Small intestinal submucosa (SIS) is a naturally occurring tissue matrix composed of extracellular matrix proteins and various growth factors. SIS is derived from the porcine jejunum and functions as a remodeling scaffold for tissue repair. While SIS has proven to be a useful biomaterial for implants in vivo, problems associated with endothelialization and thrombogenicity of SIS implants may limit its vascular utility. The goal of this study was to determine if the biological properties of SIS could be improved by growing human umbilical vein endothelial cells (HUVEC) on SIS and allowing these cells to deposit human basement membrane proteins on the porcine substrate to create what we have called "conditioned" SIS (c-SIS). Using an approach in which HUVEC were grown for 2 weeks on SIS and then removed via a technique that leaves behind an intact basement membrane, we hypothesized that the surface properties of SIS might be improved. We found that when re-seeded on c-SIS, HUVEC exhibited enhanced organization of cell junctions and had increased metabolic activity compared to cells on native SIS (n-SIS). Furthermore, HUVEC grown on c-SIS released lower amounts of the pro-inflammatory prostaglandin PGI2 into the media compared to cells grown on n-SIS. Additionally, we found that adhesion of resting or activated human platelets to c-SIS was significantly decreased compared to n-SIS suggesting that, in addition to improved cell growth characteristics, conditioning SIS with human basement membrane proteins might decrease its thrombogenic potential. In summary, conditioning of porcine SIS by human endothelial cells improves key biological properties of the material that may improve its usefulness as remodeling scaffold for tissue repair. Identification of critical modifications of SIS by human endothelial cells should help guide future efforts to develop more biocompatible vascular grafts.

译文

小肠粘膜下层(SIS)是由细胞外基质蛋白和各种生长因子组成的天然组织基质。 SIS来源于猪空肠,并作为组织修复的重塑支架。尽管已证明SIS是体内植入物的有用生物材料,但与SIS植入物的内皮化和血栓形成有关的问题可能会限制其血管利用。这项研究的目的是确定SIS的生物学特性是否可以通过在SIS上生长人脐静脉内皮细胞(HUVEC)并使这些细胞在猪基质上沉积人基底膜蛋白来创造,从而创造出我们所谓的“条件” SIS(c-SIS)。我们假设使用HUVEC在SIS上生长2周,然后通过留下完整的基底膜的技术将其除去的方法,我们假设SIS的表面性能可能会得到改善。我们发现,当在c-SIS上重新播种时,与天然SIS(n-SIS)上的细胞相比,HUVEC表现出增强的细胞连接组织,并具有增加的代谢活性。此外,与在n-SIS上生长的细胞相比,在c-SIS上生长的HUVEC将较少量的促炎性前列腺素PGI2释放到培养基中。此外,我们发现与n-SIS相比,静止或激活的人类血小板对c-SIS的粘附力显着降低,这表明,除了改善细胞生长特性外,用人类基底膜蛋白调节SIS可能会降低其血栓形成潜能。总之,人内皮细胞对猪SIS的调节改善了该材料的关键生物学特性,可以提高其作为用于组织修复的重塑支架的有用性。人内皮细胞对SIS的关键修饰的鉴定应有助于指导未来开发更具生物相容性的血管移植物的努力。

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