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Biological Designer Self-Assembling Peptide Nanofiber Scaffolds Significantly Enhance Osteoblast Proliferation Differentiation and 3-D Migration

机译:生物设计器自组装肽纳米纤维支架显着增强成骨细胞的增殖分化和3-D迁移。

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摘要

A class of self-assembling peptide nanofiber scaffolds has been shown to be an excellent biological material for 3-dimension cell culture and stimulating cell migration into the scaffold, as well as for repairing tissue defects in animals. We report here the development of several peptide nanofiber scaffolds designed specifically for osteoblasts. We designed one of the pure self-assembling peptide scaffolds RADA16-I through direct coupling to short biologically active motifs. The motifs included osteogenic growth peptide ALK (ALKRQGRTLYGF) bone-cell secreted-signal peptide, osteopontin cell adhesion motif DGR (DGRGDSVAYG) and 2-unit RGD binding sequence PGR (PRGDSGYRGDS). We made the new peptide scaffolds by mixing the pure RAD16 and designer-peptide solutions, and we examined the molecular integration of the mixed nanofiber scaffolds using AFM. Compared to pure RAD16 scaffold, we found that these designer peptide scaffolds significantly promoted mouse pre-osteoblast MC3T3-E1 cell proliferation. Moreover, alkaline phosphatase (ALP) activity and osteocalcin secretion, which are early and late markers for osteoblastic differentiation, were also significantly increased. We demonstrated that the designer, self-assembling peptide scaffolds promoted the proliferation and osteogenic differentiation of MC3T3-E1. Under the identical culture medium condition, confocal images unequivocally demonstrated that the designer PRG peptide scaffold stimulated cell migration into the 3-D scaffold. Our results suggest that these designer peptide scaffolds may be very useful for promoting bone tissue regeneration.
机译:一类自组装肽纳米纤维支架已被证明是用于3维细胞培养和刺激细胞向支架中迁移以及修复动物组织缺陷的优良生物材料。我们在这里报告了几种专门为成骨细胞设计的肽纳米纤维支架的开发。我们通过直接偶联至短的生物学活性基序,设计了一种纯的自组装肽支架RADA16-I。这些基序包括成骨生长肽ALK(ALKRQGRTLYGF)骨细胞分泌信号肽,骨桥蛋白细胞粘附基序DGR(DGRGDSVAYG)和2单元RGD结合序列PGR(PRGDSGYRGDS)。我们通过混合纯RAD16和Designer-Peptide溶液制备了新的肽支架,并使用AFM研究了混合纳米纤维支架的分子整合。与纯RAD16支架相比,我们发现这些设计器肽支架可显着促进小鼠成骨细胞MC3T3-E1细胞增殖。此外,碱性磷酸酶(ALP)活性和骨钙素分泌是成骨细胞分化的早期和晚期标志,也显着增加。我们证明了设计师的自组装肽支架能够促进MC3T3-E1的增殖和成骨分化。在相同的培养基条件下,共聚焦图像明确表明设计者PRG肽支架刺激了细胞向3-D支架的迁移。我们的结果表明这些设计器肽支架可能对促进骨组织再生非常有用。

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