乙二醇
化学
单层
表面改性
X射线光电子能谱
高分子化学
组合化学
有机化学
化学工程
生物化学
物理化学
工程类
作者
Simon J. Todd,David J. Scurr,Julie E. Gough,Morgan R. Alexander,Rein V. Ulijn
出处
期刊:Langmuir
[American Chemical Society]
日期:2009-04-30
卷期号:25 (13): 7533-7539
被引量:59
摘要
We report on the design, stepwise synthesis, and surface analysis of enzyme-responsive surfaces that present cell adhesive RGD sequences on-demand, that is, by enzymatic hydrolysis of inactive RGD containing precursors that carry cleavable steric blocking groups. These surfaces, incorporating poly(ethylene glycol) (PEG) monolayers coupled via epoxy silanes to glass, are functionalized via stepwise solid phase synthesis, presenting a versatile and straightforward approach to preparation of peptide surfaces. Successive amino acid coupling and deprotection steps using fluorenylmethoxycarbonyl (Fmoc) chemistry are verified using surface analysis with time-of-flight secondary-ion mass spectrometry (ToF-SIMS) and X-ray photoelectron spectroscopy (XPS). Exposure of surfaces to elastase results in activation of cell binding ligands as demonstrated using osteoblast cells. These surfaces may have applications in spatiotemporally controlled attachment of cells as relevant for three-dimensional tissue engineering scaffolds and cell-based biosensors.
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