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Characterisation of the Stability and Bio-functionality of Tethered Proteins on Bioengineered Scaffolds: Implications for Stem Cell Biology and Tissue Repair

机译:生物工程支架上系束性蛋白质的稳定性和生物功能的特征:干细胞生物学和组织修复的影响

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In the context of biological applications, the timely delivery of molecules can be critical for cellular and organ function. As such, previous studies have demonstrated the superior long-term protein delivery, by way of protein tethering onto bioengineered scaffolds, compared to conventional delivery of soluble protein in vitro and in vivo. Despite such benefits little knowledge exists regarding the stability, release kinetics, longevity, activation of intracellular pathway and functionality of these proteins over time. By way of example, here we examined the stability, degradation and functionality of a protein, glial derived neurotrophic factor (GDNF), which is known to influence neuronal survival, differentiation and neurite morphogenesis. Enzyme-linked immuno-sorbent assays revealed that GDNF, covalently tethered onto polycaprolactone electrospun nanoiibrous scaffolds, remained present on the scaffold surface for 120 days, with no evidence of protein leaching or degradation. The tethered GDNF protein remained functional and capable of activating downstream signalling cascades, as revealed by its capacity to phosphorylate intracellular Erk in a neural cell line. Furthermore, immobilisation of GDNF protein promoted cell survival and differentiation in culture at both 3 and 7 days. This study provides important evidence of the stability and functionality kinetics of tethered molecules.
机译:在生物应用的背景下,及时递送分子对于细胞和器官功能至关重要。因此,与在体外和体内的可溶性蛋白质的常规递送相比,以前的研究通过蛋白质束缚,通过蛋白质束缚,通过蛋白质束缚,证明了优异的长期蛋白质递送。尽管存在这种益处,但对于稳定性,释放动力学,寿命,长时间途径的激活以及这些蛋白质随时间的效果存在很少的知识。举例来说,在这里,我们研究了蛋白质,胶质衍生的神经营养因子(GDNF)的稳定性,降解和功能,这已知会影响神经元存活,分化和神经态的形态发生。酶联免疫吸附剂测定表明,与聚己内酯电纺纳米颤膜纳米颤膜支架上的GDNF保持在支架表面上持续120天,没有蛋白质浸出或降解的证据。束缚的GDNF蛋白仍然是官能的并且能够激活下游信号传导级联,如其在神经细胞系中磷酸化细胞内ERK的能力所揭示的。此外,在3和7天内,将GDNF蛋白的固定促进细胞存活和培养物的分化。本研究提供了束缚分子稳定性和功能动力学的重要证据。

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