首页> 外文期刊>Cellular and Molecular Neurobiology >Pre-clinical analysis of changes in intra-cellular biochemistry of glioblastoma multiforme (GBM) cells due to c-Myc silencing.
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Pre-clinical analysis of changes in intra-cellular biochemistry of glioblastoma multiforme (GBM) cells due to c-Myc silencing.

机译:临床前分析多形性胶质母细胞瘤(GBM)细胞由于c-Myc沉默而引起的细胞内生化变化的临床前分析。

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Glioblastoma Multiforme (GBM) is an aggressive form of brain Tumor that has few cures. In this study, we analyze the anti-proliferative effects of a new molecule JQ1 against GBMs induced in Wistar Rats. JQ1 is essentially a Myc inhibitor. c-Myc is also known for altering the biochemistry of a tumor cell. Therefore, the study is intended to analyze certain other oncogenes associated with c-Myc and also the change in cellular biochemistry upon c-Myc inhibition. The quantitative analysis of gene expression gave a co-expressive pattern for all the three genes involved namely; c-Myc, Bcl-2, and Akt. The cellular biochemistry analysis by transmission electron microscopy revealed high glycogen and lipid aggregation in Myc inhibited cells and excessive autophagy. The study demonstrates the role of c-Myc as a central metabolic regulator and Bcl-2 and Akt assisting in extending c-Myc half-life as well as in regulation of autophagy, so as to regulate cell survival on the whole. The study also demonstrates that transient treatment by JQ1 leads to aggressive development of tumor and therefore, accelerating death, emphasizing the importance of dosage fixation, and duration for clinical use in future.
机译:胶质母细胞瘤(GBM)是一种侵袭性的脑肿瘤,几乎无法治愈。在这项研究中,我们分析了新分子JQ1对Wistar大鼠诱导的GBM的抗增殖作用。 JQ1本质上是Myc抑制剂。 c-Myc还因改变肿瘤细胞的生物化学而闻名。因此,该研究旨在分析与c-Myc相关的某些其他致癌基因,以及c-Myc抑制后细胞生物化学的变化。基因表达的定量分析给出了涉及的所有三个基因的共表达模式。 c-Myc,Bcl-2和Akt。通过透射电子显微镜进行的细胞生化分析显示,Myc抑制的细胞中糖原和脂质聚集高,自噬过多。该研究证明了c-Myc作为中央代谢调节剂的作用,Bcl-2和Akt有助于延长c-Myc半衰期以及调节自噬,从而从整体上调节细胞存活。这项研究还表明,JQ1的瞬时治疗会导致肿瘤的侵袭性发展,因此会加速死亡,强调剂量固定的重要性以及未来临床使用的持续时间。

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