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Novel biologically-inspired rosette nanotube PLLA scaffolds for improving human mesenchymal stem cell chondrogenic differentiation

机译:新型生物启发的玫瑰花纳米管PLLA支架,用于改善人间充质干细胞的软骨分化

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Cartilage defects are a persistent issue in orthopedic tissue engineering where acute and chronic tissue damage stemming from osteoarthritis, trauma, and sport injuries, present a common and serious clinical problem. Unlike bone, cartilage repair continues to be largely intractable due to the tissue's inherently poor regenerative capacity. Thus, the objective of this study is to design a novel tissue engineered nanostructured cartilage scaffold via biologically-inspired self-assembling rosette nanotubes (RNTs) and biocompatible non-woven poly (L-lactic acid) (PLLA) for enhanced human bone marrow mesenchymal stem cell (hMSC) chondrogenic differentiation. Specifically, RNTs are a new class of biomimetic supramolecular nanomaterial obtained through the self-assembly of low-molecular-weight modified guanine/cytosine DNA base hybrids (the G∧C motif) in an aqueous environment. In this study, we synthesized a novel twin G∧C-based RNT (TB-RGDSK) functionalized with cell-favorable arginine-glycine-aspartic acid-serine-lysine (RGDSK) integrin binding peptide and a twin G∧C based RNT with an aminobutane linker molecule (TBL). hMSC adhesion, proliferation and chondrogenic differentiation were evaluated in vitro in scaffold groups consisting of biocompatible PLLA with TBL, 1:9 TB-RGDSK:TBL, and TB-RGDSK, respectively. Our results show that RNTs can remarkably increase total glycosaminoglycan, collagen, and protein production when compared to PLLA controls without nanotubes. Furthermore, the TB-RGDSK with 100% well-organized RGDSK peptides achieved the highest chondrogenic differentiation of hMSCs. The current in vitro study illustrated that RNT nanotopography and surface chemistry played an important role in enhancing hMSC chondrogenic differentiation thus making them promising for cartilage regeneration.
机译:软骨缺损在整形外科组织工程中是一个持续存在的问题,在该问题中,由于骨关节炎,外伤和运动损伤而引起的急性和慢性组织损伤是常见且严重的临床问题。与骨骼不同,由于组织固有的再生能力差,软骨修复在很大程度上仍然难以解决。因此,本研究的目的是通过生物启发的自组装玫瑰花碳纳米管(RNT)和生物相容性非织造聚(L-乳酸)(PLLA)设计一种新型的组织工程化纳米结构软骨支架,以增强人骨髓间充质干细胞(hMSC)软骨分化。具体而言,RNT是通过在水环境中自组装低分子量修饰的鸟嘌呤/胞嘧啶DNA基础杂化物(G∧C基序)而获得的新型仿生超分子纳米材料。在这项研究中,我们合成了一种新型的基于双G∧C的RNT(TB-RGDSK),其功能是对细胞有利的精氨酸-甘氨酸-天冬氨酸-丝氨酸-赖氨酸(RGDSK)整合素结合肽和一个双G∧C的RNT氨基丁烷接头分子(TBL)。在分别由具有TBL,1:9 TB-RGDSK:TBL和TB-RGDSK的生物相容性PLLA组成的支架组中,体外评估了hMSC的粘附,增殖和软骨形成分化。我们的结果表明,与不含纳米管的PLLA对照相比,RNTs可以显着增加总糖胺聚糖,胶原蛋白和蛋白质的产生。此外,具有100%组织良好的RGDSK肽的TB-RGDSK实现了hMSCs的最高软骨分化。当前的体外研究表明,RNT纳米形貌和表面化学在增强hMSC软骨形成分化中起着重要作用,因此使其有望用于软骨再生。

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