M2 Macrophages as a Potential Target for Antiatherosclerosis Treatment

Bi, Ying; Chen, Jixiang; Hu, Feng; Liu, Jing; Li, Man; Zhao, Lei

doi:10.1155/2019/6724903

Cited by 111 publications

(100 citation statements)

References 174 publications

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“…In past decades, research on antiatherosclerosis drugs mainly focused on lipid-reducing, anti-inflammatory, and antioxidative strategies, endothelial protection and foam cell inhibition. Few studies have focused on macrophage polarization, which is also a promising target for atherosclerosis therapy [37,38]. Generally, the anti-inflammatory macrophage phenotype is considered atheroprotective, although CD163 + macrophages promote atherosclerosis [3,4].…”

Section: Discussionmentioning

confidence: 99%

Araloside C attenuates atherosclerosis by modulating macrophage polarization via Sirt1-mediated autophagy

Luo

Gao

et al. 2020

Aging

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Atherosclerosis-related cardiovascular disease is still the predominant cause of death worldwide. Araloside C (AsC), a natural saponin, exerts extensive anti-inflammatory properties. In this study, we explored the protective effects and mechanism of AsC on macrophage polarization in atherosclerosis in vivo and in vitro. Using a high-fat diet (HFD)-fed ApoE-/-mouse model and RAW264.7 macrophages exposed to ox-LDL, AsC was evaluated for its effects on polarization and autophagy. AsC significantly reduced the plaque area in atherosclerotic mice and lipid accumulation in ox-LDL-treated macrophages, promoted M2 phenotype macrophage polarization, increased the number of autophagosomes and modulated the expression of autophagy-related proteins. Moreover, the autophagy inhibitor 3-methyladenine and BECN1 siRNA obviously abolished the antiatherosclerotic and M2 macrophage polarization effects of AsC. Mechanistically, AsC targeted Sirt1and increased its expression, and this increase in expression was associated with increased autophagy and M2 phenotype polarization. In contrast, the effects of AsC were markedly blocked by EX527 and Sirt1 siRNA. Altogether, AsC attenuates foam cell formation and lessens atherosclerosis by modulating macrophage polarization via Sirt1-mediated autophagy.

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Section: Discussionmentioning

confidence: 99%

Araloside C attenuates atherosclerosis by modulating macrophage polarization via Sirt1-mediated autophagy

Luo

Gao

et al. 2020

Aging

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“…Both of these populations are plastic cells because they can switch from the M1 to M2 state and vice versa upon specific signals; the changes from M1 to M2 has been defined as "macrophage polarization" [28]. Furthermore, M1 macrophages exhibit elevated lipid accumulation, which contribute to the acceleration of atherosclerosis; whereas in contrast, M2 macrophages are located far from the lipid core of the plaque, contain smaller lipid droplets, and are involved in phagocytosis [29][30][31]. In particular, Chinetti et al showed that in the adventitia, M2 macrophages are twofold to threefold more abundant than M1 macrophages [29].…”

Section: Discussionmentioning

confidence: 99%

Beneficial Effects of Melatonin on Apolipoprotein-E Knockout Mice by Morphological and 18F-FDG PET/CT Assessments

Nardo

Rezzani

Facchetti

et al. 2020

IJMS

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Atherosclerosis represents one of the main risk factors for the development of cardiovascular diseases. Their etiologies have been studied in recent years in order to better define therapeutic targets for intervention and to identify diagnostic methods. Two different subtypes of macrophages, M1 and M2, have been described in physiological conditions. They can also be found in the atherosclerotic process, where they both have opposite roles in disease progression. Perivascular brown adipose tissue is also involved in inflammation and endothelial damage. In this work, we provide insights into the protective role of melatonin in the atherosclerotic process by morphological and 18F-FDG-PET/CT analyses. In particular, we examined the effects of melatonin on pathways that are linked to atherosclerosis development. We showed that melatonin, by suppressing M1 activity, reduced inflammation and directed macrophage polarization toward the M2 macrophage subtype. Moreover, melatonin preserved the activity of perivascular brown adipose tissue. In addition, 18F-FDG uptake is very high in mice treated with melatonin, confirming that other factors may alter 18F-FDG distribution. In conclusion, we showed that melatonin affects inflammatory pathways that have been linked to atherosclerosis, assessed the relationships of the 18F-FDG PET/CT parameters with macrophage markers and the production of their cytokines, which that have been defined by morphological evaluations.

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“…The opposite strategy of forcing macrophages into M2 phenotypes may be applied for the treatment of atherosclerosis [ 28 ]. LAIR1 (CD305) is an inhibitory collagen receptor expressed by certain blood cells, e.g., by monocytes.…”

Section: Macrophages As Perfect Cells For Reprogrammingmentioning

confidence: 99%

Macrophage Modification Strategies for Efficient Cell Therapy

Poltavets

Vishnyakova

Elchaninov

et al. 2020

Cells

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Macrophages, important cells of innate immunity, are known for their phagocytic activity, capability for antigen presentation, and flexible phenotypes. Macrophages are found in all tissues and therefore represent an attractive therapeutic target for the treatment of diseases of various etiology. Genetic programming of macrophages is an important issue of modern molecular and cellular medicine. The controllable activation of macrophages towards desirable phenotypes in vivo and in vitro will provide effective treatments for a number of inflammatory and proliferative diseases. This review is focused on the methods for specific alteration of gene expression in macrophages, including the controllable promotion of the desired M1 (pro-inflammatory) or M2 (anti-inflammatory) phenotypes in certain pathologies or model systems. Here we review the strategies of target selection, the methods of vector delivery, and the gene editing approaches used for modification of macrophages.

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M2 Macrophages as a Potential Target for Antiatherosclerosis Treatment

Cited by 111 publications

References 174 publications

Araloside C attenuates atherosclerosis by modulating macrophage polarization via Sirt1-mediated autophagy

Araloside C attenuates atherosclerosis by modulating macrophage polarization via Sirt1-mediated autophagy

Beneficial Effects of Melatonin on Apolipoprotein-E Knockout Mice by Morphological and 18F-FDG PET/CT Assessments

Macrophage Modification Strategies for Efficient Cell Therapy

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