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一种基于细胞外囊泡的无支架无血清模拟人稳定软骨的方法。

A Scaffold- and Serum-Free Method to Mimic Human Stable Cartilage Validated by Secretome.

机构信息

Laboratory of Tissue Bioengineering, National Institute of Metrology, Quality and Technology (Inmetro), Duque de Caxias, Brazil.

Post-Graduation Program of Translational Biomedicine (Biotrans), Unigranrio, Campus I, Duque de Caxias, Brazil.

出版信息

Tissue Eng Part A. 2021 Mar;27(5-6):311-327. doi: 10.1089/ten.TEA.2018.0311. Epub 2019 May 2.

Abstract

A stabilized cartilage construct without signs of hypertrophy in chondrocytes is still a challenge. Suspensions of adipose stem/stromal cells (ASCs) and cartilage progenitor cells (CPCs) were seeded into micromolded nonadhesive hydrogel to produce spheroids (scaffold- and serum-free method) characterized by size, immunohistochemistry, fusion, and biomechanical properties. After cell dissociation, they were characterized for mesenchymal cell surface markers, cell viability, and quantitative real-time polymerase chain reaction. Both targeted and nontargeted (shotgun mass spectrometry) analyses were conducted on the culture supernatants. Induced ASC spheroids (ø = 350 μm) showed high cell viability and CD73 downregulation contrasting to CD90. The transforming growth factor (TGF)-β3/TGF-β1 ratio and increased ( < 0.05), whereas interleukin (IL)-6, IL-8, , and decreased. Induced ASC spheroids were able to completely fuse and showed a higher force required to compression at day 14 ( < 0.0001). Strong collagen type II was associated with gradual decrease of collagen type X and a lower gene expression at day 14 compared with day 7 ( = 0.0352). The comparison of the secretome content of induced and non-induced ASCs and CPCs identified 138 proteins directly relevant to chondrogenesis of 704 proteins in total. Although collagen X was absent, thrombospondin-1 (TSP-1), described as antiangiogenic and antihypertrophic, and cartilage oligomeric matrix protein (COMP), a biomarker of chondrogenesis, were upregulated in induced ASC spheroids. Our scaffold- and serum-free method mimics stable cartilage acting as a tool for biomarker discovery and for regenerative medicine protocols. Impact Statement Promising adult stem cell sources for cartilage regeneration include adipose stem/stromal cells (ASCs) from subcutaneous adipose tissue. Our main objective was the development of a reproducible and easy-to-handle scaffold- and serum-free method to obtain stable cartilage from induced ASC spheroids. In addition to targeted protein profiling and biomechanical analysis, we provide the first characterization of the secretome composition for ASC spheroids, providing a useful tool to monitor chondrogenesis and a noninvasive quality control of tissue-engineered constructs. Furthermore, our secretome analysis revealed a potential novel biomarker-thrombospondin-1 (TSP-1), known by its antiangiogenic properties and recently described as an antihypertrophic protein.

摘要

仍然难以获得无软骨细胞肥大迹象的稳定软骨构建体。将脂肪干细胞/基质细胞(ASCs)和软骨祖细胞(CPCs)的悬浮液接种到微成型非粘附水凝胶中,以产生具有大小、免疫组织化学、融合和生物力学特性的球体(无支架和无血清方法)。细胞解离后,用间充质细胞表面标志物、细胞活力和实时定量聚合酶链反应对其进行表征。对培养上清液进行了靶向和非靶向(shotgun 质谱)分析。诱导的 ASC 球体(ø = 350μm)表现出高细胞活力和 CD73 下调,与 CD90 相反。转化生长因子(TGF)-β3/TGF-β1 比值增加( < 0.05),而白细胞介素(IL)-6、IL-8、和 IL-1β 减少。诱导的 ASC 球体能够完全融合,并在第 14 天( < 0.0001)时显示出更高的压缩所需力。与第 7 天相比,第 14 天的胶原 II 明显增加,胶原 X 基因表达降低( = 0.0352)。诱导的 ASC 和 CPCs 的分泌组内容物的比较确定了 704 种总蛋白中与软骨形成直接相关的 138 种蛋白。尽管缺乏胶原 X,但诱导的 ASC 球体中上调了血小板反应蛋白 1(TSP-1)和软骨寡聚基质蛋白(COMP),TSP-1 被描述为抗血管生成和抗肥大,COMP 是软骨形成的生物标志物。我们的无支架和无血清方法模拟稳定的软骨,作为生物标志物发现和再生医学方案的工具。 影响说明 用于软骨再生的有前途的成人干细胞来源包括来自皮下脂肪组织的脂肪干细胞/基质细胞(ASCs)。我们的主要目标是开发一种可重复且易于处理的无支架和无血清方法,从诱导的 ASC 球体中获得稳定的软骨。除了靶向蛋白质分析和生物力学分析外,我们还提供了 ASC 球体分泌组组成的首次表征,为监测软骨形成提供了有用的工具,并为组织工程构建体提供了非侵入性的质量控制。此外,我们的分泌组分析揭示了一种潜在的新型生物标志物-血小板反应蛋白 1(TSP-1),它以其抗血管生成特性而闻名,最近被描述为一种抗肥大蛋白。

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