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高镁与西罗莫司对兔血管细胞的影响——一项体外概念验证研究

High Magnesium and Sirolimus on Rabbit Vascular Cells-An In Vitro Proof of Concept.

作者信息

Fedele Giorgia, Castiglioni Sara, Maier Jeanette A, Locatelli Laura

机构信息

Department of Biomedical and Clinical Sciences L. Sacco, Università di Milano, Via GB Grassi 74, 20157 Milano, Italy.

Interdisciplinary Centre for Nanostructured Materials and Interfaces (CIMaINa), Università di Milano, 20133 Milan, Italy.

出版信息

Materials (Basel). 2021 Apr 14;14(8):1970. doi: 10.3390/ma14081970.

Abstract

Drug-eluting bioresorbable scaffolds represent the last frontier in the field of angioplasty and stenting to treat coronary artery disease, one of the leading causes of morbidity and mortality worldwide. In particular, sirolimus-eluting magnesium-based scaffolds were recently introduced in clinical practice. Magnesium alloys are biocompatible and dissolve in body fluids, thus determining high concentrations of magnesium in the local microenvironment. Since magnesium regulates cell growth, we asked whether high levels of magnesium might interfere with the antiproliferative action of sirolimus. We performed in vitro experiments on rabbit coronary artery endothelial and smooth muscle cells (rCAEC and rSMC, respectively). The cells were treated with sirolimus in the presence of different concentrations of extracellular magnesium. Sirolimus inhibits rCAEC proliferation only in physiological concentrations of magnesium, while high concentrations prevent this effect. On the contrary, high extracellular magnesium does not rescue rSMC growth arrest by sirolimus and accentuates the inhibitory effect of the drug on cell migration. Importantly, sirolimus and magnesium do not impair rSMC response to nitric oxide. If translated into a clinical setting, these results suggest that, in the presence of sirolimus, local increases of magnesium concentration maintain normal endothelial proliferative capacity and function without affecting rSMC growth inhibition and response to vasodilators.

摘要

药物洗脱生物可吸收支架代表了血管成形术和支架置入领域治疗冠状动脉疾病的最新前沿,冠状动脉疾病是全球发病和死亡的主要原因之一。特别是,西罗莫司洗脱镁基支架最近已引入临床实践。镁合金具有生物相容性,可溶于体液,从而在局部微环境中产生高浓度的镁。由于镁调节细胞生长,我们不禁要问,高浓度的镁是否会干扰西罗莫司的抗增殖作用。我们分别对兔冠状动脉内皮细胞和平滑肌细胞(分别为rCAEC和rSMC)进行了体外实验。在不同浓度的细胞外镁存在的情况下,用西罗莫司处理细胞。西罗莫司仅在生理浓度的镁存在时抑制rCAEC增殖,而高浓度则阻止这种作用。相反,高细胞外镁不能挽救西罗莫司引起的rSMC生长停滞,反而会增强药物对细胞迁移的抑制作用。重要的是,西罗莫司和镁不会损害rSMC对一氧化氮的反应。如果转化为临床情况,这些结果表明,在存在西罗莫司的情况下,局部镁浓度升高可维持正常的内皮增殖能力和功能,而不会影响rSMC的生长抑制和对血管扩张剂的反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/855f/8070902/e5e76e39b40e/materials-14-01970-g001.jpg

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