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即用型肝素化小直径血管移植物可降低猪模型中的急性血栓形成。

Off-the-shelf, heparinized small diameter vascular graft limits acute thrombogenicity in a porcine model.

机构信息

Department of Biomedical Engineering, Johns Hopkins University School of Medicine, Baltimore, MD 21205, United States; Department of Chemical and Biomolecular Engineering, Johns Hopkins University Whiting School of Engineering, Baltimore, MD 21218, United States; Institute for NanoBioTechnology, Johns Hopkins University, Baltimore, MD 21218, United States.

Section of Cardiac Surgery, Department of Surgery, The University of Chicago, Chicago, IL 60637, United States.

出版信息

Acta Biomater. 2022 Oct 1;151:134-147. doi: 10.1016/j.actbio.2022.07.061. Epub 2022 Aug 4.

Abstract

Thrombogenicity poses a challenge to the clinical translation of engineered grafts. Previously, small-diameter vascular grafts (sdVG) composed of fibrin hydrogel microfiber tubes (FMT) with an external poly(ε-caprolactone) (PCL) sheath supported long-term patency in mice. Towards the development of an sdVG with off-the-shelf availability, the FMT's shelf stability, scale-up, and successful conjugation of an antithrombotic drug to the fibrin scaffold are reported here. FMTs maintain mechanical stability and high-water retention after storage for one year in a freezer, in a refrigerator, or at room temperature. Low molecular weight heparin-conjugated fibrin scaffolds enabled local and sustained delivery during two weeks of enzymatic degradation. Upscaled fabrication of sdVGs provides natural biodegradable grafts with size and mechanics suitable for human application. Implantation in a carotid artery interposition porcine model exhibited no rupture with thrombi prevented in all heparinized sdVGs (n = 4) over 4-5 weeks. Remodeling of the sdVGs is demonstrated with endothelial cells on the luminal surface and initial formation of the medial layer by 4-5 weeks. However, neointimal hyperplasia at 4-5 weeks led to the stenosis and occlusion of most of the sdVGs, which must be resolved for future long-term in vivo assessments. The off-the-shelf, biodegradable heparinized fibrin sdVG layer limits acute thrombogenicity while mediating extensive neotissue formation as the PCL sheath maintains structural integrity. STATEMENT OF SIGNIFICANCE: To achieve clinical and commercial utility of small-diameter vascular grafts as arterial conduits, these devices must have off-the-shelf availability for emergency arterial bypass applications and be scaled to a size suitable for human applications. A serious impediment to clinical translation is thrombogenicity. Treatments have focused on long-term systemic drug therapy, which increases the patient's risk of bleeding complications, or coating grafts and stents with anti-coagulants, which minimally improves patient outcomes even when combined with dual anti-platelet therapy. We systematically modified the biomaterial properties to develop anticoagulant embedded, biodegradable grafts that maintain off-the-shelf availability, provide mechanical stability, and prevent clot formation through local drug delivery.

摘要

血栓形成对工程移植物的临床转化提出了挑战。此前,由纤维蛋白水凝胶微纤维管(FMT)组成的小直径血管移植物(sdVG),外部有聚(ε-己内酯)(PCL)护套,在小鼠体内支持长期通畅。为了开发具有现货供应能力的 sdVG,本文报道了 FMT 的货架稳定性、扩大规模以及将抗血栓药物成功结合到纤维蛋白支架上。FMT 在冷冻室、冰箱或室温下储存一年后,仍保持机械稳定性和高保水能力。低分子量肝素结合的纤维蛋白支架在两周的酶降解过程中实现了局部和持续的药物传递。大规模制造的 sdVG 提供了具有适合人体应用的尺寸和力学性能的天然可生物降解移植物。在颈动脉间置猪模型中的植入物未发生破裂,所有肝素化 sdVG(n=4)在 4-5 周内均未发生血栓。4-5 周时,sdVG 表面有内皮细胞,中层开始形成,表明 sdVG 发生了重塑。然而,4-5 周时的新生内膜增生导致大多数 sdVG 出现狭窄和闭塞,这必须在未来的长期体内评估中得到解决。现成的、可生物降解的肝素化纤维蛋白 sdVG 层可限制急性血栓形成,同时介导广泛的新生组织形成,而 PCL 护套则保持结构完整性。意义声明:为了使小直径血管移植物作为动脉导管在临床上和商业上得到应用,这些装置必须具有现货供应能力,以满足紧急动脉旁路应用的需要,并按适合人体应用的尺寸进行放大。血栓形成是临床转化的一个严重障碍。治疗方法集中在长期的全身药物治疗上,这会增加患者出血并发症的风险,或者用抗凝剂涂覆移植物和支架,即使与双联抗血小板治疗联合使用,也只能最小程度地改善患者的预后。我们系统地改变了生物材料的性质,开发了具有现货供应能力的、可生物降解的、抗凝剂嵌入的移植物,这些移植物具有机械稳定性,并通过局部药物输送来防止血栓形成。

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