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固定有血管内皮生长因子(VEGF)的聚多巴胺(PDA)涂层可抑制大鼠主动脉植入锌丝后新生内膜的形成。

Polydopamine (PDA) coatings with endothelial vascular growth factor (VEGF) immobilization inhibiting neointimal formation post zinc (zn) wire implantation in rat aortas.

作者信息

Fu Jiayin, Zhu Qiongjun, Chen Zhezhe, Zhao Jing, Wu Shaofei, Zhao Meng, Xu Shihui, Lai Dongwu, Fu Guosheng, Zhang Wenbin

机构信息

Key Laboratory of Cardiovascular Intervention and Regenerative Medicine of Zhejiang Province, Department of Cardiology, Sir Run Run Shaw Hospital, Zhejiang University, Hangzhou, 310016, China.

出版信息

Biomater Res. 2023 Sep 4;27(1):84. doi: 10.1186/s40824-023-00423-5.

Abstract

BACKGROUND

Bioresorbable stents are designed to provide temporary mechanical support to the coronary arteries and then slowly degrade in vivo to avoid chronic inflammation. Zinc (Zn) is a promising material for bioresorbable stents; However, it can cause inflammation and neointimal formation after being implanted into blood vessels.

METHODS

To improve biocompatibility of Zn, we first coated it with polydopamine (PDA), followed by immobilization of endothelial vascular growth factor (VEGF) onto the PDA coatings. Adhesion, proliferation, and phenotype maintenance of endothelial cells (ECs) on the coated Zn were evaluated in vitro. Then, a wire aortic implantation model in rats mimicking endovascular stent implantation in humans was used to assess vascular responses to the coated Zn wires in vivo. Thrombosis in aortas post Zn wire implantation, degradation of Zn wires in vivo, neointimal formation surrounding Zn wires, and macrophage infiltration and extracellular matrix (ECM) remodeling in the neointimas were examined.

RESULTS

In vitro data showed that the PDA-coated Zn encouraged EC adhesion, spreading, proliferation, and phenotype maintenance on its surfaces. VEGF functionalization on PDA coatings further enhanced the biocompatibility of Zn to ECs. Implantation of PDA-coated Zn wires into rat aortas didn't cause thrombosis and showed a faster blood flow than pure Zn or the Zn wires coated with VEGF alone. In addition, the PDA coating didn't affect the degradation of Zn wires in vivo. Besides, the PDA-coated Zn wires reduced neointimal formation, increased EC coverage, decreased macrophage infiltration, and declined aggrecan accumulation in ECM. VEGF immobilization onto PDA coatings didn't cause thrombosis and affect Zn degradation in vivo as well, and further increased the endothelization percentage as compared to PDA coating alone, thus resulting in thinner neointimas.

CONCLUSION

These results indicate that PDA coatings with VEGF immobilization would be a promising approach to functionalize Zn surfaces to increase biocompatibility, reduce inflammation, and inhibit neointimal formation after Zn implantation in vivo.

摘要

背景

生物可吸收支架旨在为冠状动脉提供临时机械支撑,然后在体内缓慢降解以避免慢性炎症。锌(Zn)是一种有前景的生物可吸收支架材料;然而,它植入血管后会引发炎症和新生内膜形成。

方法

为提高锌的生物相容性,我们首先用聚多巴胺(PDA)对其进行涂层,随后将内皮血管生长因子(VEGF)固定在PDA涂层上。体外评估了内皮细胞(ECs)在涂覆锌表面的黏附、增殖和表型维持情况。然后,使用大鼠的丝线主动脉植入模型模拟人体血管内支架植入,以评估体内血管对涂覆锌丝的反应。检查了锌丝植入后主动脉中的血栓形成、锌丝在体内的降解、锌丝周围的新生内膜形成以及新生内膜中的巨噬细胞浸润和细胞外基质(ECM)重塑。

结果

体外数据表明,PDA涂层的锌促进了EC在其表面的黏附、铺展、增殖和表型维持。PDA涂层上的VEGF功能化进一步增强了锌对EC的生物相容性。将PDA涂层的锌丝植入大鼠主动脉未引起血栓形成,且与纯锌或仅涂有VEGF的锌丝相比,血流更快。此外,PDA涂层不影响锌丝在体内的降解。此外,PDA涂层的锌丝减少了新生内膜形成,增加了EC覆盖,减少了巨噬细胞浸润,并降低了ECM中聚集蛋白聚糖的积累。VEGF固定在PDA涂层上也未引起血栓形成,也不影响体内锌的降解,并且与单独的PDA涂层相比,进一步提高了内皮化百分比,从而使新生内膜更薄。

结论

这些结果表明,固定有VEGF的PDA涂层将是一种有前景的方法,可使锌表面功能化,以提高生物相容性、减少炎症并抑制锌在体内植入后的新生内膜形成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8abd/10478185/97a2481ef540/40824_2023_423_Fig1_HTML.jpg

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