Iron corroded granules inhibiting vascular smooth muscle cell proliferation

• Published in: Materials today bio Vol. 16; p. 100420
• Main Authors: Qiu, Dongxu, Deng, Yalan, Wen, Yanbin, Yin, Jun, Feng, Jie, Huang, Jiabing, Song, Mingyu, Zhang, Gui, Chen, Changqing, Xia, Jian
• Format: Journal Article
• Language: English
• Published: Elsevier 01.12.2022
• Subjects: Corroded granules; Full Length; In-stent restenosis; Iron-based stent; Neointimal hyperplasia; Proliferation; Vascular smooth muscle cell
• ISSN: 2590-0064; 2590-0064
• DOI: 10.1016/j.mtbio.2022.100420

In-stent restenosis after interventional therapy remains a severe clinical complication. Current evidence indicates that neointimal hyperplasia induced by vascular smooth muscle cell (VSMC) proliferation is a major cause of restenosis. Thus, inhibiting VSMC proliferation is critical for preventing in-stent restenosis. The incidence of restenosis was reduced in nitrided iron-based stents (hereafter referred to as iron stents). We hypothesized that the corroded granules produced by the iron stent would prevent in-stent restenosis by inhibiting VSMC proliferation. To verify this hypothesis, we introduced a dynamic circulation device to analyze the components of corroded granules. To investigate the effects of corroded granules on VSMC proliferation, we implanted the corroded iron stent into the artery of the atherosclerotic artery stenosis model. Moreover, we explored the mechanism underlying the inhibition of VSMC proliferation by iron corroded granules. The results indicated that iron stent produced the corroded granules after implantation, and the main component of the corrosion granules was iron oxide. Remarkably, the corroded granules reduced the neointimal hyperplasia in an atherosclerotic artery stenosis model, and iron corroded granules decreased the neointimal hyperplasia by inhibiting VSMC proliferation. In addition, we revealed that corroded granules reduced VSMC proliferation by activating autophagy through the AMPK/mTOR signaling pathway. Importantly, safety of iron corroded granules was evaluated and proved to be satisfactory hemocompatibility in rabbit model. Overall, the role of corroded granules in restenosis prevention was described for the first time. This finding highlighted the implication of corroded granules produced by iron stent in inhibiting VSMC proliferation, pointing to a new direction to prevent in-stent restenosis. Illustration of the study. Corroded granules were produced by the iron-based stent after implantation. The corroded granules released from iron-based stent will accumulate around the vascular smooth muscle cell (VSMC) of implanted artery. The iron corroded granules inhibit VSMC proliferation by activating autophagy through the AMPK/mTOR pathway, which prevented the intimal hyperplasia and in-stent restenosis after iron-based stent implantation. Image 1 • Corroded granules were produced from the iron stent, and the main component of the corrosion granules was iron oxide. • The corroded granules prevent in-stent restenosis by inhibiting VSMC proliferation. • The corroded granules inhibited VSMC proliferation by activating autophagy through the AMPK/mTOR signaling pathway. • Iron corroded granules proved to be satisfactory hemocompatibility in rabbit model.