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Functional neovascularization of biodegradable dextran hydrogels with multiple angiogenic growth factors.

机译:具有多种血管生成生长因子的可生物降解的葡聚糖水凝胶的功能性新血管形成。

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摘要

Slow vascularization of functional blood limits the transplantation of tissue constructs and the recovery of ischemic and wounded tissues. Despite the widespread investigation of polysaccharide-based hydrogel scaffolds for their therapeutic applications, blood vessel ingrowth into these hydrogel scaffolds remains a challenge. We hypothesized that modifying the properties of biodegradable hydrogel scaffolds with immobilization of multiple angiogenic growth factors (GFs) would induce a rapid proliferation of functional vasculature into the scaffolds. To this end, we remodeled the hydrogel structure by decreasing crosslinking density via reduced degree of substitution of crosslinking groups, which resulted in improved hydrogel properties including reduced rigidity, increased swelling, increased vascular endothelial GF (VEGF) release capability, and facilitated rapid hydrogel disintegration and tissue ingrowth. Immobilizing VEGF in the scaffolds promoted tissue ingrowth and expedited biodegradation. Furthermore, a synergistic effect of multiple angiogenic GFs was established; the coimmobilization of VEGF+ angiopoietin-1, and VEGF+ insulin-like GF+ stromal cell-derived factor-1 induced more and larger blood vessels than any individual GF, while the combination of all GFs dramatically increased the size and number of newly formed functional vessels. Altogether, our data demonstrate that rapid, efficient, and functional neovascularization can be achieved by precisely manipulating hydrogel scaffold properties and immobilizing defined angiogenic GFs.
机译:功能性血液的缓慢血管形成限制了组织结构的移植以及缺血和受伤组织的恢复。尽管对基于多糖的水凝胶支架的治疗应用进行了广泛的研究,但是血管向内渗入这些水凝胶支架仍然是一个挑战。我们假设通过固定多个血管生成生长因子(GFs)来修饰可生物降解的水凝胶支架的特性将诱导功能性脉管系统迅速扩散到支架中。为此,我们通过降低交联基团的取代度来降低交联密度,从而重塑了水凝胶的结构,从而改善了水凝胶的性能,包括降低了刚性,增加了溶胀,增加了血管内皮GF(VEGF)的释放能力,并促进了快速的水凝胶崩解和组织向内生长。将VEGF固定在支架上可促进组织向内生长并加速生物降解。此外,建立了多种血管生成GF的协同作用。 VEGF +血管生成素-1和VEGF +胰岛素样GF +基质细胞衍生因子1的共固定作用诱导的血管比任何单个GF都更多和更大,而所有GF的组合显着增加了新形成的功能性血管的大小和数量。总而言之,我们的数据表明,可以通过精确地操纵水凝胶支架特性并固定确定的血管生成GF来实现快速,有效和功能性的新血管形成。

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