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腹膜预处理影响长期血管移植物通畅性和重塑。

Peritoneal pre-conditioning impacts long-term vascular graft patency and remodeling.

机构信息

Department of Biomedical, Chemical Engineering, and Science, Florida Institute of Technology, Melbourne, FL 32901, United States.

Department of Biomedical, Chemical Engineering, and Science, Florida Institute of Technology, Melbourne, FL 32901, United States.

出版信息

Biomater Adv. 2023 May;148:213386. doi: 10.1016/j.bioadv.2023.213386. Epub 2023 Mar 16.

DOI:10.1016/j.bioadv.2023.213386
PMID:36948108
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11459558/
Abstract

There are questions about how well small-animal models for tissue-engineered vascular grafts (TEVGs) translate to clinical patients. Most TEVG studies used grafting times ≤6 months where conduits from generally biocompatible materials like poly(ε-caprolactone) (PCL) perform well. However, longer grafting times can result in significant intimal hyperplasia and calcification. This study tests the hypothesis that differences in pro-inflammatory response from pure PCL conduits will be consequential after long-term grafting. It also tests the long-term benefits of a peritoneal pre-implantation strategy on rodent outcomes. Electrospun conduits with and without peritoneal pre-implantation, and with 0 % and 10 % (w/w) collagen/PCL, were grafted into abdominal aortae of rats for 10 months. This study found that viability of control grafts without pre-implantation was reduced unlike prior studies with shorter grafting times, confirming the relevance of this model. Importantly, pre-implanted grafts had a 100 % patency rate. Further, pre-implantation reduced intimal hyperplasia within the graft. Differences in response between pure PCL and collagen/PCL conduits were observed (e.g., fewer CD80 and CD3 cells for collagen/PCL), but only pre-implantation had an effect on the overall graft viability. This study demonstrates how long-term grafting in rodent models can better evaluate viability of different TEVGs, and the benefits of the peritoneal pre-implantation step.

摘要

小型动物组织工程血管移植物(TEVG)模型在多大程度上能转化为临床患者,这方面存在一些问题。大多数 TEVG 研究使用的移植物时间都不超过 6 个月,在此期间,一般生物相容性材料(如聚己内酯(PCL))制成的导管性能良好。然而,较长的移植物时间可能导致显著的内膜增生和钙化。本研究测试了这样一个假设,即来自纯 PCL 导管的促炎反应的差异在长期移植物后会产生后果。它还测试了在啮齿动物中进行腹膜植入前策略对长期结果的影响。带有和不带有腹膜植入前策略的电纺导管,以及 0%和 10%(w/w)胶原蛋白/PCL 的导管,被移植到大鼠的腹主动脉中 10 个月。本研究发现,与先前较短移植物时间的研究不同,未经植入前处理的对照移植物的存活率降低,这证实了该模型的相关性。重要的是,植入前的移植物具有 100%的通畅率。此外,植入前减少了移植物内的内膜增生。在纯 PCL 和胶原蛋白/PCL 导管之间观察到了反应的差异(例如,胶原蛋白/PCL 的 CD80 和 CD3 细胞较少),但只有植入前处理对整个移植物的存活率有影响。本研究表明,在啮齿动物模型中进行长期移植物可以更好地评估不同 TEVG 的存活率,以及腹膜植入前步骤的益处。