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characterization of glycidyl methacrylate - crosslinked hyaluronan hydrogel scaffolds incorporating elastogenic hyaluronan oligomers

Characterization of glycidyl methacrylate - crosslinked hyaluronan hydrogel scaffolds incorporating elastogenic hyaluronan oligomers.

机构信息

Department of Bioengineering, Clemson University, Clemson, SC 29634, USA.

出版信息

Acta Biomater. 2011 Feb;7(2):653-65. doi: 10.1016/j.actbio.2010.08.006. Epub 2010 Aug 13.

Abstract

Prior studies on two-dimensional cell cultures suggest that hyaluronic acid (HA) stimulates cell-mediated regeneration of extracellular matrix structures, specifically those containing elastin, though such biologic effects are dependent on HA fragment size. Towards being able to regenerate three-dimensional (3-D) elastic tissue constructs, the present paper studies photo-crosslinked hydrogels containing glycidyl methacrylate (GM)-derivatized bio-inert high molecular weight (HMW) HA (1 × 10(6)Da) and a bioactive HA oligomer mixture (HA-o: MW ∼0.75 kDa). The mechanical (rheology, degradation) and physical (apparent crosslinking density, swelling ratio) properties of the gels varied as a function of incorporated HA oligomer content; however, overall, the mechanics of these hydrogels were too weak for vascular applications as stand-alone materials. Upon in vivo subcutaneous implantation, only a few inflammatory cells were evident around GM-HA gels, however their number increased as HA-o content within the gels increased, and the collagen I distribution was uniform. Smooth muscle cells (SMC) were encapsulated into GM hydrogels, and calcein acetoxymethyl detection revealed that the cells were able to endure twofold the level of UV exposure used to crosslink the gels. After 21 days of culture, SMC elastin production, measured by immunofluorescence quantification, showed HA-o to increase cellular deposition of elastic matrix twofold relative to HA-o-free GM-HA gels. These results demonstrate that cell response to HA/HA-o is not altered by their methacrylation and photo-crosslinking into a hydrogel, and that HA-o incorporation into cell-encapsulating hydrogel scaffolds can be useful for enhancing their production of elastic matrix structures in a 3-D space, important for regenerating elastic tissues.

摘要

先前关于二维细胞培养的研究表明,透明质酸(HA)可刺激细胞介导的细胞外基质结构的再生,特别是那些含有弹性蛋白的结构,但这种生物效应取决于 HA 片段大小。为了能够再生三维(3-D)弹性组织构建体,本文研究了含有甲基丙烯酸缩水甘油酯(GM)衍生的生物惰性高分子量(HMW)HA(1×10(6)Da)和生物活性 HA 低聚物混合物(HA-o:MW∼0.75 kDa)的光交联水凝胶。凝胶的机械(流变学、降解)和物理(表观交联密度、溶胀比)性质随掺入的 HA 低聚物含量而变化;然而,总的来说,这些水凝胶的力学性能太弱,无法作为独立材料用于血管应用。在体内皮下植入后,GM-HA 凝胶周围仅可见少数炎症细胞,但随着凝胶中 HA-o 含量的增加,其数量增加,胶原 I 分布均匀。平滑肌细胞(SMC)被包封在 GM 水凝胶中,钙黄绿素乙酰氧甲酯检测显示细胞能够承受交联凝胶所用的 UV 照射水平的两倍。培养 21 天后,通过免疫荧光定量法测量SMC 弹性蛋白的产生,结果表明与不含 HA-o 的 GM-HA 凝胶相比,HA-o 使细胞弹性基质的沉积增加了一倍。这些结果表明,HA/HA-o 被甲基丙烯酰化和光交联成水凝胶后,细胞对其的反应没有改变,并且将 HA-o 掺入细胞包封水凝胶支架中对于增强其在 3-D 空间中弹性基质结构的产生可能是有用的,这对于再生弹性组织很重要。

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本文引用的文献

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Trends Cardiovasc Med. 1994 Jul-Aug;4(4):165-9. doi: 10.1016/1050-1738(94)90053-1.
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