首页> 外文期刊>International Journal of Nanomedicine >Sustained dual release of placental growth factor-2 and bone morphogenic protein-2 from heparin-based nanocomplexes for direct osteogenesis
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Sustained dual release of placental growth factor-2 and bone morphogenic protein-2 from heparin-based nanocomplexes for direct osteogenesis

机译:从基于肝素的纳米复合物中持续双重释放胎盘生长因子2和骨形态发生蛋白2以直接成骨

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Objective: To compare the direct osteogenic effect between placental growth factor-2 (PlGF-2) and bone morphogenic protein-2 (BMP-2). Methods: Three groups of PlGF-2/BMP-2-loaded heparin–N-(2-hydroxyl) propyl-3-trimethyl ammonium chitosan chloride (HTCC) nanocomplexes were prepared: those with 0.5 μg PlGF-2; with 1.0 μg BMP-2; and with 0.5 μg PlGF-2 combined with 1.0 μg BMP-2. The loading efficiencies and release profiles of these growth factors (GFs) in this nanocomplex system were quantified using enzyme-linked immunosorbent assay, their biological activities were evaluated using cell counting kit-8, cell morphology, and cell number counting assays, and their osteogenic activities were quantified using alkaline phosphatase and Alizarin Red S staining assays. Results: The loading efficiencies were more than 99% for the nanocomplexes loaded with just PlGF-2 and for those loaded with both PlGF-2 and BMP-2. For the nanocomplex loaded with just BMP-2, the loading efficiency was more than 97%. About 83%–84% of PlGF-2 and 89%–91% of BMP-2 were stably retained on the nanocomplexes for at least 21 days. In in vitro biological assays, PlGF-2 exhibited osteogenic effects comparable to those of BMP-2 despite its dose in the experiments being lower than that of BMP-2. Moreover, the results implied that heparin-based nanocomplexes encapsulating two GFs have enhanced potential in the enhancement of osteoblast function. Conclusion: PlGF-2-loaded heparin–HTCC nanocomplexes may constitute a promising system for bone regeneration. Moreover, the dual delivery of PlGF-2 and BMP-2 appears to have greater potential in bone tissue regeneration than the delivery of either GFs alone.
机译:目的:比较胎盘生长因子2(PlGF-2)和骨形态发生蛋白2(BMP-2)的直接成骨作用。方法:制备三组PlGF-2 / BMP-2肝素-N-(2-羟基)丙基-3-三甲基铵壳聚糖氯化物(HTCC)纳米复合物:0.5μgPlGF-2;含1.0μgBMP-2;并与0.5μgPlGF-2和1.0μgBMP-2结合使用。使用酶联免疫吸附测定法对这些纳米复合物系统中这些生长因子(GFs)的负载效率和释放曲线进行了定量,使用细胞计数试剂盒8,细胞形态学和细胞数计数测定法评估了它们的生物学活性,以及​​它们的成骨性使用碱性磷酸酶和茜素红S染色测定法定量活性。结果:对于仅装载PlGF-2的纳米复合物以及同时装载PlGF-2和BMP-2的纳米复合物,装载效率均超过99%。对于仅负载BMP-2的纳米复合物,负载效率超过97%。约83%–84%的PlGF-2和89%–91%的BMP-2稳定保留在纳米复合物中至少21天。在体外生物学测定中,尽管PlGF-2在实验中的剂量低于BMP-2的剂量,但仍显示出与BMP-2相当的成骨作用。此外,该结果暗示包封两个GF的基于肝素的纳米复合物具有增强成骨细胞功能的潜力。结论:加载PlGF-2的肝素-HTCC纳米复合物可能构成有希望的骨再生系统。而且,PlGF-2和BMP-2的双重递送似乎在骨组织再生中具有比单独的任一GF的递送更大的潜力。

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