Influence of Nanohelical Shape and Periodicity on Stem Cell Fate

被引:87
作者
Das, Rajat K. [1 ]
Zouani, Omar F. [1 ]
Labrugere, Christine [2 ]
Oda, Reiko [1 ]
Durrieu, Marie-Christine [1 ]
机构
[1] Univ Bordeaux, UMR 5248, CBMN, CNRS,ENITAB,Inst Europeen Chim & Biol, F-33607 Pessac, France
[2] Univ Bordeaux, CNRS, ICMCB, F-33608 Pessac, France
关键词
silica nanostructures; nanohelical periodicity; surface functionalization; stem cell microenvironment; cell differentiation; PEPTIDE AMPHIPHILE NANOFIBERS; OSTEOGENESIS-IMPERFECTA; OSTEOPROGENITOR RESPONSE; SILICA NANOHELICES; CHIRAL COUNTERIONS; MATRIX ELASTICITY; DIFFERENTIATION; COLLAGEN; NANOSTRUCTURES; MODULATION;
D O I
10.1021/nn4001325
中图分类号
O6 [化学];
学科分类号
070301 [无机化学];
摘要
Microenvironments such as protein composition, physical features, geometry, and elasticity play important roles in stem cell lineage specification. The components of the extracellular matrix are known to subsequently assemble into fibrillar networks in vivo with defined periodicity. However, the effect of the most critical parameter, which involves the periodicity of these fibrillar networks, on the stem cell fate is not yet investigated. Here, we show the effect of synthetic fibrillar networks patterned with nanometric periodicities, using bottom-up approaches, on the response of stem cells. We have used helical organic nanoribbons based on self-assemblies of Gemini-type amphiphiles to access chiral silica nanoribbons with two different shapes and periodicities (twisted ribbons and helical ribbons) from the same native self-assembled organic nanostructure. We demonstrate the covalent grafting of these silica nanoribbons onto activated glass substrates and the influence of this programmed isotropically oriented matrix to direct the commitment of human mesenchymal stem cells (hMSCs) into osteoblast lineage in vitro, free of osteogenic-inducing media. The specific periodicity of 63 nm (5 nm) with helical ribbon shape induces specific cell adhesion through the fibrillar focal adhesion formation and leads to stem cell commitment into osteoblast lineage. In contrast, the matrix of periodicity 100 nm (15 nm) with twisted ribbon shape does not lead to osteoblast commitment. The inhibition of non-muscle myosin II with blebbistatin is sufficient to block this osteoblast commitment on helical nanoribbon matrix, demonstrating that stem cells interpret the nanohelical shape and periodicity environment physically. These results indicate that hMSCs could interpret nanohelical shape and periodicity in the same way they sense microenvironment elasticity. This provides a promising tool to promote hMSC osteogenic capacity, which can be exploited in a 3D scaffold for bone tissue engineering.
引用
收藏
页码:3351 / 3361
页数:11
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