Your search keyword '"MACROPHAGE POLARIZATION"' showing total 11,893 results

151. Modified Si Miao Powder granules alleviates osteoarthritis progression by regulating M1/M2 polarization of macrophage through NF-κB signaling pathway.

Author

Qi He, Ding Tian, Zhiyuan Wang, Dan Zheng, Liqiang Zhi, Jianbing Ma, Jing An, and Rui Zhang

Subjects

HERBAL medicine, CHINESE medicine, ANCIENT medicine, LABORATORY mice, DEGENERATION (Pathology)

Abstract

Background: Osteoarthritis (OA) is a chronic degenerative disease mainly characterized by cartilage damage and synovial inflammation. Si Miao Powder, an herbal formula, was recorded in ancient Chinese medicine prescription with excellent anti-inflammatory properties. Based on the classical formula, the modified Si Miao Powder (MSMP) was developed with the addition of two commonly Chinese orthopedic herbs, which had the efficacy of strengthening the therapeutic effect for OA. Methods: In the in vivo experiments, thirty-six 8-week-old male C57BL/6mice were randomly divided into six groups: sham group, OA group, celecoxib group, low-MSMP group, middle-MSMP group, and high-MSMP group. OA mice were constructed by destabilization of medial meniscus (DMM) and treated with MSMP granules or celecoxib by gavage. The effects of MSMP on cartilage, synovitis and inflammatory factor of serum were tested. For in vitro experiments, control serum and MSMP-containing serum were prepared from twenty-five C57BL/6 mice. Macrophages (RAW264.7 cells) were induced by lipopolysaccharide (LPS) and then treated with MSMP-containing serum. The expression of inflammatory factors and the change of the NF-κB pathway were tested. Results: In vivo, celecoxib and MSMP alleviated OA progression in the treated groups compared with OA group. The damage was partly recovered in cartilage, the synovial inflammatory were reduced in synovium, and the concentrations of IL-6 and TNF-α were reduced and the expression of IL-10 was increased in serum. The function of the middle MSMP was most effective for OA treatment. The results of in vitro experiments showed that compared with the LPS group, the MSMP-containing serum significantly reduced the expression levels of pro-inflammatory (M1-type) factors, such as CD86, iNOS, TNF-α and IL-6, and promoted the expression levels of anti-inflammatory (M2-type) factors, such as Arg1 and IL-10. The MSMP-containing serum further inhibited NF-κB signaling pathway after LPS induction. Conclusion: The study demonstrated that MSMP alleviated OA progression in mice and MSMP-containing serum modulated macrophage M1/M2 phenotype by inhibiting the NF-κB signaling pathway. Our study provided experimental evidence and therapeutic targets of MSMP for OA treatment. [ABSTRACT FROM AUTHOR]

Published

2024

152. Novel insights into vancomycin-loaded calcium sulfate and negative pressure wound therapy in preventing infections in open fractures.

Author

Jia, Bei, Xue, Rui, Li, Jia, Guo, Jichao, and Liu, Jianning

Subjects

*INFECTION prevention, *WOUND healing, *FLOW cytometry, *MACROPHAGES, *GENOMICS, *CLUSTER analysis (Statistics), *T-test (Statistics), *DATA analysis, *ENZYME-linked immunosorbent assay, *KRUSKAL-Wallis Test, *COMPOUND fractures, *REVERSE transcriptase polymerase chain reaction, *MANN Whitney U Test, *STAPHYLOCOCCUS aureus, *DESCRIPTIVE statistics, *VANCOMYCIN, *NEGATIVE-pressure wound therapy, *CALCIUM compounds, *MICE, *RNA, *ANIMAL experimentation, *GENE expression profiling, *WESTERN immunoblotting, *ANALYSIS of variance, *STATISTICS, *BACTERIAL diseases, *SURGICAL site infections, *COMPARATIVE studies, *STAINS & staining (Microscopy), *DATA analysis software, *SEQUENCE analysis

Abstract

Background: Open fractures are challenging due to susceptibility to Staphylococcus aureus infections. This study examines the impact of Vancomycin-Loaded Calcium Sulfate (VLCS) and negative pressure wound therapy (NPWT) on macrophage behavior in enhancing healing and infection resistance. Both VLCS and NPWT were evaluated individually and in combination to determine their effects on macrophage polarization and infection resistance in open fractures. Methods: Through single-cell RNA sequencing, genomic expressions in macrophages from open fracture patients treated with VLCS and NPWT were compared to a control group. The analysis focused on MBD2 gene changes related to macrophage polarization. Results: Remarkable modifications in MBD2 expression in the treatment group indicate a shift towards M2 macrophage polarization. Additionally, the combined treatment group exhibited greater improvements in infection resistance and healing compared to the individual treatments. This shift suggests a healing-promoting atmosphere with improved infection resilience. Conclusions: VLCS and NPWT demonstrate the ability to alter macrophage behavior toward M2 polarization, which is crucial for infection prevention in open fractures. The synergistic effect of their combined use shows even greater promise in enhancing outcomes in orthopedic trauma care. [ABSTRACT FROM AUTHOR]

Published

2024

153. Ovarian cancer derived extracellular vesicles promote the cancer progression and angiogenesis by mediating M2 macrophages polarization.

Author

Tang, Xue, Ma, Chengbin, Wu, Qiongwei, and Yu, Meng

Subjects

*EXTRACELLULAR vesicles, *CANCER invasiveness, *OVARIAN cancer, *CANCER prognosis, *CANCER cells

Abstract

Background: Extracellular vesicles (EVs) are mediators between cancer cells and other types of cells, such as tumor-associated macrophages (TAMs), in the tumor microenvironment. EVs can remodel the tumor microenvironment and regulate tumor progression. However, the underlying molecular mechanism of these interactions remains unclear. Methods: First, we explored the effect of TAMs on the survival prognosis of patients with ovarian cancer. Next, we isolated EVs derived from ovarian cancer cells (OV-EVs) through ultracentrifugation and analyzed the capacity of OV-EVs to regulate macrophage polarization in ovarian tumors and in whole peripheral blood. Moreover, we explored the roles of OV-EVs-induced macrophages in tumor progression through in vitro and in vivo assays. Results: OV-EVs were encapsulated by macrophages and induced the polarization of macrophages toward the M2 phenotype. Moreover, OV-EVs-induced M2 macrophages promoted angiogenesis and cancer progression both in vitro and in vivo. In addition, OV-EVs-induced macrophages increased the expression level of VEGF and increased the expression level of VEGFR in tumors, which resulted in angiogenesis in ovarian cancer. Conclusions: The present study demonstrated that OV-EVs induce M2 polarization in macrophages and promote the progression of ovarian cancer. This study provides novel insight into the mechanism of ovarian cancer progression. [ABSTRACT FROM AUTHOR]

Published

2024

154. Mn-ZIF nanozymes kill tumors by generating hydroxyl radical as well as reversing the tumor microenvironment.

Author

Jiyu Han, Hairong Ma, Songtao Ai, and Daqian Wan

Subjects

HYDROXYL group, TUMOR microenvironment, HABER-Weiss reaction, METAL-organic frameworks, SYNTHETIC enzymes

Abstract

Tumor tissues are well known for their unique high hydrogen peroxide (H2O2) microenvironment. How to exploit this tumor microenvironment for tumor cell killing is a question. In this study, a Mn-doped metal-organic framework (Mn-ZIF) was constructed. It possesses good peroxidase (POD) activity, which can oxidize tumor-localized H2O2 into hydroxyl radicals (·OH), that possesses the ability to directly kill tumor cells. More surprisingly, in vivo experiments the researchers not only observed the tumor-killing effect of Mn-ZIF, but also found it changes in macrophage phenotype in the tumor region. There was an increase in macrophage polarization towards the M1 subtype. This suggests that the tumor-killing effect of Mn-ZIF not only comes from its POD activity, but also regulates the immune microenvironment in the tumor region. In conclusion, the preparation of Mn-ZIF provides a new way for comprehensive tumor therapy. [ABSTRACT FROM AUTHOR]

Published

2024

155. S-adenosyl-L-methionine supplementation alleviates aortic dissection by decreasing inflammatory infiltration.

Author

Wang, Qian, An, Jun, Zhou, Wei, Zhang, Yujing, Huang, Jiang, Liao, Geping, Wang, Mingzhe, Xia, Lingbo, Le, Aiping, and Zhu, Jianbing

Subjects

*INFLAMMATION prevention, *FLOW cytometry, *RESEARCH funding, *MACROPHAGES, *T cells, *AORTIC dissection, *NEUTROPHILS, *MAJOR histocompatibility complex, *MICE, *GENE expression, *ANIMAL experimentation, *ONE-way analysis of variance, *CYTOKINES, *DIETARY supplements, *ADENOSYLMETHIONINE, *INTERLEUKINS, *TUMOR necrosis factors

Abstract

Methionine, an indispensable amino acid crucial for dietary balance, intricately governs metabolic pathways. Disruption in its equilibrium has the potential to heighten homocysteine levels in both plasma and tissues, posing a conceivable risk of inducing inflammation and detriment to the integrity of vascular endothelial cells. The intricate interplay between methionine metabolism, with a specific focus on S-adenosyl-L-methionine (SAM), and the onset of thoracic aortic dissection (TAD) remains enigmatic despite acknowledging the pivotal role of inflammation in this vascular condition. In an established murine model induced by β-aminopropionitrile monofumarate (BAPN), we delved into the repercussions of supplementing with S-adenosyl-L-methionine (SAM) on the progression of TAD. Our observations uncovered a noteworthy improvement in aortic dissection and rupture rates, accompanied by a marked reduction in mortality upon SAM supplementation. Notably, SAM supplementation exhibited a considerable protective effect against BAPN-induced degradation of elastin and the extracellular matrix. Furthermore, SAM supplementation demonstrated a robust inhibitory influence on the infiltration of immune cells, particularly neutrophils and macrophages. It also manifested a notable reduction in the inflammatory polarization of macrophages, evident through diminished accumulation of MHC-IIhigh macrophages and reduced expression of inflammatory cytokines such as IL1β and TNFα in macrophages. Simultaneously, SAM supplementation exerted a suppressive effect on the activation of CD4 + and CD8 + T cells within the aorta. This was evidenced by an elevated proportion of CD44- CD62L + naïve T cells and a concurrent decrease in CD44 + CD62L- effector T cells. In summary, our findings strongly suggest that the supplementation of SAM exhibits remarkable efficacy in alleviating BAPN-induced aortic inflammation, consequently impeding the progression of thoracic aortic dissection. [ABSTRACT FROM AUTHOR]

Published

2024

156. A Multifunctional Tissue‐Engineering Hydrogel Aimed to Regulate Bacterial Ferroptosis‐Like Death and Overcoming Infection Toward Bone Remodeling.

Author

Lu, Renjie, Luo, Zhiyuan, Zhang, Yuanyuan, Chen, Jiahao, Zhang, Yang, and Zhang, Chi

Subjects

*BIOPOLYMERS, *BACTERIAL metabolism, *IRON metabolism, *CELL physiology, *EXTRACELLULAR matrix

Abstract

Infection is the most common complication after orthopedic surgery and can result in prolonged ailments such as chronic wounds, enlarged bone defects, and osteomyelitis. Iron, which is essential for bacterial metabolism and immune cell functions, is extremely important. Bacteria harness iron from nearby cells to promote biofilm formation, ensuring their survival. Iron deficiency within the infection microenvironment (IME) consequently hampers macrophage function, enabling further dissemination of the infection and hindering macrophage polarization to the M2 phenotype. Therefore, a novel approach is proposed to regulate macrophage polarization, aiming to restore the inflammatory immune environment. A composite hydrogel derived from natural polymers is developed to address infections and manage iron metabolism in macrophages. This IME‐responsive hydrogel, named FCL‐ECMH, is synthesized by encapsulating vermiculite functional core layers within a decellularized extracellular matrix hydrogel. It is noteworthy that FCL‐ECMH can produce reactive oxygen species within the IME. Supplementary photothermal treatment enhances bacterial iron uptake, leading to ferroptosis‐like death. This process also rejuvenates the iron‐enriched macrophages around the IME, thereby enhancing their antibacterial and tissue repair functions. In vivo experiments confirmed the antibacterial and repair‐promoting capabilities of FCL‐ECMH, indicating its potential for clinical applications. [ABSTRACT FROM AUTHOR]

Published

2024

157. β,β-Dimethylacrylalkannin, a Natural Naphthoquinone, Inhibits the Growth of Hepatocellular Carcinoma Cells by Modulating Tumor-Associated Macrophages.

Author

Shen, Li-Sha, Lin, Zesi, Gong, Rui-Hong, Lin, Yu-Shan, Qiao, Xing-Fang, Hu, Qian-Mei, Qin, Wei-Han, Chen, Sibao, Yang, Yong, and Chen, Guo-Qing

Subjects

*HEPATOCELLULAR carcinoma, *CANCER invasiveness, *TUMOR microenvironment, *CELL growth, *NAPHTHOQUINONE

Abstract

Tumor-associated macrophages (TAMs) are pivotal in the tumor microenvironment (TME) of hepatocellular carcinoma (HCC), influencing various stages from initiation to metastasis. Understanding the role of TAMs in HCC is crucial for developing novel therapeutic strategies. Macrophages exhibit plasticity, resulting in M1 and M2 phenotypes, with M1 macrophages displaying antitumor properties and M2 macrophages promoting tumor progression. Targeting TAMs to alter their polarization could offer new avenues for HCC treatment. β,β-dimethylacrylalkannin (DMAKN), a natural naphthoquinone, has gained attention for its antitumor properties. However, its impact on TAMs modulation remains unclear. This study investigates DMAKN's modulation of TAMs and its anti-HCC activity. Using an in vitro model with THP-1 cells, we induced M1 macrophages with LPS/IFN-γ and M2 macrophages with IL-4/IL-13, confirming polarization with specific markers. Co-culturing these macrophages with HCC cells showed that M1 cells inhibited HCC growth, while M2 cells promoted it. Screening for non-toxic DMAKN concentrations revealed its ability to induce M1 polarization and enhance LPS/IFN-γ-induced M1 macrophages, both showing anti-HCC effects. Conversely, DMAKN suppressed IL-4/IL-13-induced M2 polarization, inhibiting M2 macrophages' promotion of HCC cell viability. In summary, DMAKN induces and enhances M1 polarization while inhibiting M2 polarization of macrophages, thereby inhibiting HCC cell growth. These findings suggest that DMAKN has the potential to regulate TAMs in HCC, offering promise for future therapeutic development. [ABSTRACT FROM AUTHOR]

Published

2024

158. The biological applications of near-infrared optical nanomaterials in atherosclerosis.

Author

Shen, Lin, Bi, Yanran, Yu, Junchao, Zhong, Yi, Chen, Weiqian, Zhao, Zhongwei, Ding, Jiayi, Shu, Gaofeng, Chen, Minjiang, Lu, Chenying, and Ji, Jiansong

Subjects

*CARDIOVASCULAR disease diagnosis, *ATHEROSCLEROTIC plaque, *NANOPARTICLES, *VASCULAR diseases, *ANGIOGRAPHY

Abstract

Purpose of review: Atherosclerosis, a highly pathogenic and lethal disease, is difficult to locate accurately via conventional imaging because of its scattered and deep lesions. However, second near-infrared (NIR-II) nanomaterials show great application potential in the tracing of atherosclerotic plaques due to their excellent penetration and angiographic capabilities. Recent findings: With the development of nanotechnology, among many nanomaterials available for the visual diagnosis and treatment of cardiovascular diseases, optical nanomaterials provide strong support for various biomedical applications because of their advantages, such as noninvasive, nondestructive and molecular component imaging. Among optical nanomaterials of different wavelengths, NIR-II-range (900 ~ 1700 nm) nanomaterials have been gradually applied in the visual diagnosis and treatment of atherosclerosis and other vascular diseases because of their deep biological tissue penetration and limited background interference. Summary: This review explored in detail the prospects and challenges of the biological imaging and clinical application of NIR-II nanomaterials in treating atherosclerosis. [ABSTRACT FROM AUTHOR]

Published

2024

159. Class A1 scavenger receptor antibody improves murine colitis by influencing macrophage and gut microbiota.

Author

Su, Jingling, Liu, Lupeng, Ren, Yandan, Gan, Yutong, Lin, Yumei, and Xie, Chenxi

Abstract

This study aimed to investigate whether class A1 scavenger receptor (SR-A1) regulated macrophage polarization and gut microbial alteration during intestinal inflammation of colitis. A murine colitis model was established by feeding with dextran sulfate sodium (DSS), and treatment groups were injected intravenously with SR-A1 antibody. Results showed a preventive effect on colitis symptoms and fewer inflammatory cell infiltrates in treatment groups. Down-regulation of inflammatory cytokines and up-regulation of anti-inflammatory cytokine related to macrophages were seen in murine PBMC and LPMC after injected with SR-A1 antibody. The percentage of M2 macrophages was also elevated in treatment groups. In addition, SR-A1 antibody treatment resulted in the decreased apoptosis and increased proliferation of colonic epithelial cells. Other findings indicated that SR-A1 antibody injection could mediate its anti-inflammatory effect via inhibiting TLR4-MyD88-NF-kB signaling pathway and alterating the gut microbiota composition. Our research identified SR-A1 as a potential therapeutic target in inflammatory bowel disease (IBD). [ABSTRACT FROM AUTHOR]

Published

2024

160. Biomimetic HA-GO implant coating for enhanced osseointegration via macrophage M2 polarization-induced osteo-immunomodulation.

Author

Baheti, Wufanbieke, Chen, Xiaotao, La, Mi, and He, Huiyu

Subjects

*MESENCHYMAL stem cells, *BONE marrow, *ELECTROPHORETIC deposition, *GRAPHENE oxide, *OXIDE coating

Abstract

The pro-inflammatory/anti-inflammatory polarized phenotypes of macrophages (M1/M2) can be used to predict the success of implant integration. Hence, activating and inducing the transformation of immunocytes that promote tissue repair appears to be a highly promising strategy for facilitating osteo-anagenesis. In a previous study, titanium implants were coated with a graphene oxide-hydroxyapatite (GO-HA) nanocomposite via electrophoretic deposition, and the osteogenic differentiation of bone marrow mesenchymal stem cells (BMSCs) was found to be significantly enhanced when the GO content was 2wt%. However, the effectiveness of the GO-HA nanocomposite coating in modifying the in vivo immune microenvironment still remains unclear. In this study, the effects of GO-HA coatings on osteogenesis were investigated based on the GO-HA-mediated immune regulation of macrophages. The HA-2wt%GO nanocomposite coatings exhibited good biocompatibility and favored M2 macrophage polarization. Meanwhile, they could also significantly upregulate IL-10 (anti-inflammatory factor) expression and downregulate TNF-α (pro-inflammatory factor) expression. Additionally, the microenvironment, which was established by M2 macrophages, favored the osteogenesis of BMSCs both in vivo and in vitro. These findings show that the GO-HA nanocomposite coating is a promising surface-modification material. Hence, this study provides a reference for the development of next-generation osteoimmunomodulatory biomaterials. [ABSTRACT FROM AUTHOR]

Published

2024

161. Gastric cancer cell-derived exosomal miR-541-5p induces M2 macrophage polarization through DUSP3/JAK2/STAT3 pathway.

Author

Xiao, Haimin, Fu, Jia, Liu, Ruiting, Yan, Likun, Zhou, Zheqi, and Yuan, Jinyan

Subjects

*CELL populations, *JAK-STAT pathway, *STOMACH cancer, *EXOSOMES, *MACROPHAGE activation

Abstract

Purpose: Exosomal microRNAs have been identified as important mediators of communication between tumor cells and macrophages in the microenvironment. miR-541-5p was reported to be involved in hepatocellular carcinoma progression, but its role in gastric cancer (GC) and in GC cell-macrophage crosstalk is unknown. Methods: Cell proliferation, migration and invasion were respectively assessed by CCK-8 assay, scratch and Transwell assays. RT-qPCR was used to detect the level of miR-541-5p, macrophage markers and DUSP3. The percentage of CD11b+CD206+ cell population was analyzed by flow cytometry. Western blotting was employed to evaluate DUSP3-JAK2/STAT3 pathway proteins and exosome markers. The interaction between miR-541-5p and DUSP3 was verified by luciferase assay. Results: The results showed that miR-541-5p was upregulated in GC tissues and cells, and stimulated GC cell growth, migration and invasion in vitro. GC cells induce M2 macrophage polarization by secreting the exosomal miR-541-5p. Exosomal miR-541-5p maintained JAK2/STAT3 pathway activation in macrophages by targeting negative regulation of DUSP3. Inhibiting miR-541-5p significantly limited tumor growth in vivo. Conclusion: In conclusion, miR-541-5p promotes GC cell progression. GC cells may induce macrophage M2 polarization through the exosomal miR-541-5p-mediated DUSP3/JAK2/STAT3 pathway. miR-541-5p may be a potential therapeutic target for GC. [ABSTRACT FROM AUTHOR]

Published

2024

162. Construction and validation of prognostic signatures related to mitochondria and macrophage polarization in gastric cancer.

Author

Yan Zhang, Jian Cao, Zhen Yuan, Hao Zuo, Jiacong Yao, Xiaodie Tu, and Xinhua Gu

Subjects

DISEASE risk factors, GENE expression, GENE regulatory networks, STOMACH cancer, STROMAL cells

Abstract

Background: Increasing evidence reveals the involvement of mitochondria and macrophage polarisation in tumourigenesis and progression. This study aimed to establish mitochondria and macrophage polarisation-associated molecular signatures to predict prognosis in gastric cancer (GC) by single-cell and transcriptional data. Methods: Initially, candidate genes associated with mitochondria and macrophage polarisation were identified by differential expression analysis and weighted gene co-expression network analysis. Subsequently, candidate genes were incorporated in univariateCox analysis and LASSO to acquire prognostic genes in GC, and risk model was created. Furthermore, independent prognostic indicators were screened by combining risk score with clinical characteristics, and a nomogram was created to forecast survival in GC patients. Further, in single-cell data analysis, cell clusters and cell subpopulations were yielded, followed by the completion of pseudo-time analysis. Furthermore, a more comprehensive immunological analysis was executed to uncover the relationship between GC and immunological characteristics. Ultimately, expression level of prognostic genes was validated through public datasets and qRT-PCR. Results: A risk model including six prognostic genes (GPX3, GJA1, VCAN, RGS2, LOX, and CTHRC1) associated with mitochondria and macrophage polarisation was developed, which was efficient in forecasting the survival of GC patients. The GC patients were categorized into high-/low-risk subgroups in accordance with median risk score, with the high-risk subgroup having lower survival rates. Afterwards, a nomogram incorporating risk score and age was generated, and it had significant predictive value for predicting GC survival with higher predictive accuracy than risk model. Immunological analyses revealed showed higher levels of M2 macrophage infiltration in high-risk subgroup and the strongest positive correlation between risk score and M2 macrophages. Besides, further analyses demonstrated a better outcome for immunotherapy in low-risk patients. In single-cell and pseudo-time analyses, stromal cells were identified as key cells, and a relatively complete developmental trajectory existed for stromal C1 in three subclasses. Ultimately, expression analysis revealed that the expression trend of RGS2, GJA1, GPX3, and VCAN was consistent with the results of the TCGAGC dataset. Conclusion: Our findings demonstrated that a novel prognostic model constructed in accordance with six prognostic genes might facilitate the improvement of personalised prognosis and treatment of GC patients. [ABSTRACT FROM AUTHOR]

Published

2024

163. Macrophage polarization and its impact on idiopathic pulmonary fibrosis.

Author

Zhouling Ge, Yong Chen, Leikai Ma, Fangjun Hu, and Lubin Xie

Subjects

IDIOPATHIC pulmonary fibrosis, PULMONARY fibrosis, IMMUNE system, RESPIRATORY insufficiency, LUNG diseases

Abstract

Idiopathic pulmonary fibrosis (IPF) is a lung disease that worsens over time, causing fibrosis in the lungs and ultimately resulting in respiratory failure and a high risk of death. Macrophages play a crucial role in the immune system, showing flexibility by transforming into either pro-inflammatory (M1) or antiinflammatory (M2) macrophages when exposed to different stimuli, ultimately impacting the development of IPF. Recent research has indicated that the polarization of macrophages is crucial in the onset and progression of IPF. M1 macrophages secrete inflammatory cytokines and agents causing early lung damage and fibrosis, while M2 macrophages support tissue healing and fibrosis by releasing anti-inflammatory cytokines. Developing novel treatments for IPF relies on a thorough comprehension of the processes involved in macrophage polarization in IPF. The review outlines the regulation of macrophage polarization and its impact on the development of IPF, with the goal of investigating the possible therapeutic benefits of macrophage polarization in the advancement of IPF. [ABSTRACT FROM AUTHOR]

Published

2024

164. Role of macrophage polarization in heart failure and traditional Chinese medicine treatment.

Author

Zheqin Zhu, Min Wang, Shenghua Lu, Sisi Dai, and Jianhe Liu

Subjects

CHINESE medicine, CELL populations, IMMUNE response, HEART failure, DYNAMIC balance (Mechanics)

Abstract

Heart failure (HF) has a severe impact on public health development due to high morbidity and mortality and is associated with imbalances in cardiac immunoregulation. Macrophages, a major cell population involved in cardiac immune response and inflammation, are highly heterogeneous and polarized into M1 and M2 types depending on the microenvironment. M1 macrophage releases inflammatory factors and chemokines to activate the immune response and remove harmful substances, while M2 macrophage releases antiinflammatory factors to inhibit the overactive immune response and promote tissue repair. M1 and M2 restrict each other to maintain cardiac homeostasis. The dynamic balance of M1 and M2 is closely related to the Traditional Chinese Medicine (TCM) yin-yang theory, and the imbalance of yin and yang will result in a pathological state of the organism. Studies have confirmed that TCM produces positive effects on HF by regulating macrophage polarization. This review describes the critical role of macrophage polarization in inflammation, fibrosis, angiogenesis and electrophysiology in the course of HF, as well as the potential mechanism of TCM regulation of macrophage polarization in preventing and treating HF, thereby providing new ideas for clinical treatment and scientific research design of HF. [ABSTRACT FROM AUTHOR]

Published

2024

165. Mesenchymal stromal cell-derived exosomes protect against abdominal aortic aneurysm formation through CD74 modulation of macrophage polarization in mice.

Author

Xu, Jiamin, Zhao, Jiling, Chen, Haiting, Tan, Xi, Zhang, Wenfeng, Xia, Zhongnan, Yao, Dejiang, Lei, Yuhua, Xu, Biao, Wei, Zhonghai, and Hu, Jiaxin

Subjects

*ABDOMINAL aortic aneurysms, *TREATMENT effectiveness, *ANGIOTENSIN II, *TRANSMISSION electron microscopy, *STROMAL cells

Abstract

Background: Mesenchymal stromal cell (MSC)-derived exosomes (MSC-Exo) have been recognized for their significant role in regulating macrophage polarization, a process crucial to the pathogenesis of abdominal aortic aneurysm (AAA). However, the therapeutic effects of MSC-Exo on AAA remain largely unexplored. Therefore, this study aimed to investigate the functional and mechanistic aspects of MSC-Exo in the progression of AAA. Methods: The MSC-derived exosomes were characterized using Transmission Electron Microscopy, Nanoparticle Tracking Analysis, and Western blotting. An experimental mouse model of AAA was established through the administration of angiotensin II (Ang II) in male apoe−/− mice and calcium chloride (CaCl2) in male C57/B6 mice, with subsequent tail vein injection of exosomes to evaluate their efficacy against AAA. Macrophage polarization was assessed using immunofluorescence staining and WB analysis. Mechanistic analysis was performed using 4D Label-free Proteomics analysis. Results: We found that intravenous administration of MSC-Exo induced M2 polarization of macrophages within an inflammatory environment, effectively impeding AAA development in Ang II or CaCl2-induced AAA model. The therapeutic efficacy of MSC-Exo treatment was dependent on the presence of macrophages. Mechanistically, MSC-Exo suppressed the levels of cluster of differentiation 74 (CD74), modulating macrophage polarization through the TSC2-mTOR-AKT pathway. These findings highlight the potential of MSC-Exo as a therapeutic strategy for AAA by modulating macrophage polarization. [ABSTRACT FROM AUTHOR]

Published

2024

166. Formononetin Alleviates Ischemic Acute Kidney Injury by Regulating Macrophage Polarization through KLF6/STAT3 Pathway.

Author

Zhang, Ning-Xin, Guan, Chen, Li, Chen-Yu, Xu, Ling-Yu, Xin, Yan-Lu, Song, Zhuo, Li, Tian-Yang, Yang, Cheng-Yu, Zhao, Long, Che, Lin, Wang, Yan-Fei, Man, Xiao-Fei, and Xu, Yan

Subjects

*ACUTE kidney failure prevention, *CHINESE medicine, *BIOLOGICAL models, *IN vitro studies, *FLOW cytometry, *MACROPHAGES, *CARRIER proteins, *ISCHEMIA, *RESEARCH funding, *DATA analysis, *ISOFLAVONES, *ENZYME-linked immunosorbent assay, *CELLULAR signal transduction, *TRANSCRIPTION factors, *IN vivo studies, *BLOOD urea nitrogen, *REVERSE transcriptase polymerase chain reaction, *DNA, *MICE, *RNA, *IMMUNOHISTOCHEMISTRY, *ANIMAL experimentation, *WESTERN immunoblotting, *ONE-way analysis of variance, *STATISTICS, *CYTOKINES, *STAINS & staining (Microscopy), *DATA analysis software, *INTERLEUKINS, *TUMOR necrosis factors

Abstract

Recent research has indicated that formononetin demonstrates a potent anti-inflammatory effect in various diseases. However, its impact on sterile inflammation kidney injury, specifically acute kidney injury (AKI), remains unclear. In this study, we utilized an ischemia/reperfusion-induced AKI (IRI-AKI) mouse model and bone marrow-derived macrophages (BMDMs) to investigate the effects of formononetin on sterile inflammation of AKI and to explore the underlying mechanism. The administration of formononetin significantly preserved kidney function from injury, as evidenced by lower serum creatinine and blood urea nitrogen levels compared to IRI-AKI mice without treatment. This was further confirmed by less pathological changes in renal tubules and low expression of tubular injury markers such as KIM-1 and NGAL in the formononetin-treated IRI-AKI group. Furthermore, formononetin effectively suppressed the expression of pro-inflammatory cytokines (MCP-1, TNF-α, and IL-1β) and macrophage infiltration into the kidneys of AKI mice. In vitro studies showed that formononetin led to less macrophage polarization towards a pro-inflammatory phenotype in BMDMs stimulated by LPS and IFN- γ. The mechanism involved the KLF6 and p-STAT3 pathway, as overexpression of KLF6 restored pro-inflammatory cytokine levels and pro-inflammatory polarization. Our findings demonstrate that formononetin can significantly improve renal function and reduce inflammation in IRI-AKI, which may be attributed to the inhibition of KLF6/STAT3-mediated macrophage pro-inflammatory polarization. This discovery presents a new promising therapeutic option for the treatment of IRI-AKI. [ABSTRACT FROM AUTHOR]

Published

2024

167. 微重力介导Notch1 信号通路调控巨噬细胞极化影响骨稳态.

Author

许静, 郭健, 罗永贵, 李大星, 唐英, 娄宝佳, 彭淼, and 郑永

Subjects

*RUNX proteins, *BONE cells, *CELL proliferation, *OSTEOCALCIN, *WESTERN immunoblotting

Abstract

Objective: To investigate the effect of microgravity-mediated Notch1 signaling on macrophage polarization on bone homeostasis. Methods: The animal model was constructed by tail-limb suspension （HLS） to simulate the microgravity environment. The animals were grouped into Control group, HLS group, HLS+NC group, HLS+si group, HLS+rhNF-κB group. ELISA was used to detect the content of TNF-α and IL-1β in serum of rats. TUNEL staining was used to detect the apoptosis of bone tissue. Immunofluorescence was used to detect the polarization of macrophages in bone tissue. The rat osteoblast CP-R091 microgravity model was constructed by simulating the microgravity environment with a rotating wall bioreactor. The cell experiments were divided into Control group, HLS group, HLS+NC group, HLS+si group, HLS+rhNF-κB group. CCK-8 test was used to detect the proliferation activity of cells in each group, and AO test was used to test the apoptosis rate of cells in each group. PCR was used to detect the expression of osteogenesis- related genes in bone tissues and cells. Western blot was used to detect the expression of Notch1, hair division-related enhancer-1 （HES-1）, and Notch pathway ligand 1 （Jagged1） in bone tissues and cells of each group. Results: Compared with control group, the contents of TNF-α and IL-1β in the serum of the rats in the HLS group, the apoptosis rate, and the proportion of M1 macrophages were significantly increased. Compared with HLS group, the HLS+si group could obviously partially reverse the change trend of the above parameters, while HLS+rhNF-κB group significantly changed the above parameter values. Compared with control group, the proliferation activity of the cells in the HLS group was significantly reduced, and the apoptosis rate was significantly increased. Compared with HLS group, the HLS+si group could obviously partially reverse the change trend of the above parameters, while the HLS+ rhNF-κB group made the above parameter values worse. The expressions of the osteogenesis-related genes collagen type Ⅰ（COL1）, osteocalcin （OCN） and Runt-related transcription factor 2 （RUNX2） in bone tissues and cells in the microgravity environment were significantly decreased, while the expressions of Notch-1, Hes-1 and Jagged1 were significantly increased, and the differences were statistically significant （all P<0.05）. Conclusion: Microgravity-mediated Notch1 signaling regulates M1/M2 polarization of macrophages, participates in cell proliferation and apoptosis in bone tissue, and affects the progress of bone homeostasis. [ABSTRACT FROM AUTHOR]

Published

2024

168. TRIM24 调控STAT6 磷酸化介导的巨噬细胞M2 极化缓解病毒性心肌炎.

Author

朱良宇, 李雪琴, 张欣, 殷国泉, 张苑, and 吕坤

Subjects

*COXSACKIEVIRUSES, *STAT proteins, *PHAGOCYTOSIS, *CELLULAR signal transduction, *LABORATORY mice

Abstract

Objective: To study the role and preliminary molecular mechanism of TRIM24 regulating macrophage polarization in viral myocarditis （VM）. Methods: VM mouse model was established by Coxsackie virus B3（ CVB3）, and expression of TRIM24 in myocardial tissue was detected. Cardiac inflammation level and polarization phenotype of cardiac infiltrating macrophages in a murine model of cardiac TRIM24 inhibition were detected in vivo. A polarization model of mouse bone marrow-derived macrophages（ BMDMs） in vitro was established to observe the role of TRIM24 inhibition in polarizing BMDMs to M1 and M2, as well as its effects on phagocytosis and bactericidal function of BMDMs. Effects of TRIM24 inhibition on total STAT6 protein level and phosphorylation were investigated. Results: TRIM24 was significantly highly expressed in myocardial tissue of VM mice （P<0.001）. Inhibition of TRIM24 expression in myocardium had an attenuating effect on VM and promoted polarization of cardiac infiltrating macrophages to M2. TRIM24 was significantly down-regulated in vitro during the polarization of BMDMs toward M2 （P<0.01）. Inhibition of TRIM24 expression significantly promoted macrophage polarization toward M2 type and inhibited polarization toward M1 type, accompanied by a significant increase in STAT6 phosphorylation levels （P<0.01）. Conclusion: TRIM24 regulates macrophage M2 polarization via activation of STAT6 signaling pathway to attenuate VM. [ABSTRACT FROM AUTHOR]

Published

2024

169. Genistein alleviates dextran sulfate sodium-induced colitis in mice through modulation of intestinal microbiota and macrophage polarization.

Author

Jia, Qiang, Fang, Shanshan, Yang, Rui, Ling, Yunzhi, Mehmood, Shomaila, Ni, Hong, and Gao, Qin

Subjects

*MACROPHAGES, *HOMEOSTASIS, *RESEARCH funding, *SHORT-chain fatty acids, *GUT microbiome, *BODY weight, *POLYMERASE chain reaction, *GENISTEIN, *ULCERATIVE colitis, *DESCRIPTIVE statistics, *MICE, *DEXTRAN, *ANIMAL experimentation, *WESTERN immunoblotting, *ONE-way analysis of variance, *INFLAMMATION, *CYTOKINES, *BIOMARKERS

Abstract

Objectives: Ulcerative colitis (UC) is a colonic immune system disorder, manifested with long duration and easy relapse. Genistein has been reported to possess various biological activities. However, it remains unclear whether genistein can ameliorate UC by modulating the homeostasis of the intestinal bacterial community. Methods: The dextran sodium sulfate (DSS)-induced UC mice were administrated with genistein (20 mg/kg/day) or genistein (40 mg/kg/day) for ten days. The general physical condition of the mice was monitored. After sacrifice, the changes in colon length and colonic pathological morphology were observed. The expression of intestinal barrier proteins, inflammatory cytokines, and macrophage markers in the colon was detected. The composition and metabolic products of the intestinal microbiota were analyzed. Results: Genistein treatment visibly improved body weight change and disease activity index in DSS-induced mice. Genistein treatment ameliorated colonic pathological alterations and promoted the expression of mucin-2 and tight junction proteins. Genistein administration inhibited myeloperoxidase activity and colonic inflammatory cytokines. Furthermore, genistein administration improved the structure of the intestinal microbial community, promoted the production of short-chain fatty acids, and modulated macrophage polarization. Conclusions: These results revealed that genistein mediated macrophage polarization balance by improving intestinal microbiota and its metabolites, thereby alleviating DSS-induced colitis. [ABSTRACT FROM AUTHOR]

Published

2024

170. SARS-CoV-2 Modulation of HIV Latency Reversal in a Myeloid Cell Line: Direct and Bystander Effects.

Author

Jarmoluk, Patricio, Sviercz, Franco Agustín, Cevallos, Cintia, Freiberger, Rosa Nicole, López, Cynthia Alicia, Poli, Guido, Delpino, M. Victoria, and Quarleri, Jorge

Subjects

*COVID-19, *MYELOID cells, *TOLL-like receptor agonists, *IMMUNOLOGIC memory, *HIV-positive persons

Abstract

Coronavirus disease 2019 (COVID-19) might impact disease progression in people living with HIV (PLWH), including those on effective combination antiretroviral therapy (cART). These individuals often experience chronic conditions characterized by proviral latency or low-level viral replication in CD4+ memory T cells and tissue macrophages. Pro-inflammatory cytokines, such as TNF-α, IL-1β, IL-6, and IFN-γ, can reactivate provirus expression in both primary cells and cell lines. These cytokines are often elevated in individuals infected with SARS-CoV-2, the virus causing COVID-19. However, it is still unknown whether SARS-CoV-2 can modulate HIV reactivation in infected cells. Here, we report that exposure of the chronically HIV-1-infected myeloid cell line U1 to two different SARS-CoV-2 viral isolates (ancestral and BA.5) reversed its latent state after 24 h. We also observed that SARS-CoV-2 exposure of human primary monocyte-derived macrophages (MDM) initially drove their polarization towards an M1 phenotype, which shifted towards M2 over time. This effect was associated with soluble factors released during the initial M1 polarization phase that reactivated HIV production in U1 cells, like MDM stimulated with the TLR agonist resiquimod. Our study suggests that SARS-CoV-2-induced systemic inflammation and interaction with macrophages could influence proviral HIV-1 latency in myeloid cells in PLWH. [ABSTRACT FROM AUTHOR]

Published

2024

171. Human Umbilical Cord Mesenchymal Stem Cells Promote Anti-Inflammation and Angiogenesis by Targeting Macrophages in a Rat Uterine Scar Model.

Author

Yang, Qian, Huang, Jinfa, Liu, Yixuan, Mai, Qiqing, Zhou, Yuan, Zhou, Lei, Zeng, Lingling, and Deng, Kaixian

Subjects

*LABORATORY rats, *MESENCHYMAL stem cells, *UMBILICAL cord, *WESTERN immunoblotting, *REGENERATIVE medicine

Abstract

Background: Human umbilical cord-derived mesenchymal stem cells (hUC-MSCs) have demonstrated efficacy in repairing uterine scars, although the underlying mechanisms remain unclear. Methods: Uterine injury was surgically induced in a rat model, followed by immediate transplantation of 5 × 10 ^ 5 hUC-MSCs to each side of the uterus. Uterine morphology was evaluated at days 14 and 30 using HE and Masson staining. Immunohistochemistry assessed macrophage polarization, angiogenesis and endometrial receptivity in the endometrium. Additionally, the regulatory effects of hUC-MSCs on macrophage polarization were explored through coculture. qRT-PCR quantified the expression of anti-inflammatory (IL10 and Arg1) and pro-inflammatory (iNOS and TNF-α) factors. Western blotting evaluated CD163 expression. Results: Transplantation of hUC-MSCs promoted the healing of uterine injuries and tissue regeneration while inhibiting tissue fibrosis. Immunohistochemistry at days 14 and 30 post-transplantation demonstrated the polarization of macrophages toward the M2 phenotype in the uterine injury area in the presence of hUC-MSCs. Furthermore, hUC-MSC transplantation improved angiogenesis and endometrial receptivity in the uterine injury rat model, associated with increased IL10 expression. hUC-MSC-induced angiogenesis can be resisted by depleted macrophages. In vitro coculture experiments further demonstrated that hUC-MSCs promoted IL10 expression in macrophages while suppressing TNF-α and iNOS expression. Western blotting showed enhanced CD163 expression in macrophages following hUC-MSC treatment. Conclusions: hUC-MSCs contribute to the healing of uterine injuries by targeting macrophages to promote angiogenesis and the expression of anti-inflammatory factors. [ABSTRACT FROM AUTHOR]

Published

2024

172. Mesenchymal Stromal Cell Therapy Alleviates Ovalbumin-Induced Chronic Airway Remodeling by Suppressing M2 Macrophage Polarization.

Author

Yu, Haiyang, Zhu, Guiyin, Qin, Qiangqiang, Wang, Xueting, Guo, Xuejun, and Gu, Wen

Subjects

*TRANSFORMING growth factors, *OXIDATIVE stress, *EXTRACELLULAR matrix, *STEM cells, *STROMAL cells, *OVALBUMINS

Abstract

Chronic asthma is characterized by airway hyperresponsiveness, inflammation, and remodeling. Previous studies have shown that mesenchymal stromal/stem cells (MSCs) exert anti-inflammatory effects on asthma via regulation of the immune cells. However, the therapeutic mechanism of MSCs, especially the mechanism of airway remodeling in chronic asthma, remains to be elucidated. Here, we aimed to investigate the therapeutic effect of MSCs on airway remodeling in chronic asthma and explored the mechanisms by analyzing the polarization phenotype of macrophages in the lungs. We established a mouse model of chronic asthma induced by ovalbumin (OVA) and evaluated the effect of MSCs on airway remodeling. The data showed that MSCs treatment before the challenge exerted protective effects on OVA-induced chronic asthma, i.e., decreased the inflammatory cell infiltration, Th2 cytokine levels, subepithelial extracellular matrix deposition, and transforming growth factor β (TGF-β)/Smad signaling. Additionally, we found that MSCs treatment markedly suppressed macrophage M2 polarization in lung tissue. At the same time, MSCs treatment inhibited NF-κB p65 nuclear translocation, ER stress, and oxidative stress in the OVA-induced chronic allergic airway remodeling mice model. In conclusion, these results demonstrated that MSCs treatment prevents OVA-induced chronic airway remodeling by suppressing macrophage M2 polarization, which may be associated with the dual inhibition of ER stress and oxidative stress. This discovery may provide a new theoretical basis for the future clinical application of MSCs. [ABSTRACT FROM AUTHOR]

Published

2024

173. Adipose‐derived stem cells transplantation improves survival and alleviates contraction of skin grafts via promoting macrophages M2 polarization.

Author

Cui, Yuying, He, Jiahao, Yu, Zheyuan, Zhou, Sizheng, Cao, Dejun, Jiang, Taoran, Fang, Bin, and Li, Guangshuai

Subjects

*SKIN grafting, *STEM cell transplantation, *VASCULAR endothelial growth factors, *PLASTIC surgery, *PERFUSION imaging

Abstract

Background: Full‐thickness skin grafts are widely used in plastic and reconstructive surgery. The main limitation of skin grafting is the poor textural durability and associated contracture, which often needs further corrective surgery. Excessive inflammation is the main reason for skin graft contractions, which involve overactivation of myofibroblasts. These problems have prompted the development of new therapeutic approaches, including macrophage polarization modulation and stem cell–based therapies. Currently, adipose‐derived stem cells (ASCs) have shown promise in promoting skin grafts survival and regulating macrophage phenotypes. However, the roles of ASCs on macrophages in decreasing skin grafts contraction remain unknown. Materials and Methods: Rat adipose‐derived stem cells (rASCs) were isolated from rat inguinal adipose tissues. Full‐thickness skin graft model was constructed on male rats divided into control group and rASCs treatment group. Skin graft was assessed for concentration, elasticity modulus and stiffness. Rat bone marrow‐derived macrophages (rBMDMs) were isolated from rat femurs, and subsequent RT‐qPCR and coculture assays were carried out to explore the cellular mechanisms. Immunohistochemical and immunofluorescence staining were used to verify mechanisms in vivo. Results: In vivo results showed that after injection of ASCs, improved texture, increased survival and inhibited contraction of skin grafts were seen. Vascularization was also improved as illustrated by laser perfusion image and vascular endothelial growth factor (VEGF) concentration. Histological analysis revealed that ASCs injection significantly reduced expression of pro‐inflammatory cytokines (TNF‐a, IL‐1β) and increased expression of anti‐inflammatory (IL‐10) and pro‐healing cytokines (IGF‐1). At cellular level, after co‐culturing with rASCs, rat bone marrow derived macrophages (rBMDMs) favored M2 polarization even under inflammatory stimulus. Conclusion: ASCs treatment enhanced vascularization via angiogenic cytokines secretion and alleviated inflammatory environment in skin grafts by driving M2 macrophages polarization, which improved survival and decreased skin grafts contraction. Our work showed that ASCs transplantation can be harnessed to enhance therapeutic efficacy of skin grafting in cutaneous defects treatment. [ABSTRACT FROM AUTHOR]

Published

2024

174. Surface immobilized α-1 acid glycoprotein and collagen VI modulate mouse macrophage polarization and reduce the foreign body capsule.

Author

Chen, Alex C., Ciridon, Winston, Creason, Sharon, and Ratner, Buddy D.

Abstract

Macrophages are widely recognized in modulating the foreign body response, and the manner in which they do so largely depends on their activation state, often referred to as their polarization. This preliminary study demonstrates that surface immobilized α-1 acid glycoprotein (AGP), as well as collagen VI (Col6) in conjunction with AGP, can direct macrophages towards the M2 polarization state in vitro and modify the foreign body response in vivo. AGP and Col6 are immobilized onto poly(2-hydroxyethyl methacrylate) (pHEMA) surfaces using carbonyl diimidazole chemistry. Mouse bone marrow derived macrophages are cultured on modified surfaces with or without lipopolysaccharide stimulation. Surface modified pHEMA discs are implanted subcutaneously into mice to observe differences in the foreign body response. After stimulation with lipopolysaccharide, macrophages cultured on AGP or Col6 modified surfaces showed a reduction in TNF-α expression compared to controls. Arg1 expression was also increased in macrophages cultured on modified surfaces. Explanted tissues showed that the foreign body capsule around implants with AGP or AGP and Col6 modification had reduced thickness, while also being more highly vascularized. These data demonstrate that α-1 acid glycoprotein and collagen VI could potentially be used for the surface modification of medical devices to influence macrophage polarization leading to a reduced and modulated foreign body response. [ABSTRACT FROM AUTHOR]

Published

2024

175. Laggera alata Attenuates Inflammatory Response by Regulating Macrophage Polarization in Rheumatoid Arthritis Mice.

Author

Wei, Jiangcun, Tang, Yunli, Qin, Suhong, Ma, Xiumei, Zhong, Wen, Yang, Peng, Deng, Qingmei, and Ma, Jiabao

Abstract

Rheumatoid arthritis (RA) is a type of joint injury, which can induce the activation of inflammatory factors and polarization of tissue macrophages. Total phenolics from Laggera alata (TPLA) has been reported to exhibit anti-inflammatory effect in various diseases. However, its specific function in RA is still unknown. Here, the protective properties of TPLA were studied in collagen-induced arthritis (CIA)-induced RA mice. RA mouse model was established through the CIA induction. Arthritis score, hind paw thickness, and the body weight of the RA mice were evaluated in each group. H&E staining was conducted in hind paw and joint tissues for histopathological staining. The distal femur was analyzed by microCT, and bone loss-related indicators were assessed. The expression of macrophage polarization markers was detected by immunofluorescence staining in RA mice. The serum levels of inflammatory markers were determined by enzyme-linked immunosorbent assay (ELISA). TPLA reduced the CIA-induced arthritis score and hind paw thickness in mice. The body weight of the CIA mouse was significantly increased by TPLA treatment. TPLA improved the CIA-induced histopathological changes in the hind paw and joint tissues from the mice. TPLA inhibited the bone loss and alleviated bone destruction in CIA mouse model. TPLA altered the macrophage phenotype from M1 macrophages into M2 in CIA mice. TPLA suppressed the levels of inflammatory markers both in the serum and joint tissues of the CIA mice. TPLA mitigated RA development by suppressing inflammatory reaction through the inhibition of M1 microphage polarization. [ABSTRACT FROM AUTHOR]

Published

2024

176. The macrophage polarization in Entamoeba histolytica infection modulation by the C fragment of the intermediate subunit of Gal/GalNAc-inhibitable lectin.

Author

Dai Dong, Yuhan Zhang, Wenjie Li, Hongze Zhang, Xunjia Cheng, and Meng Feng

Subjects

TRANSCRIPTION factors, IMMUNOREGULATION, ENTAMOEBA histolytica, IMMUNE system, AMEBIASIS

Abstract

The protozoan parasite Entamoeba histolytica is the causative agent of amebiasis, with clinical outcomes ranging from asymptomatic infections to severe invasive diseases. The innate immune system, particularly macrophages, is of paramount importance in resisting the invasion of host tissues and organs by the trophozoites of E. histolytica. Parasite-derived pathogenic factors, such as lectins, play a pivotal role in the promotion of macrophage polarization phenotypes that have undergone alteration. Nevertheless, the precise mechanisms by which E. histolytica modulates immune polarization remain largely unknown. The current study focused on the immunomodulatory effects of the Igl-C fragment of E. histolytica Gal/GalNAc lectin on macrophage polarization. These results demonstrated that Igl-C could induce the secretion of IL-1b, IL-6, and other cytokines, activating a mixed M1/M2 polarization state. M1 polarization of macrophages occurs in the early stages and gradually transitions to M2 polarization in the later stages, which may contribute to the persistence of the infection. Igl-C induces the macrophage M1 phenotype and causes the release of immune effector molecules, including iNOS and cytokines, by activating the NF-kB p65 and JAK-STAT1 transcription factor signaling pathways. Furthermore, Igl-C supports the macrophage M2 phenotype via JAK-STAT3 and IL-4-STAT6 pathways, which activate arginase expression in later stages, contributing to the tissue regeneration and persistence of the parasite. The involvement of distinct signaling pathways in mediating this response highlights the complex interplay between the parasite and the host immune system. These findings enhance our understanding of the Igl-Cmediated pathogenic mechanisms during E. histolytica infection. [ABSTRACT FROM AUTHOR]

Published

2024

177. Multi-omics strategy reveals that Cordyceps sinensis ameliorates sepsis-associated acute kidney injury via reprogramming of mitochondrial energy metabolism and macrophage polarization.

Author

Lin Chen, Tong Yang, Jiangpeng Wu, Guangqing Cheng, Minghong Zhao, Yanyan Zhou, Yin Kwan Wong, Junzhe Zhang, Qiuyan Guo, Huan Tang, and Jigang Wang

Subjects

CORDYCEPS, ACUTE kidney failure, MITOCHONDRIAL DNA, ENERGY metabolism, MACROPHAGES

Abstract

Cordyceps sinensis (CS) has been widely used as a dietary supplement or traditional medicine for the prevention, treatment, and prognostication of various diseases, because of its pleiotropic pharmacological properties. However, the potential pharmacological action of CS in sepsis-associated acute kidney injury (S-AKI) remains poorly understood. Herein, we investigated the potential pharmacological action of CS against S-AKI and the underlying mechanisms. CS treatment effectively ameliorated renal dysfunction and injury in mice with lipopolysaccharide (LPS)-induced S-AKI, as indicated by the suppression of inflammatory cytokine expression and secretion. Multiomic analyses suggested that the promotion of mitochondrial energy metabolism might be a potential mechanism through which CS protects mice against S-AKI induced by LPS. Subsequent validation assays confirmed that CS treatment substantially restored the activity of mitochondrial complexes, mitochondrial membrane potential, and ATP production. Moreover, CS concomitantly promoted transition of M1 macrophages to M2 macrophages with increased oxidative phosphorylation, thus indicating that macrophage polarization may also be a potential target for S-AKI treatment. Our findings demonstrated that CS significantly ameliorated renal injury and inflammation in S-AKI by regulating mitochondrial energy metabolism and macrophage polarization, thus providing new insights into the clinical use of CS for the prevention and treatment of S-AKI. [ABSTRACT FROM AUTHOR]

Published

2024

178. BBR affects macrophage polarization via inhibition of NF‐κB pathway to protect against T2DM‐associated periodontitis.

Author

Xia, Siying, Jing, Rui, Shi, Mingyan, Yang, Yanan, Feng, Meiting, Deng, Li, and Luo, Lijun

Subjects

INFLAMMATION prevention, NF-kappa B, BONE resorption, MACROPHAGES, ALKALOIDS, RESEARCH funding, INFLAMMATORY mediators, POLYMERASE chain reaction, COMPUTED tomography, GINGIVA, CELLULAR signal transduction, MICE, MESSENGER RNA, GENE expression, EXPERIMENTAL design, TYPE 2 diabetes, ANIMAL experimentation, WESTERN immunoblotting, CYTOKINES, PERIODONTITIS, CHEMICAL inhibitors, DISEASE complications

Abstract

Background and Objective: Periodontitis is intimately associated with the development of various systemic diseases, among which type 2 diabetes mellitus (T2DM) has a bidirectional relationship with the pathogenesis of periodontitis. The objective of the present work was to investigate the role of berberine (BBR) in periodontitis with T2DM and related mechanisms. Methods: The mRNA expression of macrophage polarization‐related factors in the microenvironment of periodontal inflammation was detected using real‐time quantitative PCR (RT‐qPCR). The experimental periodontitis model was constructed in wild‐type (WT) and T2DM (db/db) mice, which were administered BBR after 7 days of modeling. Alveolar bone loss (ABL) in each group of mice was measured utilizing micro‐computed tomography images. RT‐qPCR was performed to analyze the levels of macrophage polarization‐related factors in mouse gingiva. Lastly, using western blotting and RT‐qPCR, the signaling pathway of BBR affecting macrophage polarization in the microenvironment of periodontitis was explored. Results: BBR inhibited M1 polarization and stimulated M2 polarization in the periodontitis microenvironment. BBR decreased ABL in the WT and T2DM periodontitis models. And BBR reduced the production of proinflammatory cytokines and increased anti‐inflammatory cytokine expression in the gingiva of WT and T2DM model mice. Ultimately, BBR mediates its anti‐inflammatory effects on periodontitis through inhibition of the NF‐κB pathway. Conclusions: BBR had a therapeutic effect on T2DM‐associated periodontitis via inhibiting the NF‐κB pathway to affect macrophage polarization, which may have implications for the new pharmacological treatment of T2DM‐associated periodontitis. [ABSTRACT FROM AUTHOR]

Published

2024

179. Exosomes derived from umbilical cord‐derived mesenchymal stem cells exposed to diabetic microenvironment enhance M2 macrophage polarization and protect against diabetic nephropathy.

Author

Su, Wanlu, Yin, Yaqi, Zhao, Jian, Hu, Ruofan, Zhang, Haixia, Hu, Jia, Ren, Rui, Zhang, Yue, Wang, Anning, Lyu, Zhaohui, Mu, Yiming, and Cheng, Yu

Abstract

The role of mesenchymal‐stem‐cell‐derived exosomes (MSCs‐Exo) in the regulation of macrophage polarization has been recognized in several diseases. There is emerging evidence that MSCs‐Exo partially prevent the progression of diabetic nephropathy (DN). This study aimed to investigate whether exosomes secreted by MSCs pre‐treated with a diabetic environment (Exo‐pre) have a more pronounced protective effect against DN by regulating the balance of macrophages. Exo‐pre and Exo‐Con were isolated from the culture medium of UC‐MSCs pre‐treated with a diabetic mimic environment and natural UC‐MSCs, respectively. Exo‐pre and Exo‐Con were injected into the tail veins of db/db mice three times a week for 6 weeks. Serum creatinine and serum urea nitrogen levels, the urinary protein/creatinine ratio, and histological staining were used to determine renal function and morphology. Macrophage phenotypes were analyzed by immunofluorescence, western blotting, and quantitative reverse transcription polymerase chain reaction. In vitro, lipopolysaccharide‐induced M1 macrophages were incubated separately with Exo‐Con and Exo‐pre. We performed microRNA (miRNA) sequencing to identify candidate miRNAs and predict their target genes. An miRNA inhibitor was used to confirm the role of miRNAs in macrophage modulation. Exo‐pre were more potent than Exo‐Con at alleviating DN. Exo‐pre administration significantly reduced the number of M1 macrophages and increased the number of M2 macrophages in the kidney compared to Exo‐Con administration. Parallel outcomes were observed in the co‐culture experiments. Moreover, miR‐486‐5p was distinctly expressed in Exo‐Con and Exo‐pre groups, and it played an important role in macrophage polarization by targeting PIK3R1 through the PI3K/Akt pathway. Reducing miR‐486‐5p levels in Exo‐pre abolished macrophage polarization modulation. Exo‐pre administration exhibited a superior effect on DN by remodeling the macrophage balance by shuttling miR‐486‐5p, which targets PIK3R1. [ABSTRACT FROM AUTHOR]

Published

2024

180. Glycolytic enzyme PGK1 promotes M1 macrophage polarization and induces pyroptosis of acute lung injury via regulation of NLRP3.

Author

Zhu, Guiyin, Yu, Haiyang, Peng, Tian, Yang, Kun, Xu, Xue, and Gu, Wen

Abstract

Acute lung injury (ALI) is characterized by an unregulated inflammatory reaction, often leading to severe morbidity and ultimately death. Excessive inflammation caused by M1 macrophage polarization and pyroptosis has been revealed to have a critical role in ALI. Recent study suggests that glycolytic reprogramming is important in the regulation of macrophage polarization and pyroptosis. However, the particular processes underlying ALI have yet to be identified. In this study, we established a Lipopolysaccharide(LPS)-induced ALI model and demonstrated that blocking glycolysis by using 2-Deoxy-D-glucose(2-DG) significantly downregulated the expression of M1 macrophage markers and pyroptosis-related genes, which was consistent with the in vitro results. Furthermore, our research has revealed that Phosphoglycerate Kinase 1(PGK1), an essential enzyme in the glycolysis pathway, interacts with NOD-, LRR- and pyrin domain-containing protein 3(NLRP3). We discovered that LPS stimulation improves the combination of PGK1 and NLRP3 both in vivo and in vitro. Interestingly, the absence of PGK1 reduces the phosphorylation level of NLRP3. Based on in vitro studies with mice bone marrow-derived macrophages (BMDMs), we further confirmed that siPGK1 plays a protective role by inhibiting macrophage pyroptosis and M1 macrophage polarization. The PGK1 inhibitor NG52 suppresses the occurrence of excessive inflammation in ALI. In general, it is plausible to consider a therapeutic strategy that focuses on modulating the relationship between PGK1 and NLRP3 as a means to mitigate the activation of inflammatory macrophages in ALI. [ABSTRACT FROM AUTHOR]

Published

2024

181. Engineering Efferocytosis‐Mimicking Nanovesicles to Regulate Joint Anti‐Inflammation and Peripheral Immunosuppression for Rheumatoid Arthritis Therapy.

Author

Yuan, Shanshan, Chai, Yingqian, Xu, Jianghua, Wang, Youchao, Jiang, Lihua, Lu, Ning, Jiang, Hongyi, Wang, Jilong, Pan, Xiaoyun, and Deng, Junjie

Subjects

*RHEUMATOID arthritis, *REGULATORY T cells, *T helper cells, *T cells, *JOINT pain, *JOINTS (Anatomy)

Abstract

Rheumatoid arthritis (RA) is an autoimmune disorder characterized by chronic inflammation of the synovial joints and the dysfunction of regulatory T cells (Tregs) in the peripheral blood. Therefore, an optimal treatment strategy should aim to eliminate the inflammatory response in the joints and simultaneously restore the immune tolerance of Tregs in peripheral blood. Accordingly, we developed an efferocytosis‐mimicking nanovesicle that contains three functional factors for immunomodulating of efferocytosis, including "find me" and "eat me" signals for professional (macrophage) or non‐professional phagocytes (T lymphocyte), and "apoptotic metabolite" for metabolite digestion. We showed that efferocytosis‐mimicking nanovesicles targeted the inflamed joints and spleen of mice with collagen‐induced arthritis, further recruiting and selectively binding to macrophages and T lymphocytes to induce M2 macrophage polarization and Treg differentiation and T helper cell 17 (Th17) recession. Under systemic administration, the efferocytosis‐mimicking nanovesicles effectively maintained the pro‐inflammatory M1/anti‐inflammatory M2 macrophage balance in joints and the Treg/Th17 imbalance in peripheral blood to prevent RA progression. This study demonstrates the potential of efferocytosis‐mimicking nanovesicles for RA immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2024

182. Artificial Vasa‐Vasorum Serves as an On‐Site Regenerative Promoter of Cell‐Free Vascular Grafting.

Author

Ha, Hyun‐su, Baek, Sewoom, Lee, Kyubae, Cho, Sungwoo, Cho, Min Jeong, Chung, Seyong, Choi, Hyeongyun, Lee, Chan Hee, Kim, Min Seok, Kim, Si Yeong, Kim, Dae‐Hyun, Kang, Sang‐Wook, and Sung, Hak‐Joon

Subjects

*VASCULAR grafts, *EXTERIOR walls, *MUSCLE cells, *SMOOTH muscle, *ARTERIES

Abstract

The control paradigm of small vessel pathophysiology has changed to focus on the vascular out‐wall rather than the lumen‐intimal factors. As an emerging controller of the external wall, the microvasculature ("vasa vasorum") provides interactional routes between the in‐and out‐sides of the vascular wall. Despite numerous approaches to developing small‐diameter vascular grafts, engineering artificial vasa vasorum (AVV) has not been projected as a multi‐functional solution to address long‐standing issues such as thrombotic and immune controls for wall regeneration. Here, the AVV is engineered using a microchannel network hydrogel after a multi‐study validation of implantation functions and then used to wrap the external wall of the cell‐free vessel post‐decellularization while preserving its mechanical properties. Upon inter‐positional and bypass grafting to rabbit arteries, the AVV graft facilitates the recruitment of vascular cells into the cell‐free wall by promoting invasion of angiogenic and vasculogenic cells through the microchannel‐mediated M2 polarization of macrophages. This function results in the efficient restoration of smooth muscle cells, and the revitalized vascular elasticity helps to maintain long‐term patency. The AVV, therefore, serves as an effective catalyst for vascular wall regeneration, offering a solution to clinically successful small‐diameter vascular grafting. [ABSTRACT FROM AUTHOR]

Published

2024

183. Progress in reeducating tumor-associated macrophages in tumor microenvironment.

Author

Zhao, Yiming, Ni, Qianyang, Zhang, Weijian, and Yu, Suyang

Subjects

TUMOR microenvironment, MACROPHAGES, THERAPEUTICS, CLINICAL medicine, CANCER invasiveness

Abstract

Malignant tumor, one of the most threatening diseases to human health, has been comprehensively treated with surgery, radiotherapy, chemotherapy and targeted therapy, but the prognosis has not always been ideal. In the past decade, immunotherapy has shown increased efficacy in tumor treatment; however, for immunotherapy to achieve its fullest potential, obstacles are to be conquered, among which tumor microenvironment (TME) has been widely investigated. In remodeling the tumor immune microenvironment to inhibit tumor progression, macrophages, as the most abundant innate immune population, play an irreplaceable role in the immune response. Therefore, how to remodel TME and alter the recruitment and polarization status of tumor-associated macrophages (TAM) has been of wide interest. In this context, nanoparticles, photodynamic therapy and other therapeutic approaches capable of affecting macrophage polarization have emerged. In this paper, we categorize and organize the existing means and methods for reprogramming TAM to provide ideas for clinical application of novel tumor-related therapies. [ABSTRACT FROM AUTHOR]

Published

2024

184. 巨噬细胞极化在牙周炎发病及治疗中的作用.

Author

葛叡扬, 倪 璨, 杨 琨, and 闫福华

Subjects

*INFLAMMATION, *INFLAMMATORY mediators, *IMMUNE response, *PERIODONTITIS, *MACROPHAGES, *GUIDED tissue regeneration, *BIOMATERIALS, *PERIODONTIUM, *BONE growth

Abstract

BACKGROUND: Host immune response triggered by plaque biofilm is an initiator of periodontitis progression and destruction. Macrophages are an important component of the innate immune response, which play an important role in inflammation occurrence and development. OBJECTIVE: To review the relationship between macrophage polarization and periodontitis and the related progress in the treatment of periodontitis by regulating macrophage polarization. METHODS: PubMed and CNKI databases were searched for relevant literature published from 1990 to 2023, with “macrophage polarization, M1/M2 macrophage, periodontitis, periodontitis treatment, macrophage polarization and periodontitis, osteoimmunology, ferroptosis, macrophage polarization and ferroptosis, periodontitis and ferroptosis” as the English and Chinese search terms. After the initial screening, 96 articles were selected for review. RESULTS AND CONCLUSION: The switch between different phenotypes of macrophages is closely related to the tissue destruction caused by periodontitis, and various cytokines and inflammatory mediators secreted from macrophages are involved in the destruction and repair of periodontal tissue. Therefore,regulation of macrophage polarization and cytokine secretion in inflammatory state helps to alleviate periodontitis inflammation and improve the periodontal microenvironment, thereby reducing tissue destruction or promoting periodontal tissue regeneration. Many studies have been conducted to develop drugs or biomaterials to modulate macrophage function for the purpose of immunomodulatory treatment of periodontitis. However, macrophages act throughout the development of periodontitis and play an important role in the process of anti-infection, bone destruction and bone repair, and polarization is a complex and dynamic process influenced by many factors. Therefore, further exploration on possible mechanisms is still needed to clarify the interaction between materials or drugs and macrophages. [ABSTRACT FROM AUTHOR]

Published

2024

185. Nanomaterial-Based Repurposing of Macrophage Metabolism and Its Applications.

Author

Meng, Tingting, He, Danfeng, Han, Zhuolei, Shi, Rong, Wang, Yuhan, Ren, Bibo, Zhang, Cheng, Mao, Zhengwei, Luo, Gaoxing, and Den, Jun

Subjects

*MACROPHAGES, *IMMUNE response, *THERAPEUTICS, *METABOLIC reprogramming, *RESEARCH personnel

Abstract

Highlights: A large-scale metabolic adaptation in M1-polarized macrophages compared with M2 macrophages, along with multiple altered metabolite parameters that can serve as potential targets, have been discussed. Nanomaterial-based repurposing of macrophage metabolism and its applications are systematically summarized and illustrated using representative examples. Potential challenges, additional information about future research objectives, and priorities of nanomaterial-based macrophage immunotherapy are highlighted. Macrophage immunotherapy represents an emerging therapeutic approach aimed at modulating the immune response to alleviate disease symptoms. Nanomaterials (NMs) have been engineered to monitor macrophage metabolism, enabling the evaluation of disease progression and the replication of intricate physiological signal patterns. They achieve this either directly or by delivering regulatory signals, thereby mapping phenotype to effector functions through metabolic repurposing to customize macrophage fate for therapy. However, a comprehensive summary regarding NM-mediated macrophage visualization and coordinated metabolic rewiring to maintain phenotypic equilibrium is currently lacking. This review aims to address this gap by outlining recent advancements in NM-based metabolic immunotherapy. We initially explore the relationship between metabolism, polarization, and disease, before delving into recent NM innovations that visualize macrophage activity to elucidate disease onset and fine-tune its fate through metabolic remodeling for macrophage-centered immunotherapy. Finally, we discuss the prospects and challenges of NM-mediated metabolic immunotherapy, aiming to accelerate clinical translation. We anticipate that this review will serve as a valuable reference for researchers seeking to leverage novel metabolic intervention-matched immunomodulators in macrophages or other fields of immune engineering. [ABSTRACT FROM AUTHOR]

Published

2024

186. Cellular In Vitro Responses Induced by Human Mesenchymal Stem/Stromal Cell-Derived Extracellular Vesicles Obtained from Suspension Culture.

Author

Souza, Ingrid L. M., Suzukawa, Andreia A., Josino, Raphaella, Marcon, Bruna H., Robert, Anny W., Shigunov, Patrícia, Correa, Alejandro, and Stimamiglio, Marco A.

Subjects

*EXTRACELLULAR vesicles, *EXTRACELLULAR matrix, *CELL migration, *STROMAL cells, *IMMUNE response, *CELL suspensions, *TISSUE remodeling

Abstract

Mesenchymal stem/stromal cells (MSCs) and their extracellular vesicles (MSC-EVs) have been described to have important roles in tissue regeneration, including tissue repair, control of inflammation, enhancing angiogenesis, and regulating extracellular matrix remodeling. MSC-EVs have many advantages for use in regeneration therapies such as facility for dosage, histocompatibility, and low immunogenicity, thus possessing a lower possibility of rejection. In this work, we address the potential activity of MSC-EVs isolated from adipose-derived MSCs (ADMSC-EVs) cultured on cross-linked dextran microcarriers, applied to test the scalability and reproducibility of EV production. Isolated ADMSC-EVs were added into cultured human dermal fibroblasts (NHDF-1), keratinocytes (HaCat), endothelial cells (HUVEC), and THP-1 cell-derived macrophages to evaluate cellular responses (i.e., cell proliferation, cell migration, angiogenesis induction, and macrophage phenotype-switching). ADMSC viability and phenotype were assessed during cell culture and isolated ADMSC-EVs were monitored by nanotracking particle analysis, electron microscopy, and immunophenotyping. We observed an enhancement of HaCat proliferation; NHDF-1 and HaCat migration; endothelial tube formation on HUVEC; and the expression of inflammatory cytokines in THP-1-derived macrophages. The increased expression of TGF-β and IL-1β was observed in M1 macrophages treated with higher doses of ADMSC-EVs. Hence, EVs from microcarrier-cultivated ADMSCs are shown to modulate cell behavior, being able to induce skin tissue related cells to migrate and proliferate as well as stimulate angiogenesis and cause balance between pro- and anti-inflammatory responses in macrophages. Based on these findings, we suggest that the isolation of EVs from ADMSC suspension cultures makes it possible to induce in vitro cellular responses of interest and obtain sufficient particle numbers for the development of in vivo concept tests for tissue regeneration studies. [ABSTRACT FROM AUTHOR]

Published

2024

187. Scutellarin alleviates renal ischemia–reperfusion injury by inhibiting the MAPK pathway and pro‐inflammatory macrophage polarization.

Author

Deng, Ge, Zheng, Bingxuan, Dou, Meng, Gao, Yang, Zhang, Xingzhe, Niu, Zejiaxin, Wei, Tian, Han, Feng, Ding, Chenguang, and Tian, Puxun

Abstract

Renal ischemia–reperfusion injury (IRI) is an integral process in renal transplantation, which results in compromised graft survival. Macrophages play an important role in both the early inflammatory period and late fibrotic period in response to IRI. In this study, we investigated whether scutellarin (SCU) could protect against renal IRI by regulating macrophage polarization. Mice were given SCU (5–50 mg/kg) by gavage 1 h earlier, followed by a unilateral renal IRI. Renal function and pathological injury were assessed 24 h after reperfusion. The results showed that administration of 50 mg/kg SCU significantly improved renal function and renal pathology in IRI mice. In addition, SCU alleviated IRI‐induced apoptosis. Meanwhile, it reduced macrophage infiltration and inhibited pro‐inflammatory macrophage polarization. Moreover, in RAW 264.7 cells and primary bone marrow‐derived macrophages (BMDMs) exposed to SCU, we found that 150 μM SCU inhibited these cells to polarize to an inflammatory phenotype induced by lipopolysaccharide (LPS) and interferon‐γ (IFN‐γ). However, SCU has no influence on anti‐inflammatory macrophage polarization in vivo and in vitro induced by in interleukin‐4 (IL‐4). Finally, we explored the effect of SCU on the activation of the mitogen‐activated protein kinase (MAPK) pathway both in vivo and in vitro. We found that SCU suppressed the activation of the MAPK pathway, including the extracellular signal‐regulated kinase (ERK), Jun N‐terminal kinase (JNK), and p38. Our results demonstrated that SCU protects the kidney against IRI by inhibiting macrophage infiltration and polarization toward pro‐inflammatory phenotype via the MAPK pathway, suggesting that SCU may be therapeutically important in treatment of IRI. [ABSTRACT FROM AUTHOR]

Published

2024

188. The regulatory effect of TiO2 nanotubes loaded with graphene oxide on macrophage polarization in an inflammatory environment.

Author

Cao, Xu, Luo, Bin, Mu, Yanting, Wang, Caiyun, Lu, Ran, Yao, Yao, and Chen, Su

Subjects

RAMAN spectroscopy, MACROPHAGES, RESEARCH funding, CELL proliferation, TITANIUM, ELECTRON microscopy, CELL adhesion molecules, ENZYME-linked immunosorbent assay, FLUORESCENT antibody technique, MICE, BIOMEDICAL materials, GENE expression, RNA, REACTIVE oxygen species, OXIDES, ANIMAL experimentation, LIPOPOLYSACCHARIDES, INFLAMMATION, NANOPARTICLES, SEQUENCE analysis

Abstract

Background: Excessive inflammation is a major cause of implant failure. The surface morphology, hydrophilicity, and loading of biomaterials are major properties modulating anti-inflammatory macrophage activation. This paper investigates the regulatory effects of modifying the surface of Titanium dioxide nanotubes (TNTs) with graphene oxide (GO) on the polarization of mouse monocyte macrophages (RAW264.7). Methods: TNT was produced by the anodic oxidation of titanium. GO was subsequently electrodeposited on the TNT to obtain a TNT–GO composite. The samples were characterised through scanning electron microscopy (SEM), Raman spectroscopy, and X-ray diffraction. RAW264.7 cells were separately seeded onto the surface of three groups of samples: pure Ti, TNT, and TNT–GO. Under the condition of lipopolysaccharide stimulation, the influence of the sample surfaces on the gene expression profiles was investigated through RNA sequence analysis. In addition, cell spreading was observed through SEM, cell adhesion and proliferation were analysed using the CCK8 assay, and the expression of inflammation-related factors was investigated by ELISA and cellular immunofluorescence staining. The production of reactive oxygen species (ROS) in the RAW264.7 cells on the surface of the three groups was detected via immunofluorescence staining. Results: The CCK8 results indicated that the adhesion and proliferation of the RAW264.7 cells were reduced on the TNT and TNT–GO surfaces. ELISA results revealed significant differences in the pro-inflammatory factors tumour necrosis factor-α and interleukin-6 secretion among the three groups at 24 h (p < 0.05). The secretion of pro-inflammatory factors significantly reduced and the expression of anti-inflammatory factor IL-10 increased on the TNT and TNT–GO surfaces. The RNA sequencing, ELISA, and cell immunofluorescence staining test results suggested that the inflammatory response of M1 polarization was reduced and the M2 polarization of macrophages was induced on the TNT–GO surface, which may be attributed to the reduction in ROS production. Conclusions: Under lipopolysaccharide stimulation, the inflammatory response of the RAW264.7 cells was reduced and the M2 polarization of macrophages was promoted on the TNT–GO surface, which may be caused by the reduced ROS production. Consequently, the designed TNT–GO material is promising for implants owing to its excellent inflammation regulation ability. [ABSTRACT FROM AUTHOR]

Published

2024

189. Endothelial cells-derived exosomes-based hydrogel improved tendinous repair via anti-inflammatory and tissue regeneration-promoting properties.

Author

Dou, Yichen, Zhai, Hong, Li, Haiqiu, Xing, Hanlin, Zhu, Cheng, and Xuan, Zhaopeng

Subjects

*ACHILLES tendon rupture, *ENDOTHELIAL cells, *TENDON injuries, *ACHILLES tendon, *HYDROGELS, *TISSUE scaffolds, *BONE regeneration, TENDON injury healing

Abstract

Tendon injuries are common orthopedic ailments with a challenging healing trajectory, especially in cases like the Achilles tendon afflictions. The healing trajectory of tendon injuries is often suboptimal, leading to scar formation and functional impairment due to the inherent low metabolic activity and vascularization of tendon tissue. As pressing is needed for effective interventions, efforts are made to explore biomaterials to augment tendon healing. However, tissue engineering approaches face hurdles in optimizing tissue scaffolds and nanomedical strategies. To navigate these challenges, an injectable hydrogel amalgamated with human umbilical vein endothelial cells-derived exosomes (HUVECs-Exos) was prepared and named H-Exos-gel in this study, aiming to enhance tendon repair. In our research involving a model of Achilles tendon injuries in 60 rats, we investigated the efficacy of H-Exos-gel through histological assessments performed at 2 and 4 weeks and behavioral assessments conducted at the 4-week mark revealed its ability to enhance the Achilles tendon's mechanical strength, regulate inflammation and facilitate tendon regeneration and functional recovery. Mechanically, the H-Exos-gel modulated the cellular behaviors of macrophages and tendon-derived stem cells (TDSCs) by inhibiting inflammation-related pathways and promoting proliferation-related pathways. Our findings delineate that the H-Exos-gel epitomizes a viable bioactive medium for tendon healing, heralding a promising avenue for the clinical amelioration of tendon injuries. [ABSTRACT FROM AUTHOR]

Published

2024

190. miR-455/GREM1 axis promotes colorectal cancer progression and liver metastasis by affecting PI3K/AKT pathway and inducing M2 macrophage polarization.

Author

Dai, Shipeng, Xu, Fan, Xu, Xiaozhang, Huang, Tian, Wang, Yiming, Wang, Hongyu, Xie, Yucheng, Yue, Lei, Zhao, Wenhu, Xia, Yongxiang, Gu, Jian, and Qian, Xiaofeng

Subjects

*COLORECTAL liver metastasis, *PI3K/AKT pathway, *INTESTINAL cancer, *LIVER metastasis, *TISSUE differentiation

Abstract

Background: Colorectal cancer is among the most common malignant tumors affecting the gastrointestinal tract. Liver metastases, a complication present in approximately 50% of colorectal cancer patients, are a considerable concern. Recently, studies have revealed the crucial role of miR-455 in tumor pathogenesis. However, the effect of miR-455 on the progression of liver metastases in colorectal cancer remains controversial. As an antagonist of bone morphogenetic protein(BMP), Gremlin 1 (GREM1) may impact organogenesis, body patterning, and tissue differentiation. Nevertheless, the role of miR-455 in regulating GREM1 in colorectal cancer liver metastases and how miR-455/GREM1 axis influences tumour immune microenvironment is unclear. Methods: Bioinformatics analysis shows that miR-455/GREM1 axis plays crucial role in liver metastasis of intestinal cancer and predicts its possible mechanism. To investigate the impact of miR-455/GREM1 axis on the proliferation, invasion, and migration of colorectal cancer cells, colony formation assay, wound healing and transwell assay were examined in vitro. The Dual-Luciferase reporter gene assay and RNA pull-down assay confirmed a possible regulatory effect between miR-455 and GREM1. In vivo, colorectal cancer liver metastasis(CRLM) model mice was established to inquiry the effect of miR-455/GREM1 axis on tumor growth and macrophage polarization. The marker of macrophage polarization was tested using immunofluorescence(IF) and quantitative real-time polymerase chain reaction(qRT-PCR). By enzyme-linked immunosorbent assay (ELISA), cytokines were detected in culture medium supernatants. Results: We found that miR-455 and BMP6 expression was increased and GREM1 expression was decreased in liver metastase compared with primary tumor. miR-455/GREM1 axis promotes colorectal cancer cells proliferation, migration, invasion via affected PI3K/AKT pathway. Moreover, downregulating GREM1 augmented BMP6 expression in MC38 cell lines, inducing M2 polarization of macrophages, and promoting liver metastasis growth in CRLM model mice. Conclusion: These data suggest that miR-455/GREM1 axis promotes colorectal cancer progression and liver metastasis by affecting PI3K/AKT pathway and inducing M2 macrophage polarization. These results offer valuable insights and direction for future research and treatment of CRLM. [ABSTRACT FROM AUTHOR]

Published

2024

191. Targeting Macrophage Polarization for Reinstating Homeostasis following Tissue Damage.

Author

Du, Qiran, Dickinson, Anna, Nakuleswaran, Pruthvi, Maghami, Susan, Alagoda, Savindu, Hook, Andrew L., and Ghaemmaghami, Amir M.

Subjects

*MACROPHAGES, *WOUND healing, *CLINICAL medicine, *TISSUE remodeling, *TISSUES, *FOREIGN bodies, *HOMEOSTASIS, *BONE regeneration

Abstract

Tissue regeneration and remodeling involve many complex stages. Macrophages are critical in maintaining micro-environmental homeostasis by regulating inflammation and orchestrating wound healing. They display high plasticity in response to various stimuli, showing a spectrum of functional phenotypes that vary from M1 (pro-inflammatory) to M2 (anti-inflammatory) macrophages. While transient inflammation is an essential trigger for tissue healing following an injury, sustained inflammation (e.g., in foreign body response to implants, diabetes or inflammatory diseases) can hinder tissue healing and cause tissue damage. Modulating macrophage polarization has emerged as an effective strategy for enhancing immune-mediated tissue regeneration and promoting better integration of implantable materials in the host. This article provides an overview of macrophages' functional properties followed by discussing different strategies for modulating macrophage polarization. Advances in the use of synthetic and natural biomaterials to fabricate immune-modulatory materials are highlighted. This reveals that the development and clinical application of more effective immunomodulatory systems targeting macrophage polarization under pathological conditions will be driven by a detailed understanding of the factors that regulate macrophage polarization and biological function in order to optimize existing methods and generate novel strategies to control cell phenotype. [ABSTRACT FROM AUTHOR]

Published

2024

192. Direct Current Electrical Stimulation Shifts THP-1-Derived Macrophage Polarization towards Pro-Regenerative M2 Phenotype.

Author

Bianconi, Santiago, Leppik, Liudmila, Oppermann, Elsie, Marzi, Ingo, and Henrich, Dirk

Subjects

*REGENERATION (Biology), *PHENOTYPES, *MACROPHAGES, *GENE expression, *NUCLEAR proteins, *TRANSCRANIAL direct current stimulation, *ELECTRIC stimulation, *INTERLEUKIN receptors

Abstract

A macrophage shift from the M1 to the M2 phenotype is relevant for promoting tissue repair and regeneration. In a previous in vivo study, we found that direct current (DC) electrical stimulation (EStim) increased the proportion of M2 macrophages in healing tissues and directed the balance of the injury response away from healing/scarring towards regeneration. These observations led us to hypothesize that DC EStim regulates macrophage polarization towards an M2 phenotype. THP-1-derived M0, M1 (IFN-γ and LPS), and M2 (IL-4 and IL-13) macrophages were exposed (or not: control group) to 100 mV/mm of DC EStim, 1 h/day for three days. Macrophage polarization was assessed through gene and surface marker expressions and cytokine secretion profiles. Following DC EStim treatment, M0 cells exhibited an upregulation of M2 marker genes IL10, CD163, and PPARG. In M1 cells, DC EStim upregulated the gene expressions of M2 markers IL10, TGM2, and CD206 and downregulated M1 marker gene CD86. EStim treatment also reduced the surface expression of CD86 and secretion of pro-inflammatory cytokines IL-1β and IL-6. Our results suggest that DC EStim differentially exerts pro-M2 effects depending on the macrophage phenotype: it upregulates typical M2 genes in M0 and M1 cells while inhibiting M1 marker CD86 at the nuclear and protein levels and the secretion of pro-inflammatory interleukins in M1 cells. Conversely, M2 cells appear to be less responsive to the EStim treatment employed in this study. [ABSTRACT FROM AUTHOR]

Published

2024

193. Sirt1 inhibits macrophage polarization and inflammation in gouty arthritis by inhibiting the MAPK/NF-κB/AP-1 pathway and activating the Nrf2/HO-1 pathway.

Author

Zhao, Xu, Li, Menglan, Lu, Yiwei, Wang, Mi, Xiao, Jiawei, Xie, Qingqing, He, Xinyi, and Shuai, Shiquan

Subjects

*SIRTUINS, *ANKLE joint, *JOINT diseases, *ARTHRITIS, *MACROPHAGE inflammatory proteins, *INFLAMMATION

Abstract

Objective and design: To elucidate Sirt1's role in gouty arthritis inflammation and its potential mechanisms. Material: Constructed murine models of gouty arthritis and conducted THP-1 cell experiments. Treatment: 1 mg of MSU crystals injected into mice ankle joints for a 72-h intervention. After a 3-h pre-treatment with Sirt1-specific inhibitor (EX527) and agonist (SRT2104), inflammation was induced for 21 h using lipopolysaccharide (LPS) plus MSU crystals. Methods: We assessed gouty arthritis severity through joint inflammation index, swelling, and hematoxylin and eosin (H&E) staining, and measured CD68 mononuclear macrophages and Sirt1 expression in synovial tissue via immunohistochemistry. ELISA, NO assay, RT-qPCR, Flow cytometry, and Western blot were utilized to examine macrophage inflammatory factors, polarization, reactive oxygen species(ROS), MAPK/NF-κB/AP-1 and Nrf2/HO-1 pathways proteins. Results: Significant joint swelling, synovial tissue edema, and inflammatory cell infiltration were observed. CD68 mononuclear macrophages and Sirt1 expression were elevated in synovium. Sirt1 activation decreased inflammatory factors, M1 polarization, and ROS generation. Sirt1 activation reduced p38/JNK phosphorylation, thereby inhibiting downstream NF-κB p65/AP-1 and enhancing Nrf2/HO-1, thus suppressing inflammation. Conclusions: Sirt1 alleviates M1 macrophage polarization and inflammation in gouty arthritis by inhibiting the MAPK/NF-κB/AP-1 pathway and activating the Nrf2/HO-1 pathway. Thus, activating Sirt1 may provide a new therapeutic target for gouty arthritis. [ABSTRACT FROM AUTHOR]

Published

2024

194. Regulatory impact of statins on macrophage polarization: mechanistic and therapeutic implications.

Author

Sadeghi, Mahvash, Khayati, Shaho, Dehnavi, Sajad, Almahmeed, Wael, Sukhorukovi, Vasily N, and Sahebkar, Amirhossein

Subjects

*STATINS (Cardiovascular agents), *MACROPHAGES, *REDUCTASE inhibitors, *THERAPEUTICS, *CARDIOVASCULAR diseases, *PHAGOCYTOSIS, *CHOLESTERYL ester transfer protein

Abstract

Statins, also known as HMG-CoA reductase inhibitors, are widely prescribed drugs for the prevention and treatment of cardiovascular diseases. In addition to their lipid-lowering effects, these compounds have been found to possess immune-modulating properties. Macrophages, which are crucial phagocytic cells in the body, can be divided into two main subsets: M1 (proinflammatory) and M2 (anti-inflammatory). While there is evidence suggesting that statins exert an anti-inflammatory action on macrophages and promote their polarization towards the M2 subset, recent studies have identified the proinflammatory impact of statins on macrophages, leading to polarization towards the M1 subset. For example, statins have been shown to inhibit NF-κB activation to promote anti-inflammatory responses. On the other hand, statins can induce NFκB/AP-1 activation and increase IL-1β secretion in macrophages to promote pro-inflammatory responses. This review aims to provide a comprehensive overview of both in vivo and in vitro studies that have investigated the effects of statins on macrophage polarization and inflammatory responses in various diseases. Furthermore, this review seeks to evaluate the underlying mechanisms involved in these effects. By summarizing the existing evidence, this review contributes to our understanding of the complex interactions between statins and macrophages in different disease contexts. [ABSTRACT FROM AUTHOR]

Published

2024

195. Targeting MS4A4A: A novel pathway to improve immunotherapy responses in glioblastoma.

Author

Shao, Guangcai, Cui, Xiangguo, Wang, Yiliang, Luo, Shuyan, Li, Chuanyu, Jiang, Yu, Cai, Dasheng, Li, Nu, and Li, Xiang

Abstract

Introduction: Glioblastoma (GBM) remains a challenging brain tumor to treat, with limited response to PD‐1 immunotherapy due to tumor‐associated macrophages (TAMs), specifically the M2 phenotype. This study explores the potential of MS4A4A (membrane spanning four domains, subfamily A, member 4A) inhibition in driving M2 macrophage polarization toward the M1 phenotype via the ferroptosis pathway to enhance the effectiveness of immunotherapy in GBM. Methods: Single‐cell RNA sequencing and spatial transcriptomic analyses were employed to characterize M2 macrophages and MS4A4A expression in GBM. In vitro studies utilizing TAM cultures, flow cytometry, and western blot validations were conducted to assess the impact of MS4A4A on the tumor immune microenvironment and M2 macrophage polarization. In vivo models, including subcutaneous and orthotopic transplantation in mice, were utilized to evaluate the effects of MS4A4A knockout and combined immune checkpoint blockade (ICB) therapy on tumor growth and response to PD‐1 immunotherapy. Results: Distinct subsets of GBM‐associated macrophages were identified, with spatial distribution in tumor tissue elucidated. In vivo experiments demonstrated that inhibiting MS4A4A and combining ICB therapy effectively inhibited tumor growth, reshaped the tumor immune microenvironment by reducing M2 TAM infiltration and enhancing CD8+ T‐cell infiltration, ultimately leading to complete tumor eradication. Conclusion: MS4A4A inhibition shows promise in converting M2 macrophages to M1 phenotype via ferroptosis, decreasing M2‐TAM infiltration, and enhancing GBM response to PD‐1 immunotherapy. These findings offer a novel approach to developing more effective immunotherapeutic strategies for GBM. [ABSTRACT FROM AUTHOR]

Published

2024

196. TREM1 facilitates the development of gastric cancer through regulating neutrophil extracellular traps-mediated macrophage polarization.

Author

Yu, Cheng, Zhou, Guoqiang, Shi, Zhiliang, Yu, Liang, and Zhou, Xiaojun

Abstract

Triggering receptor expressed on myeloid cell 1 (TREM1) elevation is associated with the unfavorable prognosis of gastric cancer (GC) patients. This work uncovered the effects and mechanism of TREM1 in GC. IHC staining examined TREM1 expression in GC tissues. TREM1 -knockout and TREM1 knock-in mice were generated prior to the construction of N-methyl-N'-nitro-N-nitrosoguanidine (MNNG)-induced GC mice model. H&E staining detected the pathological alternations of gastric tissues. IHC staining tested Ki67 expression. Wright-Giemsa staining performed neutrophil counting and flow cytometry analysis measured neutrophil infiltration. ELISA analyzed serum and tissue myeloperoxidase (MPO) levels and serum MPO-DNA levels. Immunofluorescence, Western blotting and related kits detected NETs formation. Immunofluorescence and IHC staining evaluated macrophage polarization. In MNNG-treated GES-1 cells and phorbal myristate acetate (PMA)-treated neutrophils, TREM1 expression was also examined. CCK-8 method and Western blotting assayed cell proliferation. Western blotting and immunofluorescence detected NETs formation. Flow cytometry analysis detected the changes of macrophage typing. TREM1 was overexpressed in tumor tissues, MNNG-treated GES-1 cells and PMA-treated neutrophils. TREM1 deficiency hindered tumor growth, reduced neutrophil infiltration, NETs formation and stimulated M1 macrophage polarization in MNNG-induced GC models. Neutrophil extracellular traps (NETs) degrader DNase-1 countervailed the impacts of TREM1 on MNNG-induced GC models in vivo. Collectively, TREM1 knockdown obstructed NETs-mediated M2 macrophage polarization to hamper GC progression. [ABSTRACT FROM AUTHOR]

Published

2024

197. Sequential dual-locking strategy using photoactivated Pt(IV)-based metallo-nano prodrug for enhanced chemotherapy and photodynamic efficacy by triggering ferroptosis and macrophage polarization.

Author

Li, Jun, Zhang, Qiang, Yang, Hao, Lu, Wenli, Fu, Yulong, Xiong, Yingcai, Wang, Xuan, Lu, Tianming, Xin, Yanlin, Xie, Zejuan, Chen, Weichao, Wang, Guoqiang, Guo, Yuanyuan, and Qi, Ruogu

Subjects

CANCER chemotherapy, MACROPHAGES, PRODRUGS, PHOTODYNAMIC therapy, TUMOR treatment, ANTINEOPLASTIC agents

Abstract

Selective activation of Pt(IV) prodrugs within tumors has emerged as a promising strategy in tumor treatment. Although progress has been made with photo- and ultrasound-activated Pt(IV) prodrugs, concerns remain over the non-specific activation of photosensitizers (PS) and the potential for phototoxicity and chemical toxicity. In this study, a sequential dual-locked Pt(IV) nano-prodrug that can be activated by both the acidic tumor microenvironment and light was developed. The Pt(IV) prodrug was prepared by conjugating PS-locked Pt(IV) to a polymeric core, which was then chelated with metallo iron to lock its photoactivity and form a metallo-nano prodrug. Under acidic tumor microenvironment conditions, the metallo-nano prodrug undergoes dissociation of iron, triggering a reduction process in oxaliplatin under light irradiation, resulting in the activation of both chemotherapy and photodynamic therapy (PDT). Additionally, the prodrug could induce metallo-triggered ferroptosis and polarization of tumor-associated macrophages (TAM), thereby enhancing tumor inhibition. The dual-lock strategy employed in a nanoparticle delivery system represents an expansion in the application of platinum-based anticancer drugs, making it a promising new direction in cancer treatment. A novel sequential dual-locking using photoactivated Pt(IV)-based metallo-nanoprodrug is reported. The dual-locking Pt(IV) drug was sequentially excited by acid condition and red light. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

198. Mild phototherapy mediated by IR780-Gd-OPN nanomicelles suppresses atherosclerotic plaque progression through the activation of the HSP27-regulated NF-κB pathway.

Author

He, Wenming, Tu, Shuangshuang, Han, Jinru, Cui, Haijing, Lai, Liangxue, Ye, Yonglong, Dai, Ting, Yuan, Yannan, Ji, Lili, Luo, Jiayong, Ren, Wenzhi, and Wu, Aiguo

Subjects

ATHEROSCLEROTIC plaque, PHOTOTHERAPY, FOAM cells, HEAT shock proteins, CARDIOVASCULAR disease related mortality, LIPID metabolism

Abstract

Reducing plaque lipid content and enhancing plaque stability without causing extensive apoptosis of foam cells are ideal requirements for developing a safe and effective treatment of atherosclerosis. In this study, we synthesized IR780-Gd-OPN nanomicelles by conjugating osteopontin (OPN) and loading a gadolinium-macrocyclic ligand (Gd-DOTA) onto near-infrared dye IR780-polyethylene glycol polymer. The nanomicelles were employed for mild phototherapy of atherosclerotic plaques and dual-mode imaging with near-infrared fluorescence and magnetic resonance. In vitro results reveal that the mild phototherapy mediated by IR780-Gd-OPN nanomicelles not only activates heat shock protein (HSP) 27 to protect foam cells against apoptosis but also inhibits the nuclear factor kappa-B (NF-κB) pathway to regulate lipid metabolism and macrophage polarization, thereby diminishing the inflammatory response. In vivo results further validate that mild phototherapy effectively reduces plaque lipid content and size while simultaneously enhancing plaque stability by regulating the ratio of M1 and M2-type macrophages. In summary, this study presents a promising approach for developing a safe and highly efficient method for the precise therapeutic visualization of atherosclerosis. The rupture of unstable atherosclerotic plaques is a major cause of high mortality rates in cardiovascular diseases. Therefore, the ideal outcome of atherosclerosis treatment is to reduce plaque size while enhancing plaque stability. To address this challenge, we designed IR780-Gd-OPN nanomicelles for mild phototherapy of atherosclerosis. This treatment can effectively reduce plaque size while significantly improving plaque stability by increasing collagen fiber content and elevating the ratio of M2/M1 macrophages, which is mainly attributed to the inhibition of the NF-κB signaling pathway by mild phototherapy-activated HSP27. In summary, our proposed mild phototherapy strategy provides a promising approach for safe and effective treatment of atherosclerosis. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

199. Fibroblast growth factor signaling in macrophage polarization: impact on health and diseases.

Author

Luyao Shen, Yongsheng Li, and Huakan Zhao

Subjects

FIBROBLAST growth factors, GROWTH factors, MACROPHAGES, FIBROBLAST growth factor receptors, EMBRYOLOGY

Abstract

Fibroblast growth factors (FGFs) are a versatile family of peptide growth factors that are involved in various biological functions, including cell growth and differentiation, embryonic development, angiogenesis, and metabolism. Abnormal FGF/FGF receptor (FGFR) signaling has been implicated in the pathogenesis of multiple diseases such as cancer, metabolic diseases, and inflammatory diseases. It is worth noting that macrophage polarization, which involves distinct functional phenotypes, plays a crucial role in tissue repair, homeostasis maintenance, and immune responses. Recent evidence suggests that FGF/FGFR signaling closely participates in the polarization of macrophages, indicating that they could be potential targets for therapeutic manipulation of diseases associated with dysfunctional macrophages. In this article, we provide an overview of the structure, function, and downstream regulatory pathways of FGFs, as well as crosstalk between FGF signaling and macrophage polarization. Additionally, we summarize the potential application of harnessing FGF signaling to modulate macrophage polarization. [ABSTRACT FROM AUTHOR]

Published

2024

200. M2-type macrophage membrane-mediated delivery of Carvedilol nanocomplex for acute liver failure treatment and remodeling inflammatory microenvironment.

Author

Shang, Mingge, Zhang, Yaohui, Qian, Junjie, Wang, Wenchao, Yu, Xizhi, Huang, Jiacheng, Zhou, Lin, and Zheng, Shusen

Subjects

LIVER failure, CARVEDILOL, TREATMENT failure, MACROPHAGES, RETICULO-endothelial system, SUMATRIPTAN, BIOMIMETIC materials

Abstract

Interactions of hepatic macrophages with local inflammatory microenvironment is the key factor promoting the development of acute liver failure (ALF). Hence, reprogramming pro-inflammatory M1 into anti-inflammatory M2 phenotype may offer a promising strategy for treating ALF by targeting inflammation. Our group found Carvedilol possessed potential anti-inflammatory property previously, which had been scarcely reported in ALF. We present a synergy strategy to induce macrophages into the phenotype M2-type anti-inflammatory macrophages with interleukin-4 (IL-4) and IL-10 at first. Then Carvedilol is loaded on the macrophage membrane-camouflaged biomimetic nano-platform (termed as M2M@CNP) to evade reticuloendothelial system (RES) and afford Carvedilol delivery to the inflammatory environment with overproduced reactive oxygen species (ROS), further prolonging its circulation and accumulation. Sustainably released Carvedilol produced anti-inflammatory, antioxidant and anti-apoptosis effects, combining local M2-type cell membranes (M2-CM) inhibited pro-inflammatory cytokines and ROS levels, which in turn promoted and amplified M1 to M2 phenotype polarization efficiency. This study offers new insights into the rational design of biomimetic nanosystems for safe and effective ALF therapy to accelerate the clinical translation. [ABSTRACT FROM AUTHOR]

Published

2024