首页> 美国卫生研究院文献>International Journal of Molecular Sciences >Phenotype and Viability of MLO-Y4 Cells Is Maintained by TGFβ3 in a Serum-Dependent Manner within a 3D-Co-Culture with MG-63 Cells
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Phenotype and Viability of MLO-Y4 Cells Is Maintained by TGFβ3 in a Serum-Dependent Manner within a 3D-Co-Culture with MG-63 Cells

机译:TGFβ3在与MG-63细胞的3D共培养中以血清依赖性方式维持MLO-Y4细胞的表型和活力

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摘要

The osteocyte network inside the bone matrix is of functional importance and osteocyte cell death is a characteristic feature of pathological bone diseases. Osteocytes have emerged as key regulators of bone tissue maintenance, yet maintaining their phenotype during in vitro culture remains challenging. A 3D co-culture system for osteocytes with osteoblasts was recently presented, enabling the determination of more physiological effects of growth factors on cells in vitro. MLO-Y4 cells were embedded within a type I collagen gel and cultured in the presence of surface MG-63 cells. Co-culture was performed in the presence or absence of TGFβ3. Gene expression by quantitative PCR, protein expression by fluorescent immunohistochemistry and cell viability tests were performed. The 3D co-culture induced cell differentiation of MG-63 cells seen by increased type I collagen and osteocalcin mRNA expression. TGFβ3 maintained osteocyte differentiation of MLO-Y4 cells during co-culture as determined by stable E11 and osteocalcin mRNA expression till day 4. Interestingly, most of the effects of TGFβ3 on co-cultured cells were serum-dependent. Also, TGFβ3 reduced cell death of 3D co-cultured MLO-Y4 cells in a serum-dependent manner. This study shows that 3D co-culture upregulates differentiation of MG-63 cells to a more mature osteoblast-like phenotype; while the addition of TGFβ3 maintained the characteristic MLO-Y4 osteocyte-like phenotype and viability in a serum-dependent manner.
机译:骨基质内部的骨细胞网络具有功能重要性,骨细胞死亡是病理性骨疾病的特征。骨细胞已经成为骨组织维持的关键调节剂,但是在体外培养过程中维持其表型仍然具有挑战性。最近介绍了一种用于骨细胞与成骨细胞的3D共培养系统,能够确定生长因子对细胞的更多生理效应。将MLO-Y4细胞包埋在I型胶原凝胶中,并在表面MG-63细胞存在下培养。在存在或不存在TGFβ3的情况下进行共培养。进行定量PCR的基因表达,荧光免疫组织化学的蛋白表达和细胞活力测试。通过增加的I型胶原和骨钙素mRNA表达,可以看出3D共培养诱导了MG-63细胞的细胞分化。根据稳定的E11和骨钙素mRNA的表达,直到第4天,共培养期间TGFβ3仍可维持MLO-Y4细胞的骨细胞分化。有趣的是,TGFβ3对共培养细胞的大多数影响是血清依赖性的。同样,TGFβ3以血清依赖性方式减少了3D共培养的MLO-Y4细胞的细胞死亡。这项研究表明3D共培养可将MG-63细胞的分化上调至更成熟的成骨样细胞表型。 TGFβ3的添加以血清依赖的方式保持了特征性的MLO-Y4骨细胞样表型和生存能力。

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