首页> 外文期刊>Tissue engineering >In vivo biocompatibility and degradation studies of polyhydroxyoctanoate in the rat: a new sealant for the polyester arterial prosthesis.
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In vivo biocompatibility and degradation studies of polyhydroxyoctanoate in the rat: a new sealant for the polyester arterial prosthesis.

机译:聚羟基辛酸酯在大鼠中的体内生物相容性和降解研究:聚酯动脉假体的新型密封剂。

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摘要

The present study examined the biocompatibility and degradation properties of poly (beta-hydroxy octanoate) (PHO) as an impregnation substrate on arterial prostheses. PHO-impregnated polyester grafts sterilized by ethylene oxide (EO) or gamma (gamma) radiation, and polyester Dacron(R) prostheses impregnated with fluoropolymer, gelatin, or albumin were implanted subcutaneously in rats for periods ranging from 2 to 180 days. The biocompatibility was assessed by quantifying the alkaline and acid phosphatase secretion while performing histological studies at the tissue/prosthesis interface. The degradation was determined by chemical analysis of the EO and gamma-sterilized PHO after implantation using differential scanning calorimetry (DSC), wide angle x-ray diffraction (WAXD), and size exclusion chromatography (SEC). Alkaline phosphatase activity by the sterilized PHO and by the gelatin and albumin grafts was significantly elevated early after implantation in contrast to that of the Dacron and fluoropolymer grafts that occurred later, at 7 and 5 days, respectively The peak of acid phosphatase activity for all of the grafts occurred between 5 and 10 days postimplantation, with the gamma-sterilized PHO grafts recording the greatest activity. Histological study revealed that the tissue incorporation into the graft wall was earlier and more complete for the Dacron and fluoropolymer grafts after 6 months than for the gelatin and albumin grafts, because the latter induced important inflammatory reactions during the resorption of the cross-linked protein substrates. The EO and gamma-sterilized PHO grafts exhibited a similar healing sequence characterized by the development of a collagenous tissue surrounding the prostheses. However, no infiltration of tissue into the graft wall was observed after 6 months, mainly because of the presence of the PHO. Degradation of the EO and gamma-sterilized PHO occurred preferentially by a hydrolytic mechanism as shown by a 30% molecular weight decrease after 6 months. In conclusion, PHO showed good biocompatibility in terms of enzyme activity and tissue reaction. Degradation was a slow, in vivo process controlled primarily by a random hydrolytic reaction and by a local enzymatic attack by macrophages and giant cells.
机译:本研究检查了聚(β-羟基辛酸酯)(PHO)作为动脉假体上的浸渍基质的生物相容性和降解特性。将经环氧乙烷(EO)或γ(γ)辐射灭菌的经过PHO浸渍的聚酯移植物,以及经氟聚合物,明胶或白蛋白浸渍的聚酯Dacron(R)假体,经皮下植入大鼠体内2至180天。通过在组织/假体界面进行组织学研究时,通过定量碱性磷酸酶和酸性磷酸酶的分泌来评估生物相容性。通过使用差示扫描量热法(DSC),广角X射线衍射(WAXD)和尺寸排阻色谱法(SEC)对植入后的EO和经伽马灭菌的PHO进行化学分析来确定降解程度。植入后早期,经过消毒的PHO以及明胶和白蛋白移植物的碱性磷酸酶活性显着提高,而Dacron和含氟聚合物移植物的碱性磷酸酶活性分别在后来的7天和5天出现。移植物发生在植入后5到10天之间,经伽马灭菌的PHO移植物记录了最大的活性。组织学研究表明,Dacron和含氟聚合物移植物在6个月后比明胶和白蛋白移植物更早,更完整地并入移植物壁,因为后者在交联蛋白底物吸收过程中引起重要的炎症反应。 。 EO和经伽马灭菌的PHO移植物表现出相似的愈合过程,其特征是假体周围胶原组织的发育。然而,六个月后未观察到组织浸润到移植物壁中,这主要是由于PHO的存在。 EO和伽马灭菌的PHO的降解优先通过水解机理发生,如6个月后分子量降低30%所示。总之,PHO在酶活性和组织反应方面显示出良好的生物相容性。降解是一个缓慢的体内过程,主要受随机水解反应和巨噬细胞和巨细胞的局部酶攻击控制。

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