in C57BL/6J and TekCre−negTlr4loxP/loxP mice. None of these effects were observed in the retinas of conditional Tlr4 knockout mice after the LPS challenge. Conclusions: The findings of the present study suggest that systemic LPS exposure can have detrimental effects in the healthy retina and that TLR4 expressed on endothelial cells is essential for retinal microglia activation and retinal dysfunction upon systemic LPS challenge. This important finding provides new insights into the role of microglia–endothelial cell interaction in inflammatory retinal disease. [ABSTRACT FROM AUTHOR]

Published

2023

48. The Role of Macrophages in Atherosclerosis: Participants and Therapists

Author

Liu, Xiaoyu, Pang, Shuchao, Jiang, Yangyang, Wang, Lixin, and Liu, Yi

Published

2023

49. Dasatinib interferes with HIV-1 proviral integration and the inflammatory potential of monocyte-derived macrophages from people with HIV.

Author

Rodríguez-Mora, Sara, Sánchez-Menéndez, Clara, Bautista-Carrascosa, Guiomar, Mateos, Elena, Moreno-Serna, Lucia, Megías, Diego, Cantón, Juan, García-Gutiérrez, Valentín, Murciano-Antón, María Aránzazu, Cervero, Miguel, Spivak, Adam, Planelles, Vicente, and Coiras, Mayte

Subjects

*PROTEIN-tyrosine kinase inhibitors, *CHRONIC myeloid leukemia, *DASATINIB, *ANTIRETROVIRAL agents, *GENETIC transcription

Abstract

[Display omitted] HIV-1 infection is efficiently controlled by the antiretroviral treatment (ART) but viral persistence in long-lived reservoirs formed by CD4 + T cells and macrophages impedes viral eradication and creates a chronic inflammatory environment. Dasatinib is a tyrosine kinase inhibitor clinically used against chronic myeloid leukemia (CML) that has also showed an anti-inflammatory potential. We previously reported that dasatinib is very efficient at interfering with HIV-1 infection of CD4 + T cells by preserving the antiviral activity of SAMHD1, an innate immune factor that blocks T-cell activation and proliferation and that is inactivated by phosphorylation at T592 (pSAMHD1). We observed that short-term treatment in vitro with dasatinib significantly reduced pSAMHD1 in monocyte-derived macrophages (MDMs) isolated from people with HIV (PWH) and healthy donors, interfering with HIV-1 infection. This inhibition was based on low levels of 2-LTR circles and proviral integration, while viral reverse transcription was not affected. MDMs isolated from people with CML on long-term treatment with dasatinib also showed low levels of pSAMHD1 and were resistant to HIV-1 infection. In addition, dasatinib decreased the inflammatory potential of MDMs by reducing the release of M1-related cytokines like TNFα, IL-1β, IL-6, CXCL8, and CXCL9, but preserving the antiviral activity through normal levels of IL-12 and IFNγ. Due to the production of M2-related anti-inflammatory cytokines like IL-1RA and IL-10 was also impaired, dasatinib appeared to interfere with MDMs differentiation. The use of dasatinib along with ART could be used against HIV-1 reservoir in CD4 and macrophages and to alleviate the chronic inflammation characteristic of PWH. [ABSTRACT FROM AUTHOR]

Published

2024

50. Glycyrrhizic acid alleviates concanavalin A-induced acute liver injury by regulating monocyte-derived macrophages.

Author

Lu, Juan, Gu, Xinyu, Xue, Chen, Shi, Qingmiao, Jia, Junjun, Cheng, Jinlin, Zeng, Yifan, Chu, Qingfei, Yuan, Xin, Bao, Zhengyi, and Li, Lanjuan

Abstract

• Glycyrrhizic acid (GA) intervention significantly alleviated concanavalin A (ConA)-induced acute liver injury in mice. • CyTOF analysis revealed that GA increased the abundance of anti-inflammatory F4/80loCD11bhiMHCIIhi MoMF-1. • GA decreased the abundance of pro-inflammatory F4/80loCD11bhiiNOShi MoMF-3. • scRNA-seq analysis indicated that GA facilitated the immune activation of MoMFs, and regulated the gene expression of diverse cytokines secreted by MoMFs. Autoimmune hepatitis (AIH) is characterized by persistent liver inflammation induced by aberrant immune responses. Glycyrrhizic acid (GA), a prominent bioactive ingredient of licorice, has shown potential as a safe and effective treatment for AIH. However, the immune regulatory mechanism by which GA exerts its therapeutic effect on AIH remains elusive. In this study, we found that GA intervention significantly alleviated ConA-induced acute liver injury in mice. Cytometry by time-of-flight (CyTOF) analysis revealed that GA increased the abundance of anti-inflammatory F4/80loCD11bhiMHCIIhi MoMF-1 and decreased the abundance of pro-inflammatory F4/80loCD11bhiiNOShi MoMF-3. Multiplex immunofluorescence demonstrated the infiltration of MoMFs in liver tissues. Single-cell RNA sequencing (scRNA-seq) analysis indicated that GA facilitated the immune activation in MoMFs, regulated gene expression of diverse cytokines secreted by MoMFs, and played a role in shaping the immune microenvironment. By integrating the results of CyTOF with scRNA-seq, our study comprehensively elucidates the immune landscape of ConA-induced liver injury following GA intervention, advancing the understanding of GA's mechanism of action. However, it is important to note that some single-cell data in this study remain raw and require further processing and annotation. Our findings suggest that GA alleviates ConA-induced acute liver injury by regulating the function of MoMFs, opening potential avenues for AIH treatment and management, and providing a theoretical basis for the design of novel MoMFs-centered immunotherapies. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024