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首页> 外文期刊>Biomaterials Science >Cell loaded 3D bioprinted GelMA hydrogels for corneal stroma engineering
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Cell loaded 3D bioprinted GelMA hydrogels for corneal stroma engineering

机译:Cell Loaded 3D生物印刷牙龈水凝胶用于角膜基质工程

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摘要

Tissue engineering aims to replace missing or damaged tissues and restore their functions. Three-dimensional (3D) printing has been gaining more attention because it enables the researchers to design and produce cell loaded constructs with predetermined shapes, sizes, and interior architecture. In the present study, a 3D bioprinted corneal stroma equivalent was designed to substitute for the native tissue. Reproducible outer and inner organization of the stroma was obtained by optimizing printing conditions such as the nozzle speed in the x-y direction and the spindle speed. 3D printed GelMA hydrogels were highly stable in PBS during three weeks of incubation (8% weight loss). Live-Dead cell viability assay showed 98% cell viability on day 21 indicating that printing conditions were suitable for keratocyte printing. Mechanical properties of the cell loaded 3D printed hydrogels increased 2-fold during this incubation period and approached those of the native cornea (ca. 20 kPa vs. 27 kPa, respectively). Expression of collagens types I and V, and proteoglycan (decorin) in keratocytes indicates maintenance of the phenotype in the hydrogels. Transparency of cell-loaded and cell-free hydrogels was over 80% (at 700 nm) during the three week culture period and comparable to that of the native cornea (85%) at the same wavelength. Thus, GelMA hydrogels bioprinted with keratocytes mimic the biological and physical properties of the corneal stroma with their excellent transparency, adequate mechanical strength, and high cell viability.
机译:组织工程旨在取代缺失或受损的组织并恢复其功能。三维(3D)印刷一直在受到更多关注,因为它使研究人员能够设计和生产具有预定形状,尺寸和内部架构的细胞负载构造。在本研究中,设计了3D生物印刷的角膜基质基质等同物用于替代天然组织。通过优化X-Y方向和主轴速度的诸如喷嘴速度之类的印刷条件,获得基质的可再现外部和内部组织。 3D印刷的凝胶马水凝胶在孵育的三周内PBS在PBS中高度稳定(8%减重)。活死细胞活力测定显示第21天的98%的细胞活力,表明印刷条件适合于角蛋白酶印刷。在该孵育期间,电池装载的3D印刷水凝胶的机械性能增加了2倍,并接近天然角膜(CA.20kPa和27kPa)的那些。在角蛋白细胞中表达胶原蛋白类型I和V和蛋白多糖(Degeoglycan(Deceogin)表明水凝胶中的表型维持。在三周培养期间,电池加载的细胞和无细胞水凝胶的透明度超过80%(在700nm),并且与同一波长的天然角膜(85%)相当。因此,凝胶水凝胶生成角膜细胞,模拟了角膜基质的生物和物理性质,其优异的透明度,充分的机械强度和高细胞活力。

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