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干细胞归巢信号通路影响下的心血管生物假体重塑。

The remodeling of cardiovascular bioprostheses under influence of stem cell homing signal pathways.

机构信息

Laboratory for Experimental Cardiac Surgery, Department of Cardiovascular Diseases, Katholieke Universiteit Leuven, Leuven, Belgium.

出版信息

Biomaterials. 2010 Jan;31(1):20-8. doi: 10.1016/j.biomaterials.2009.09.016. Epub 2009 Sep 22.

Abstract

Optimizing current heart valve replacement strategies by creating living prostheses is a necessity to alleviate complications with current bioprosthetic devices such as calcification and degeneration. Regenerative medicine, mostly in vitro tissue engineering, is the forerunner of this optimization search, yet here we show the functionality of an in vivo alternative making use of 2 homing axes for stem cells. In rats we studied the signaling pathways of stem cells on implanted bioprosthetic tissue (photooxidized bovine pericardium (POP)), by gene and protein expression analysis. We found that SDF-1alpha/CXCR4 and FN/VLA4 homing axes play a role. When we implanted vascular grafts impregnated with SDF-1alpha and/or FN as carotid artery interpositions, primitive cells were attracted from the circulation. Next, bioprosthetic heart valves, constructed from POP impregnated with SDF-1alpha and/or FN, were implanted in pulmonary position. As shown by CD90, CD34 and CD117 immunofluorescent staining they became completely recellularized after 5 months, had a normal function and biomechanical properties and specifically the combination of SDF-1alpha and FN had an optimal valve-cell phenotype.

摘要

通过创建活假体来优化当前的心脏瓣膜置换策略是必要的,以减轻当前生物假体设备如钙化和退化的并发症。再生医学,主要是体外组织工程,是这种优化搜索的先驱,但在这里我们展示了一种利用 2 个归巢轴的体内替代方法的功能。在大鼠中,我们通过基因和蛋白质表达分析研究了干细胞在植入的生物假体组织(光氧化牛心包(POP))上的信号通路。我们发现 SDF-1alpha/CXCR4 和 FN/VLA4 归巢轴起作用。当我们植入用 SDF-1alpha 和/或 FN 浸渍的血管移植物作为颈动脉间置时,来自循环的原始细胞被吸引。接下来,用 SDF-1alpha 和/或 FN 浸渍的 POP 构建的生物假体心脏瓣膜被植入肺动脉位置。如 CD90、CD34 和 CD117 免疫荧光染色所示,它们在 5 个月后完全再细胞化,具有正常的功能和生物力学特性,特别是 SDF-1alpha 和 FN 的组合具有最佳的瓣膜细胞表型。

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