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三维支架中的岩藻依聚糖与血管内皮生长因子相互作用并促进小鼠体内新血管形成。

Fucoidan in a 3D scaffold interacts with vascular endothelial growth factor and promotes neovascularization in mice.

作者信息

Purnama Agung, Aid-Launais Rachida, Haddad Oualid, Maire Muriel, Mantovani Diego, Letourneur Didier, Hlawaty Hanna, Le Visage Catherine

机构信息

Inserm, U698, Cardiovascular Bio-Engineering, X. Bichat Hospital, Univ. Paris Diderot, Sorbonne Paris Cité, Rue Henri Huchard, 75018, Paris, France.

出版信息

Drug Deliv Transl Res. 2015 Apr;5(2):187-97. doi: 10.1007/s13346-013-0177-4.

Abstract

The aim of this study was to functionalize 3D porous cross-linked scaffolds with natural non-animal sulfated polysaccharide fucoidans in order to allow a delivery of vascular endothelial growth factor (VEGF) and potentiate its angiogenic activity. Microporous (20 μm) and macroporous (200 μm) scaffolds were functionalized with low, medium, or high molecular weight fucoidans (named LMWF, MMWF, and HMWF, respectively). In vitro, addition of fucoidans promoted endothelial progenitor cells proliferation in both micro- and macroporous scaffolds. While control scaffolds without fucoidans loaded with VEGF165 (100 ng) showed a fast burst release in PBS during the first 24 h, MMWF significantly reduced the VEGF165 release (p < 0.001). Surface plasmon resonance experiments confirmed a direct interaction between MMWF and VEGF165, characterized by an affinity K D (K d/K a) of 1 × 10(-9) M. In a subcutaneous angiogenesis model in mice, fucoidan functionalized scaffolds showed a more intense vascularization response than control groups. Expression of isolectin-B4 and α-smooth muscle actin, as well as confinement of erythrocytes, demonstrated the neoformed blood vessels functionality. There was a significant difference in neovessel area and neovessel density between MMWF scaffolds or VEGF165 scaffolds and MMWF+VEGF165 scaffolds (p < 0.001 for all cases). Here, we demonstrate that fucoidan sequesters VEGF165 and delivers biological cues promoting angiogenesis. In conclusion, this study shows that hydrogels functionalized with fucoidan can direct the formation of mature vasculature through a local release of VEGF165 and can be a useful tool in ischemic tissues to guide therapeutic angiogenesis.

摘要

本研究的目的是用天然非动物来源的硫酸化多糖岩藻依聚糖对三维多孔交联支架进行功能化处理,以便实现血管内皮生长因子(VEGF)的递送并增强其血管生成活性。用低、中、或高分子量的岩藻依聚糖(分别命名为LMWF、MMWF和HMWF)对微孔(20μm)和大孔(200μm)支架进行功能化处理。在体外,添加岩藻依聚糖可促进内皮祖细胞在微孔和大孔支架中的增殖。未负载岩藻依聚糖但负载了VEGF165(100 ng)的对照支架在PBS中于最初24小时内显示出快速的突释,而MMWF显著降低了VEGF165的释放(p < 0.001)。表面等离子体共振实验证实了MMWF与VEGF165之间存在直接相互作用,其特征为亲和常数KD(KD/KA)为1×10(-9)M。在小鼠皮下血管生成模型中,岩藻依聚糖功能化的支架比对照组表现出更强烈的血管化反应。异凝集素-B4和α-平滑肌肌动蛋白的表达以及红细胞的聚集,证明了新形成血管的功能。MMWF支架或VEGF165支架与MMWF + VEGF165支架之间在新生血管面积和新生血管密度方面存在显著差异(所有情况p < 0.001)。在此,我们证明岩藻依聚糖可螯合VEGF165并传递促进血管生成的生物学信号。总之,本研究表明用岩藻依聚糖功能化的水凝胶可通过局部释放VEGF165来引导成熟血管系统的形成,并且在缺血组织中可能是指导治疗性血管生成的有用工具。

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