Gelatin microgel-coated balloon catheter with enhanced delivery of everolimus for long-term vascular patency

被引:2
|
作者
Lee, Simin [1 ]
Yoon, Chang-Hwan [2 ]
Oh, Dong Hwan [1 ]
Anh, Tu Quang [1 ]
Jeon, Ki-Hyun [2 ]
Chae, In -Ho [2 ]
Park, Ki Dong [1 ]
机构
[1] Ajou Univ, Dept Mol Sci & Technol, Suwon, South Korea
[2] Seoul Natl Univ, Bundang Hosp, Dept Internal Med, Div Cardiol, Seongnam, South Korea
基金
新加坡国家研究基金会;
关键词
In-stent restenosis; Drug-coated balloon; Everolimus; Gelatin; Microgel; Sustained drug delivery; Pharmacokinetics; Long-term patency; DRUG-ELUTING STENTS; CORONARY-ARTERY-DISEASE; NEOINTIMAL HYPERPLASIA; DE-NOVO; SIROLIMUS; RAPAMYCIN; INHIBITION; RELEASE; METAANALYSIS; MECHANISMS;
D O I
10.1016/j.actbio.2023.11.001
中图分类号
R318 [生物医学工程];
学科分类号
0831 ;
摘要
In-stent restenosis (ISR) after percutaneous coronary intervention is a major reason for limited long-term patency due to complex neointimal proliferation caused by vascular injury. Drug-coated balloon (DCB) has been developed to treat various cardiovascular diseases including ISR by providing anti-proliferative drugs into blood vessel tissues. However, a significant proportion of the drug is lost during balloon track-ing, resulting in ineffective drug delivery to the target region. In this study, we report an everolimus-coated balloon (ECB) using everolimus-loaded gelatin-hydroxyphenyl propionic acid microgel (GM) with enhanced everolimus delivery to vascular walls for long-term patency. GM with high drug loading (> 97%) was simply prepared by homogenizing enzyme-mediated crosslinked hydrogels. The optimal condi-tion to prepare GM-coated ECB (GM-ECB) was established by changing homogenization time and ethanol solvent concentration (30 similar to 80%). In vitro sustained everolimus release for 30 d, and cellular efficacy using smooth muscle cells and vascular endothelial cells were evaluated. Additionally, an in vivo drug transfer levels of GM-ECB using rabbit femoral arteries were assessed with reduced drug loss and effi-cient drug delivery capability. Finally, using ISR-induced porcine models, effective in vivo vascular patency 4 weeks after treatment of ECBs was also confirmed. Thus, this study strongly demonstrates that GM can be used as a potential drug delivery platform for DCB application. Statement of significance We report an ECB using everolimus-loaded GM prepared by homogenization of enzymatic cross-linked hydrogel. GM showed efficient drug loading (> 97 %) and controllable size. GM-ECB exhibited potential to deliver everolimus in a sustained manner to target area with drug efficacy and viability against SMC and EC. Although GM-ECB had much lower drug content compared to controls, animal study demonstrated enhanced drug transfer and reduced drug loss of GM-ECB due to the protection of encapsulated drugs by GM, and the possible interaction between GM and endothelium. Finally, vascular patency and safety were assessed using ISR-induced porcine models. We suggest an advanced DCB strategy to alleviate rapid drug clearance by bloodstream while improving drug delivery for a long-term vascular patency. (c) 2023 Acta Materialia Inc. Published by Elsevier Ltd. All rights reserved.
引用
收藏
页码:314 / 324
页数:11
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