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含氧化石墨烯的可降解聚甲基丙烯酸羟乙酯水凝胶的长期体内降解及生物相容性

Long-term in vivo degradation and biocompatibility of degradable pHEMA hydrogels containing graphene oxide.

作者信息

Moura Duarte, Rohringer Sabrina, Ferreira Helena P, Pereira Andreia T, Barrias Cristina C, Magalhães Fernão D, Bergmeister Helga, Gonçalves Inês C

机构信息

INEB - Instituto de Engenharia Biomédica, Universidade do Porto, Rua Alfredo Allen, 208, Porto 4200-180, Portugal; i3S - Instituto de Investigação e Inovação em Saúde, Universidade do Porto, Rua Alfredo Allen, 208, Porto 4200-180, Portugal; FEUP - Faculdade de Engenharia, Departamento de Engenharia Metalúrgica e de Materiais, Universidade do Porto, Rua Dr. Roberto Frias, Porto 4200-465, Portugal.

Center for Biomedical Research and Translational Surgery, Medical University of Vienna, Vienna, Austria.

出版信息

Acta Biomater. 2024 Jan 1;173:351-364. doi: 10.1016/j.actbio.2023.11.012. Epub 2023 Nov 19.

DOI:10.1016/j.actbio.2023.11.012
PMID:37984630
Abstract

Developing biocompatible, non-fouling and biodegradable hydrogels for blood-contacting devices remains a demanding challenge. Such materials should promote natural healing, prevent clotting, and undergo controlled degradation. This study evaluates the biocompatibility and biodegradation of degradable poly(2-hydroxyethyl methacrylate) (d-pHEMA) hydrogels with or without reinforcement with oxidized few-layer graphene (d-pHEMA/M5ox) in a long term implantation in rats, assessing non-desired side-effects (irritation, chronic toxicity, immune response). Subcutaneous implantation over 6 months revealed degradation of both hydrogels, despite slower for d-pHEMA/M5ox, with degradation products found in intracellular vesicles. No inflammation nor infection at implantation areas were observed, and no histopathological findings were detected in parenchymal organs. Immunohistochemistry confirmed d-pHEMA and d-pHEMA/M5ox highly anti-adhesiveness. Gene expression of macrophages markers revealed presence of both M1 and M2 macrophages at all timepoints. M1/M2 profile after 6 months reveals an anti-inflammatory environment, suggesting no chronic inflammation, as also demonstrated by cytokines (IL-α, TNF-α and IL-10) analysis. Overall, modification of pHEMA towards a degradable material was successfully achieved without evoking a loss of its inherent properties, specially its anti-adhesiveness and biocompatibility. Therefore, these hydrogels hold potential as blank-slate for further modifications that promote cellular adhesion/proliferation for tissue engineering applications, namely for designing blood contacting devices with different load bearing requirements. STATEMENT OF SIGNIFICANCE: Biocompatibility, tunable biodegradation kinetics, and suitable immune response with lack of chronic toxicity and irritation, are key features in degradable blood contact devices that demand long-term exposure. We herein evaluate the 6-month in vivo performance of a degradable and hemocompatible anti-adhesive hydrogel based in pHEMA, and its mechanically reinforced formulation with few-layer graphene oxide. This subcutaneous implantation in a rat model, shows gradual degradation with progressive changes in material morphology, and no evidence of local inflammation in surrounding tissue, neither signs of inflammation or adverse reactions in systemic organs, suggesting biocompatibility of degradation products. Such hydrogels exhibit great potential as a blank slate for tissue engineering applications, including for blood contact, where cues for specific cells can be incorporated.

摘要

开发用于血液接触装置的生物相容性、抗污染且可生物降解的水凝胶仍然是一项艰巨的挑战。这类材料应促进自然愈合、防止凝血并经历可控降解。本研究评估了可降解的聚甲基丙烯酸羟乙酯(d-pHEMA)水凝胶在有或没有用氧化少层石墨烯增强(d-pHEMA/M5ox)的情况下,在大鼠体内长期植入后的生物相容性和生物降解情况,评估了不良副作用(刺激、慢性毒性、免疫反应)。超过6个月的皮下植入显示两种水凝胶均发生降解,尽管d-pHEMA/M5ox降解较慢,在细胞内小泡中发现了降解产物。在植入区域未观察到炎症或感染,在实质器官中未检测到组织病理学发现。免疫组织化学证实d-pHEMA和d-pHEMA/M5ox具有高度抗粘附性。巨噬细胞标志物的基因表达显示在所有时间点均存在M1和M2巨噬细胞。6个月后的M1/M2图谱显示出抗炎环境,表明没有慢性炎症,细胞因子(IL-α、TNF-α和IL-10)分析也证明了这一点。总体而言,成功地将pHEMA改性为可降解材料,而没有丧失其固有特性,特别是其抗粘附性和生物相容性。因此,这些水凝胶作为进一步改性的空白载体具有潜力,可促进细胞粘附/增殖用于组织工程应用,即用于设计具有不同承载要求的血液接触装置。重要性声明:生物相容性、可调节的生物降解动力学以及合适的免疫反应,同时缺乏慢性毒性和刺激,是需要长期暴露于血液的可降解血液接触装置的关键特征。我们在此评估了基于pHEMA的可降解且血液相容性抗粘附水凝胶及其用少层氧化石墨烯进行机械增强的配方在体内6个月的性能。在大鼠模型中的这种皮下植入显示材料形态逐渐降解并发生渐进性变化,在周围组织中没有局部炎症的证据,在全身器官中也没有炎症或不良反应的迹象,表明降解产物具有生物相容性。这类水凝胶作为组织工程应用的空白载体具有巨大潜力,包括用于血液接触,在其中可以纳入针对特定细胞的信号。

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