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首页> 外文期刊>Journal of materials science >Growth on poly(L-lactic acid) porous scaffold preserves CD73 and CD90 immunophenotype markers of rat bone marrow mesenchymal stromal cells
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Growth on poly(L-lactic acid) porous scaffold preserves CD73 and CD90 immunophenotype markers of rat bone marrow mesenchymal stromal cells

机译:在聚(L-乳酸)多孔支架上的生长保留了大鼠骨髓间充质基质细胞的CD73和CD90免疫表型标记

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摘要

Few data are available on the effect of bioma-terials on surface antigens of mammalian bone marrow-derived, adult mesenchymal stromal cells (MSCs). Since poly(L-lactic acid) or PLLA is largely used in tissue engineering of human bones, and we are developing a reverse engineering program to prototype with biomaterials the vascular architecture of bones for their bioartificial reconstruction, both in humans and animal models, we have studied the effect of porous, flat and smooth PLLA scaffolds on the immunophenotype of in vitro grown, rat MSCs in the absence of any coating, co-polymeric enrichment, and differentiation stimuli. Similar to controls on plastic, we show that our PLLA scaffold does not modify the distribution of some surface markers in rat MSCs. In particular, the maintained expression of CD73 and CD90 on two different sub-populations (small and large cells) is consistent with their adhesion to the PLLA scaffold through specialized appendages, and to their prominent content in actin. In addition, our PLLA scaffold favours retention of the intermediate filament desmin, believed a putative marker of undifferentiated state. Finally, it preserves all rat MSCs morphotypes, and allows for their survival, adhesion to the substrate, and replication. Remarkably, a subpopulation of rat MSCs grown on our PLLA scaffold exhibited formation of membrane protrusions of uncertain significance, although in a size range and morphology compatible with either motility blebs or shedding vesicles. In summary, our PLLA scaffold has no detrimental effect on a number of features of rat MSCs, primarily the expression of CD73 and CD90.
机译:关于生物材料对哺乳动物骨髓来源的成年间充质基质细胞(MSC)表面抗原的影响,目前尚无数据可用。由于聚(L-乳酸)或PLLA广泛用于人体骨骼的组织工程,并且我们正在开发一项逆向工程程序,以利用生物材料对骨骼的血管结构进行原型设计,以在人类和动物模型中进行生物人工重建,因此我们已经研究了多孔,平坦和光滑的PLLA支架对体外生长的大鼠MSCs在没有任何包被,共聚富集和分化刺激的情况下的免疫表型的影响。与塑料对照类似,我们显示我们的PLLA支架不会改变大鼠MSC中某些表面标记的分布。特别地,CD73和CD90在两个不同亚群(小细胞和大细胞)上的维持表达与它们通过专门的附件附着在PLLA支架上以及它们在肌动蛋白中的显着含量一致。此外,我们的PLLA支架有利于中间丝desmin的保留,据信这是未分化状态的公认标记。最后,它保留了所有大鼠MSC的形态,并允许它们存活,粘附于基质和复制。值得注意的是,在我们的PLLA支架上生长的大鼠MSC亚群显示出膜凸出物的形成,具有不确定的意义,尽管其大小范围和形态与运动性小泡或脱落的小泡均相容。总之,我们的PLLA支架对大鼠MSC的许多特征没有有害作用,主要是CD73和CD90的表达。

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  • 来源
    《Journal of materials science 》 |2014年第10期| 2421-2436| 共16页
  • 作者单位

    Department of Biomedical, Biotechnological and Translational Sciences (S.Bi.Bi.T) - Laboratory of Regenerative Morphology and Bioartificial Structures/S.Bi.Bi.T. Museum - Section of Human Anatomy, University of Parma, Parma, Italy,CNR - National Research Council of Italy, IGM, and SC Laboratory of Musculoskeletal Cell Biology, IOR, Bologna, Italy;

    CNR - National Research Council of Italy, IGM, and SC Laboratory of Musculoskeletal Cell Biology, IOR, Bologna, Italy;

    Laboratories of Immunorheumatology and Tissue Regeneration, and RAMSES, IOR, Bologna, Italy;

    Department of Mathematics, University of Bologna, Bologna, Italy;

    Department of Biomedical, Biotechnological and Translational Sciences (S.Bi.Bi.T) - Laboratory of Regenerative Morphology and Bioartificial Structures/S.Bi.Bi.T. Museum - Section of Human Anatomy, University of Parma, Parma, Italy;

    Department of Biomedical, Biotechnological and Translational Sciences (S.Bi.Bi.T) - Laboratory of Regenerative Morphology and Bioartificial Structures/S.Bi.Bi.T. Museum - Section of Human Anatomy, University of Parma, Parma, Italy;

    Department of Biomedical, Biotechnological and Translational Sciences (S.Bi.Bi.T) - Laboratory of Regenerative Morphology and Bioartificial Structures/S.Bi.Bi.T. Museum - Section of Human Anatomy, University of Parma, Parma, Italy;

    ISTEC - CNR, Faenza, Italy;

    Department of Biomedical, Biotechnological and Translational Sciences (S.Bi.Bi.T) - Laboratory of Regenerative Morphology and Bioartificial Structures/S.Bi.Bi.T. Museum - Section of Human Anatomy, University of Parma, Parma, Italy;

    Laboratories of Preclinical and Surgical Studies, and Biocompatibility, Innovative Technologies, and Advanced Therapies (BITTA), Rizzoli Research Innovation Technology (RIT), IOR, Bologna, Italy;

    Laboratories of Preclinical and Surgical Studies, and Biocompatibility, Innovative Technologies, and Advanced Therapies (BITTA), Rizzoli Research Innovation Technology (RIT), IOR, Bologna, Italy;

    Laboratories of Preclinical and Surgical Studies, and Biocompatibility, Innovative Technologies, and Advanced Therapies (BITTA), Rizzoli Research Innovation Technology (RIT), IOR, Bologna, Italy;

    ISTEC - CNR, Faenza, Italy;

    ISTEC - CNR, Faenza, Italy;

    ISTEC - CNR, Faenza, Italy;

    CNR - National Research Council of Italy, IGM, and SC Laboratory of Musculoskeletal Cell Biology, IOR, Bologna, Italy;

    Department of Biomedical, Biotechnological and Translational Sciences (S.Bi.Bi.T) - Laboratory of Regenerative Morphology and Bioartificial Structures/S.Bi.Bi.T. Museum - Section of Human Anatomy, University of Parma, Parma, Italy,Division of Endocrinology Diabetes and Metabolism, Tufts Medical Center - Tufts University School of Medicine, Boston, MA, USA;

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