Effect of Chemically Modified Carbon-Coated Iron Nanoparticles on the Structure of Human Atherosclerotic Plaques Ex Vivo and on Adipose Tissue in Chronic Experiment In Vivo.
Shamil AkhmedovSergey AfanasyevNatalia BeshchasnaMarina TrusovaIvan StepanovMariya RebenkovaEkaterina PoletykinaYuri VecherskiySergey I TverdokhlebovEvgeniy N BolbasovSascha BalakinJoerg OpitzAnatoly YermakovBoris N KozlovPublished in: International journal of molecular sciences (2022)
The high mortality rate caused by atherosclerosis makes it necessary to constantly search for new and better treatments. In previous reports, chemically modified carbon-coated iron nanoparticles (Fe@C NPs) have been demonstrated a high biocompatibility and promising anti-plaque properties. To further investigate these effects, the interaction of these nanoparticles with the adipose tissue of Wistar rats (in vivo) and human atherosclerotic plaques (ex vivo) was studied. For the in vivo study, cobalt-chromium (CoCr) alloy tubes, which are used for coronary stent manufacturing, were prepared with a coating of polylactic acid (PLA) which contained either modified or non-modified Fe@C NPs in a 5% by weight concentration. The tubes were implanted into an area of subcutaneous fat in Wistar rats, where changes in the histological structure and functional properties of the surrounding tissue were observed in the case of coatings modified with Fe@C NPs. For the ex vivo study, freshly explanted human atherosclerotic plaques were treated in the physiological solution with doses of modified Fe@C NPs, with mass equal to 5% or 25% relative to the plaques. This treatment resulted in the release of cholesterol-like compounds from the surface of the plaques into the solution, thus proving a pronounced destructive effect on the plaque structure. Chemically modified Fe@C NPs, when used as an anti-atherosclerosis agent, were able to activate the activity of macrophages, which could lead to the destruction of atherosclerotic plaques structures. These findings could prove the fabrication of next-generation vascular stents with built-in anti-atherosclerotic agents.
Keyphrases
- adipose tissue
- endothelial cells
- coronary artery disease
- cardiovascular disease
- metal organic framework
- heart failure
- high fat diet
- fatty acid
- oxide nanoparticles
- gold nanoparticles
- coronary artery
- mass spectrometry
- physical activity
- risk factors
- metabolic syndrome
- visible light
- atrial fibrillation
- tissue engineering