间充质干细胞陪伴高效工程化人耳软骨

IF 3.1 3区 生物学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY
Xue Dong, Carly Askinas, Jongkil Kim, John E. Sherman, Lawrence J. Bonassar, Jason A. Spector
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引用次数: 6

摘要

用于耳部重建的组织工程耳部支架的临床转化面临的主要挑战是患者耳软骨细胞(hAuC)的产量有限。从培养中相对少量的软骨细胞开始,导致去分化和表型丧失,随后扩大。为了显著减少人弹性软骨工程所需的软骨细胞数量,我们将人间充质干细胞(hMSCs)与HAuCs共培养,以促进健康的弹性软骨形成。将HAuCs与人骨髓源性hMSCs以2500万/mL总细胞密度、不同比例(HAuCs/hMSCs: 10/90、25/75、50/50)的1% I型胶原包膜,注射到定制的3d打印聚乳酸(PLA)脊状外支架中,模拟耳廓螺旋缘形状,在裸鼠皮下植入1、3、6个月。6个月后,所有比例的外植体都显示出几乎完全的体积保存和脊状“螺旋”特征的地形维持。软骨组织在支架内形成3个月,组织学分析证实,在构建物内形成成熟的弹性软骨,软骨细胞在II型胶原蛋白和富含蛋白聚糖的基质内的腔隙中可见,并被新软骨外膜包围。6个月后达到了与人体弹性软骨相当的压缩力学性能。在外用支架内将hAuC和hMSCs共同植入胶原中,即使hAuC仅占植入细胞群的10%,也能有效地产生成形的人弹性软骨,而体积没有损失,这标志着耳廓组织工程临床转化的关键一步。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Efficient engineering of human auricular cartilage through mesenchymal stem cell chaperoning

A major challenge to the clinical translation of tissue-engineered ear scaffolds for ear reconstruction is the limited auricular chondrocyte (hAuC) yield available from patients. Starting with a relatively small number of chondrocytes in culture results in dedifferentiation and loss of phenotype with subsequent expansion. To significantly decrease the number of chondrocytes required for human elastic cartilage engineering, we co-cultured human mesenchymal stem cells (hMSCs) with HAuCs to promote healthy elastic cartilage formation. HAuCs along with human bone marrow-derived hMSCs were encapsulated into 1% Type I collagen at 25 million/mL total cell density with different ratios (HAuCs/hMSCs: 10/90, 25/75, 50/50) and then injected into customized 3D-printed polylactic acid (PLA) ridged external scaffolds, which simulate the shape of the auricular helical rim, and implanted subcutaneously in nude rats for 1, 3 and 6 months. The explanted constructs demonstrated near complete volume preservation and topography maintenance of the ridged “helical” feature after 6 months with all ratios. Cartilaginous appearing tissue formed within scaffolds by 3 months, verified by histologic analysis demonstrating mature elastic cartilage within the constructs with chondrocytes seen in lacunae within a Type II collagen and proteoglycan-enriched matrix, and surrounded by a neoperichondrial external layer. Compressive mechanical properties comparable to human elastic cartilage were achieved after 6 months. Co-implantation of hAuCs and hMSCs in collagen within an external scaffold efficiently produced shaped human elastic cartilage without volume loss even when hAuC comprised only 10% of the implanted cell population, marking a crucial step toward the clinical translation of auricular tissue engineering.

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来源期刊
CiteScore
7.50
自引率
3.00%
发文量
97
审稿时长
4-8 weeks
期刊介绍: Journal of Tissue Engineering and Regenerative Medicine publishes rapidly and rigorously peer-reviewed research papers, reviews, clinical case reports, perspectives, and short communications on topics relevant to the development of therapeutic approaches which combine stem or progenitor cells, biomaterials and scaffolds, growth factors and other bioactive agents, and their respective constructs. All papers should deal with research that has a direct or potential impact on the development of novel clinical approaches for the regeneration or repair of tissues and organs. The journal is multidisciplinary, covering the combination of the principles of life sciences and engineering in efforts to advance medicine and clinical strategies. The journal focuses on the use of cells, materials, and biochemical/mechanical factors in the development of biological functional substitutes that restore, maintain, or improve tissue or organ function. The journal publishes research on any tissue or organ and covers all key aspects of the field, including the development of new biomaterials and processing of scaffolds; the use of different types of cells (mainly stem and progenitor cells) and their culture in specific bioreactors; studies in relevant animal models; and clinical trials in human patients performed under strict regulatory and ethical frameworks. Manuscripts describing the use of advanced methods for the characterization of engineered tissues are also of special interest to the journal readership.
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