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用于组织生物相容性、血管生成和炎症测试的胚胎干细胞。

Embryonic Stem Cells for Tissue Biocompatibility, Angiogenesis, and Inflammation Testing.

作者信息

Sharifpanah Fatemeh, Reinhardt Matthias, Schönleben Johanna, Meyer Claudia, Richter Madeleine, Schnabelrauch Matthias, Rode Claudia, Wartenberg Annika, Bekhite Mohamed, Sauer Heinrich, Wartenberg Maria

机构信息

Cardiology Division, Department of Internal Medicine I, Friedrich Schiller University Jena, Jena, Germany.

出版信息

Cells Tissues Organs. 2017;204(1):1-12. doi: 10.1159/000471794. Epub 2017 May 30.

DOI:10.1159/000471794
PMID:28554187
Abstract

AIM

To introduce embryoid bodies derived from mouse embryonic stem (ES) cells, which differentiate blood vessel-like structures and leukocytes, as a novel in vitro model system for biocompatibility, inflammation, and angiogenesis studies.

METHODOLOGY/RESULTS: Punched spherical discs of bioabsorbable polymers (ε-caprolactone and L-lactide in different compositions) with a diameter of 2 mm and a thickness of 0.2 mm were inoculated with embryoid bodies for cocultivation. As reference material for biocompatible, nonbioabsorbable, and bioincompatible materials, polymer punched discs of petriPERM (PP) membrane (polytetrafluoroethylene) as well as polyvinylchloride (PVC) were used. Tissue outgrowth on the polymer discs decreased and cell toxicity increased upon confrontation on bioabsorbable biomaterials and PVC. Bioabsorbable polymers as well as PVC decreased the branching points and total tube length of CD31-positive vascular structures in embryoid bodies. With the exception of PP, all applied materials increased the differentiation of CD68-positive macrophages and the generation of reactive oxygen species, which is indicative of proinflammatory processes upon contact of tissue with biomaterials. Consequently, cocultivation with polymers increased secretion of the cytokines interleukin-6, monocyte chemotactic protein-1, and tumor necrosis factor-α.

CONCLUSION

Three-dimensional tissues cultivated from ES cells are well-suited for testing the biocompatibility, the vascular response, and the inflammatory reaction towards bioabsorbable and nonbioabsorbable polymers.

摘要

目的

引入源自小鼠胚胎干细胞(ES细胞)的胚状体,其可分化出血管样结构和白细胞,作为用于生物相容性、炎症和血管生成研究的新型体外模型系统。

方法/结果:将直径2毫米、厚度0.2毫米的可生物吸收聚合物(不同组成的ε-己内酯和L-丙交酯)冲压成的球形圆盘接种胚状体进行共培养。作为生物相容性、非生物可吸收性和生物不相容性材料的参考材料,使用了petriPERM(PP)膜(聚四氟乙烯)以及聚氯乙烯(PVC)的聚合物冲压圆盘。在与可生物吸收生物材料和PVC接触时,聚合物圆盘上的组织生长减少,细胞毒性增加。可生物吸收聚合物以及PVC减少了胚状体中CD31阳性血管结构的分支点和总管长度。除PP外,所有应用材料均增加了CD68阳性巨噬细胞的分化以及活性氧的产生,这表明组织与生物材料接触时存在促炎过程。因此,与聚合物共培养增加了细胞因子白细胞介素-6、单核细胞趋化蛋白-1和肿瘤坏死因子-α的分泌。

结论

由ES细胞培养的三维组织非常适合测试对可生物吸收和不可生物吸收聚合物的生物相容性、血管反应和炎症反应。

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