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Cell-mediated delivery and targeted erosion of vascular endothelial growth factor-crosslinked hydrogels

机译:血管内皮生长因子交联的水凝胶的细胞介导递送和靶向侵蚀

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We have previously reported a novel polymeric delivery vehicle that is assembled via interaction between heparin and the vascular endothelial growth factor (VEGF). Here, the cell-responsiveness of this hydrogel -including the delivery of VEGF in response to VEGFR-2 overexpressing PAE/KDR cells (porcine aortic endothelial cells (PAE) equipped with the transcript for the kinase insert domain receptor (KDR)), consequent erosion of the hydrogel matrix, and cellular response -are highlighted. The release of VEGF and hydrogel erosion reached 100% only in the presence of PAE/KDR. The [PEG-LMWH/VEGF] hydrogel (PEG = polyethylene glycol), LMWH = low molecular weight heparin) correspondingly prompted increases in VEGFR-2 phosphorylation and proliferation of PAE/KDR cells. This study proves that growth factor-crosslinked hydrogels can liberate VEGF in response to specific receptors, causing gel erosion and desired cell responses. The promise of these approaches in therapeutic applications, including targeted delivery, is suggested. (Figure Presented)
机译:先前我们已经报道了一种新型的聚合物递送载体,其通过肝素和血管内皮生长因子(VEGF)之间的相互作用组装而成。因此,这种水凝胶的细胞反应性-包括响应过表达VEGFR-2的PAE / KDR细胞(配备有激酶插入域受体(KDR)转录本的猪主动脉内皮细胞(PAE))响应的VEGF递送突出了水凝胶基质的侵蚀和细胞反应。仅在PAE / KDR存在下,VEGF的释放和水凝胶侵蚀才达到100%。 [PEG-LMWH / VEGF]水凝胶(PEG =聚乙二醇),LMWH =低分子量肝素)相应地促使PAE / KDR细胞的VEGFR-2磷酸化和增殖增加。这项研究证明,生长因子交联的水凝胶可以响应特定受体而释放VEGF,从而引起凝胶侵蚀和所需的细胞反应。建议在治疗应用中使用这些方法,包括靶向给药。 (图呈现)

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