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血管移植物内皮化及长期管腔通畅的挑战与策略

Challenges and strategies for endothelialization and long-term lumen patency of vascular grafts.

作者信息

Zhuang Yu, Zhang Chenglong, Cheng Mengjia, Huang Jinyang, Liu Qingcheng, Yuan Guangyin, Lin Kaili, Yu Hongbo

机构信息

Department of Oral and Cranio-maxillofacial Surgery, Shanghai Ninth People's Hospital, College of Stomatology, Shanghai Jiao Tong University School of Medicine, Shanghai, 200011, China.

National Clinical Research Center for Oral Diseases, Shanghai, 200011, China.

出版信息

Bioact Mater. 2020 Dec 5;6(6):1791-1809. doi: 10.1016/j.bioactmat.2020.11.028. eCollection 2021 Jun.

Abstract

Vascular diseases are the most prevalent cause of ischemic necrosis of tissue and organ, which even result in dysfunction and death. Vascular regeneration or artificial vascular graft, as the conventional treatment modality, has received keen attentions. However, small-diameter (diameter < 4 mm) vascular grafts have a high risk of thrombosis and intimal hyperplasia (IH), which makes long-term lumen patency challengeable. Endothelial cells (ECs) form the inner endothelium layer, and are crucial for anti-coagulation and thrombogenesis. Thus, promoting endothelialization in vascular graft remodeling takes top priority, which requires recruitment of endothelia progenitor cells (EPCs), migration, adhesion, proliferation and activation of EPCs and ECs. Chemotaxis aimed at ligands on EPC surface can be utilized for EPC homing, while nanofibrous structure, biocompatible surface and cell-capturing molecules on graft surface can be applied for cell adhesion. Moreover, cell orientation can be regulated by topography of scaffold, and cell bioactivity can be modulated by growth factors and therapeutic genes. Additionally, surface modification can also reduce thrombogenesis, and some drug release can inhibit IH. Considering the influence of macrophages on ECs and smooth muscle cells (SMCs), scaffolds loaded with drugs that can promote M2 polarization are alternative strategies. In conclusion, the advanced strategies for enhanced long-term lumen patency of vascular grafts are summarized in this review. Strategies for recruitment of EPCs, adhesion, proliferation and activation of EPCs and ECs, anti-thrombogenesis, anti-IH, and immunomodulation are discussed. Ideal vascular grafts with appropriate surface modification, loading and fabrication strategies are required in further studies.

摘要

血管疾病是组织和器官缺血性坏死最常见的原因,甚至会导致功能障碍和死亡。血管再生或人工血管移植作为传统的治疗方式,受到了广泛关注。然而,小口径(直径<4mm)血管移植物存在血栓形成和内膜增生(IH)的高风险,这使得长期管腔通畅性面临挑战。内皮细胞(ECs)形成血管内层内皮,对于抗凝和血栓形成至关重要。因此,在血管移植物重塑中促进内皮化是首要任务,这需要募集内皮祖细胞(EPCs),以及EPCs和ECs的迁移、黏附、增殖和激活。针对EPC表面配体的趋化作用可用于EPC归巢,而移植物表面的纳米纤维结构、生物相容性表面和细胞捕获分子可用于细胞黏附。此外,支架的拓扑结构可调节细胞取向,生长因子和治疗基因可调节细胞生物活性。另外,表面修饰还可减少血栓形成,一些药物释放可抑制内膜增生。考虑到巨噬细胞对ECs和平滑肌细胞(SMCs)的影响,负载可促进M2极化药物的支架是替代策略。总之,本综述总结了提高血管移植物长期管腔通畅性的先进策略。讨论了募集EPCs、EPCs和ECs的黏附、增殖和激活、抗血栓形成、抗内膜增生和免疫调节的策略。进一步的研究需要具有适当表面修饰、负载和制造策略的理想血管移植物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/60eb/7721596/47d719b3a81e/fx1.jpg

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