Extracellular vesicle miR-32 derived from macrophage promotes arterial calcification in mice with type 2 diabetes via inhibiting VSMC autophagy

Cao, Jingsong; Chen, Cong; Chen, Qian; Gao, Yan; Zhao, Zhen-Wang; Yuan, Qing; Li, Anqi; Yang, Shiqi; He, Yuan; Zu, Xuyu; Liu, Jianghua

doi:10.1186/s12967-022-03502-8

Cited by 17 publications

(16 citation statements)

References 53 publications

(48 reference statements)

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“…T2D mice were generated as previously reported. 19 , 20 Mice were group housed (2–5 mice per cage) at a controlled temperature (22 ± 2°C) under a 12‐h light/dark cycle with free access to food and water. The mice adapted to their new environment for 7 days before the behavioral tests.…”

Section: Methodsmentioning

confidence: 99%

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Pravastatin promotes type 2 diabetes vascular calcification through activating intestinal Bacteroides fragilis to induce macrophage M1 polarization

Chen,

Liang,

et al. 2023

Journal of Diabetes

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BackgroundPravastatin is an oral lipid‐lowering drug, commonly used by patients with diabetes that is positively correlated with the occurrence of vascular calcification (VC), but the mechanism is unclear.MethodsIn this study, 16S rRNA sequencing and qRT‐PCR wereused to detect the differential gut bacteria. Metabolomics and ELISA were used to analyze the differential metabolites. qRT‐PCR and western blotting (WB) were used to detect genes expression. Flow cytometry was used to analyze macrophage phenotype. Immunohistochemistry was used to analyze aortic calcification.ResultsWe found that gut Bacteroides fragilis (BF) increased significantly in patients who took pravastatin or type 2 diabetes (T2D) mice treated with pravastatin. In vitro experiments showed that pravastatin had little effect on BF but significantly promoted BF proliferation in vivo. Further analysis showed that ArsR was an important gene for pravastatin to regulate the activation of BF, and overexpression of ArsR significantly promoted the secretion of 3,4,5‐trimethoxycinnamic acid (TMCA). Importantly, pravastatin significantly promoted BF secretion of TMCA and significantly increased TMCA secretion in T2D patients or T2D mice. TMCA had little effect on vascular smooth muscle cell calcification but significantly promoted macrophage M1 polarization, which we had demonstrated that M1 macrophages promoted T2D VC. In vivo studies found that pravastatin significantly upregulated TMCA levels in the feces and serum of T2D mice transplanted with BF and promoted the macrophage M1 polarization in bone marrow and the osteoblastic differentiation of aortic cells. Similar results were obtained in T2D mice after intravenous infusion of TMCA.ConclusionsPromoting intestinal BF to secrete TMCA, which leads to macrophage M1 polarization, is an important mechanism by which pravastatin promotes calcification, and the result will be used for the optimization of clinical medication strategies of pravastatin supplying a theoretical basis and experimental basis.

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Section: Methodsmentioning

confidence: 99%

“… 17 We previously confirmed that peripheral macrophages in T2D patients are prone to polarize into the M1 phenotype and secrete inflammatory factors and extracellular vesicles to promote VC. 18 , 19 , 20 Are macrophages also the key target cells of BF to promote T2D VC?…”

Section: Introductionmentioning

confidence: 99%

Pravastatin promotes type 2 diabetes vascular calcification through activating intestinal Bacteroides fragilis to induce macrophage M1 polarization

Chen,

Liang,

et al. 2023

Journal of Diabetes

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“…Ca 2+ uptake by cells via exosomes or Ca 2+ channels further contributed to an increase in Nox5 activity (90). Under hyperglycaemic conditions, EV miR-32 in macrophages was upregulated and delivered to VSMCs, promoting osteogenic differentiation and inhibiting autophagy in VSMCs via the miR-32/Mef2d/cGMP-PKG signaling pathway (91). Lipoprotein(a) stimulation led to an increase in the annexin level in the EV cargo of primary human smooth muscle cells (SMCs) and valvular interstitial cells (VICs), and these EVs readily aggregated in the collagen matrix and induced its mineralization, leading to the formation of microcalcifications that coalesced into macrocalcifications (92).…”

Section: Exosomes and Vascular Calcificationmentioning

confidence: 99%

Emerging role of exosomes in vascular diseases

Ren

Zhang

2023

Front. Cardiovasc. Med.

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Exosomes are biological small spherical lipid bilayer vesicles secreted by most cells in the body. Their contents include nucleic acids, proteins, and lipids. Exosomes can transfer material molecules between cells and consequently have a variety of biological functions, participating in disease development while exhibiting potential value as biomarkers and therapeutics. Growing evidence suggests that exosomes are vital mediators of vascular remodeling. Endothelial cells (ECs), vascular smooth muscle cells (VSMCs), inflammatory cells, and adventitial fibroblasts (AFs) can communicate through exosomes; such communication is associated with inflammatory responses, cell migration and proliferation, and cell metabolism, leading to changes in vascular function and structure. Essential hypertension (EH), atherosclerosis (AS), and pulmonary arterial hypertension (PAH) are the most common vascular diseases and are associated with significant vascular remodeling. This paper reviews the latest research progress on the involvement of exosomes in vascular remodeling through intercellular information exchange and provides new ideas for understanding related diseases.

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“…Severe vascular calcification in diabetic has also been confirmed to be related to VSMCs ( 117 , 118 ). In addition, AGEs ( 119 , 120 ), apoptosis ( 121 , 122 ), oxidative stress ( 123 , 124 ) and a variety of noncoding RNAs ( 125 , 126 ) regulate AS under diabetic state. Recent studies about the effect of high glucose on VSMCs was listed in Table 3 .…”

Section: Diabetes and Vsmcsmentioning

confidence: 99%

Role of advanced glycation end products on vascular smooth muscle cells under diabetic atherosclerosis

Lin

Yin²,

Yang³

et al. 2022

Front. Endocrinol.

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Atherosclerosis (AS) is a chronic inflammatory disease and leading cause of cardiovascular diseases. The progression of AS is a multi-step process leading to high morbidity and mortality. Hyperglycemia, dyslipidemia, advanced glycation end products (AGEs), inflammation and insulin resistance which strictly involved in diabetes are closely related to the pathogenesis of AS. A growing number of studies have linked AGEs to AS. As one of the risk factors of cardiac metabolic diseases, dysfunction of VSMCs plays an important role in AS pathogenesis. AGEs are increased in diabetes, participate in the occurrence and progression of AS through multiple molecular mechanisms of vascular cell injury. As the main functional cells of vascular, vascular smooth muscle cells (VSMCs) play different roles in each stage of atherosclerotic lesions. The interaction between AGEs and receptor for AGEs (RAGE) accelerates AS by affecting the proliferation and migration of VSMCs. In addition, increasing researches have reported that AGEs promote osteogenic transformation and macrophage-like transformation of VSMCs, and affect the progression of AS through other aspects such as autophagy and cell cycle. In this review, we summarize the effect of AGEs on VSMCs in atherosclerotic plaque development and progression. We also discuss the AGEs that link AS and diabetes mellitus, including oxidative stress, inflammation, RAGE ligands, small noncoding RNAs.

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Extracellular vesicle miR-32 derived from macrophage promotes arterial calcification in mice with type 2 diabetes via inhibiting VSMC autophagy

Cited by 17 publications

References 53 publications

Pravastatin promotes type 2 diabetes vascular calcification through activating intestinal Bacteroides fragilis to induce macrophage M1 polarization

Pravastatin promotes type 2 diabetes vascular calcification through activating intestinal Bacteroides fragilis to induce macrophage M1 polarization

Emerging role of exosomes in vascular diseases

Role of advanced glycation end products on vascular smooth muscle cells under diabetic atherosclerosis

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