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首页> 外文期刊>Cell death & disease. >Differentiation of human neuroblastoma cells toward the osteogenic lineage by mTOR inhibitor
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Differentiation of human neuroblastoma cells toward the osteogenic lineage by mTOR inhibitor

机译:mTOR抑制剂使人神经母细胞瘤细胞向成骨细胞分化

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摘要

Current hypothesis suggest that tumors can originate from adult cells after a process of 'reprogramming' driven by genetic and epigenetic alterations. These cancer cells, called cancer stem cells (CSCs), are responsible for the tumor growth and metastases. To date, the research effort has been directed to the identification, isolation and manipulation of this cell population. Independently of whether tumors were triggered by a reprogramming of gene expression or seeded by stem cells, their energetic metabolism is altered compared with a normal cell, resulting in a high aerobic glycolytic 'Warburg' phenotype and dysregulation of mitochondrial activity. This metabolic alteration is intricately linked to cancer progression.The aim of this work has been to demonstrate the possibility of differentiating a neoplastic cell toward different germ layer lineages, by evaluating the morphological, metabolic and functional changes occurring in this process. The cellular differentiation reported in this study brings to different conclusions from those present in the current literature. We demonstrate that ' in vitro ' neuroblastoma cancer cells (chosen as experimental model) are able to differentiate directly into osteoblastic (by rapamycin, an mTOR inhibitor) and hepatic lineage without an intermediate 'stem' cell step. This process seems owing to a synergy among few master molecules, metabolic changes and scaffold presence acting in a concerted way to control the cell fate.
机译:当前的假设表明,在遗传和表观遗传学改变驱动的“重编程”过程之后,肿瘤可能起源于成年细胞。这些癌细胞称为癌症干细胞(CSC),负责肿瘤的生长和转移。迄今为止,研究工作一直致力于鉴定,分离和操纵该细胞群。不管肿瘤是由基因表达的重新编程引发还是由干细胞播种,与正常细胞相比,它们的能量代谢都会发生改变,从而导致高需氧糖酵解“ Warburg”表型和线粒体活性失调。这种代谢改变与癌症的发展有着千丝万缕的联系。这项工作的目的是通过评估在此过程中发生的形态,代谢和功能变化,来证明使肿瘤细胞向不同的细菌层谱系分化的可能性。这项研究报告的细胞分化与当前文献中得出的结论不同。我们证明“体外”神经母细胞瘤癌细胞(被选为实验模型)能够直接分化为成骨细胞(通过雷帕霉素,mTOR抑制剂)和肝谱系,而无需中间的“干”细胞步骤。该过程似乎归因于少数主要分子之间的协同作用,代谢变化和支架的存在以协同方式控制细胞命运。

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