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利用3D生物打印技术和酶交联水凝胶设计与制造成熟的工程化心脏前组织

Design and Fabrication of Mature Engineered Pre-Cardiac Tissue Utilizing 3D Bioprinting Technology and Enzymatically Crosslinking Hydrogel.

作者信息

Iwanaga Shintaroh, Hamada Yuta, Tsukamoto Yoshinari, Arai Kenichi, Kurooka Taketoshi, Sakai Shinji, Nakamura Makoto

机构信息

Graduate School of Science and Engineering, University of Toyama, Toyama 930-8555, Japan.

Department of Clinical Biomaterial Applied Science, School of Medicine, University of Toyama, Toyama 930-0194, Japan.

出版信息

Materials (Basel). 2022 Nov 9;15(22):7928. doi: 10.3390/ma15227928.

Abstract

The fabrication of mature engineered cardiac tissue is one of the major challenges in cardiac tissue engineering. For this purpose, we attempted to apply the 3D bioprinting approach. Aiming to construct an oriented tissue, a fine fiber-shaped scaffold with a support structure was first designed using CAD software. Then, a 3D bioprinter and cell-adhesive bio-inks were utilized to fabricate this structure. The cell-adhesive bio-inks were synthesized by combining sodium alginate and gelatin with tyramine, respectively, to form pre-gel materials that allow enzymatic crosslinking by horseradish peroxidase. By absorbance measurements, we confirmed that the tyramine modification rate of each polymer was 0.535 mmol/g-alginate and 0.219 mmol/g-gelatin. The width of the fiber-shaped scaffold was 216.8 ± 24.3 μm for the fabricated scaffold, while the design value was 200 μm. After 3D printing and adhesion-adding treatment of the scaffold with these bio-ink materials, cardiomyocytes were seeded and cultured. As a result, the cells spread onto the scaffold, and the entire pre-tissue contracted synchronously by day 6 of culture, showing a greater pulsatility than in the early days. Video analysis showed that the beating rate of pre-myocardial tissue on day 6 was 31 beats/min. In addition, we confirmed that the cardiomyocytes partially elongated along the long axis of the fiber-shaped scaffold in the pre-tissue cultured for 15 days by staining actin, suggesting the possibility of cell orientation. Furthermore, treatment with adrenaline resulted in a 7.7-fold increase in peak beating rate compared to that before treatment (from 6 beats/min to 46 beats/min), confirming the responsiveness of the pre-tissues to the drug. These results indicate that 3D bioprinting effectively produces mature cultured myocardial tissue that is oriented, contracts synchronously, and is responsive to drugs.

摘要

成熟工程化心肌组织的构建是心脏组织工程中的主要挑战之一。为此,我们尝试应用3D生物打印方法。为构建定向组织,首先使用CAD软件设计了一种带有支撑结构的细纤维状支架。然后,利用3D生物打印机和细胞黏附性生物墨水来制造该结构。细胞黏附性生物墨水分别通过将海藻酸钠和明胶与酪胺结合合成,形成可通过辣根过氧化物酶进行酶交联的预凝胶材料。通过吸光度测量,我们确认每种聚合物的酪胺修饰率分别为0.535 mmol/g - 海藻酸钠和0.219 mmol/g - 明胶。所制造支架的纤维状支架宽度为216.8 ± 24.3 μm,而设计值为200 μm。在用这些生物墨水材料对支架进行3D打印和添加黏附处理后,接种并培养心肌细胞。结果,细胞铺展在支架上,培养第6天时整个预组织同步收缩,显示出比早期更大的搏动性。视频分析表明,培养第6天时心肌前体组织的搏动频率为31次/分钟。此外,通过对肌动蛋白进行染色,我们确认在培养15天的预组织中,心肌细胞部分沿纤维状支架的长轴伸长,提示细胞定向的可能性。此外,与治疗前相比,肾上腺素处理使搏动峰值频率增加了7.7倍(从6次/分钟增加到46次/分钟),证实了预组织对该药物的反应性。这些结果表明,3D生物打印有效地产生了定向、同步收缩且对药物有反应的成熟培养心肌组织。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9e31/9693247/e6ce9cef1b8b/materials-15-07928-g001.jpg

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