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Induction of apoptosis through ER stress and TP53 in MCF-7 cells by the nanoparticle [Gd@C82(OH)22]n: A systems biology study

机译:纳米粒子通过MCF-7细胞中的ER应激和TP53诱导细胞凋亡[GD @ C82(OH)22] N:系统生物学研究

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摘要

The nanoparticle gadolinium endohedral metallofullerenol [Gd@C82(OH)22]n is a new candidate for cancer treatment with low toxicity. However, its anti-cancer mechanisms remain mostly unknown. In this study, we took a systems biology view of the gene expression profiles of human breast cancer cells (MCF-7) and human umbilical vein endothelial cells (ECV304) treated with and without [Gd@C82(OH)22]n, respectively, measured by the Agilent Gene Chip G4112F. To properly analyze these data, we modified a suit of statistical methods we developed. For the first time we applied the sub-sub normalization to Agilent two-color microarrays. Instead of a simple linear regression, we proposed to use a one-knot SPLINE model in the sub-sub normalization to account for nonlinear spatial effects. The parameters estimated by least trimmed squares- and S-estimators show similar normalization results. We made several kinds of inferences by integrating the expression profiles with the bioinformatic knowledge in KEGG pathways, Gene Ontology, JASPAR, and TRANSFAC. In the transcriptional inference, we proposed the BASE2.0 method to infer a transcription factor's up-regulation and down-regulation activities separately. Overall, [Gd@C82(OH)22]n induces more differentiation in MCF-7 cells than in ECV304 cells, particularly in the reduction of protein processing such as protein glucosylation, folding, targeting, exporting, and transporting. Among the KEGG pathways, the ErbB signaling pathway is up-regulated, whereas protein processing in endoplasmic reticulum (ER) is down-regulated. CHOP, a key pro-apoptotic gene downstream of the ER stress pathway, increases to nine folds in MCF-7 cells after treatment. These findings indicate that ER stress may be one important factor that induces apoptosis in MCF-7 cells after [Gd@C82(OH)22]n treatment. The expression profiles of genes associated with ER stress and apoptosis are statistically consistent with other profiles reported in the literature, such as those of HEK293T and MCF-7 cells induced by the miR-23a~27a~24-2 cluster. Furthermore, one of the inferred regulatory mechanisms comprises the apoptosis network centered around TP53, whose effective regulation of apoptosis is somehow reestablished after [Gd@C82(OH)22]n treatment. These results elucidate the application and development of [Gd@C82(OH)22]n and other fullerene derivates.
机译:纳米粒子钆胚乳金属蛋白烯醇[Gd / C82(OH)22] n是癌症治疗的新候选性低毒性。然而,其抗癌机制仍然是未知的。在这项研究中,我们分别采用了一种系统生物学观点,分别使用和不含[GD / C82(OH)22] N的人乳腺癌细胞(MCF-7)和人脐静脉内皮细胞(ECV304)的基因表达谱的系统生物学观点,由Agilent基因芯片G4112F测量。要正确分析这些数据,我们修改了我们开发的统计方法的套装。我们首次将子子归一化应用于Agilent双色微阵列。我们建议在子子归一化中使用单结样条模型来计算非线性空间效应的单结样条模型。由最小修整的方块和S估计估计的参数显示出类似的归一化结果。我们通过将表达谱与Kegg途径,基因本体,贾海普尔和Transfac中的生物信息知识集成了几种推断。在转录推断中,我们提出了基准2.0方法以单独推断转录因子的上调和下调活动。总体而言,[Gd @ C82(OH)22] n在MCF-7细胞中诱导比ECV304细胞更多的分化,特别是在蛋白质加工等蛋白质加工,折叠,靶向,出口和运输等中。在KEGG途径中,ERBB信号通路是上调的,而内质网(ER)中的蛋白质处理被下调。 Chec,ER应激途径下游的关键促凋亡基因,在处理后增加至于MCF-7细胞中的九倍。这些发现表明,ER应激可能是在[Gd @ C82(OH)22] N℃下诱导MCF-7细胞中凋亡的一个重要因素。与ER应激和凋亡相关的基因的表达谱与文献中报告的其他曲线有统计学上一致,例如由MiR-23A〜27A〜24-2簇诱导的HEK293T和MCF-7细胞的其他型材。此外,其中一种推断的调节机制包括围绕TP53为中心的细胞凋亡网络,其有效调节细胞凋亡的调节在[Gd @ C82(OH)22]ñ处理后以某种方式重新建立。这些结果阐明了[Gd @ C82(OH)22] N和其他富勒烯衍生物的应用和开发。

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  • 作者单位

    NCMIS Academy of Mathematics and Systems Science Chinese Academy of Sciences Beijing 100190;

    CAS Key Laboratory for Biomedical Effects of Nanomaterials and Nanosafety National Center for;

    CAS Key Laboratory for Biomedical Effects of Nanomaterials and Nanosafety National Center for;

    NCMIS Academy of Mathematics and Systems Science Chinese Academy of Sciences Beijing 100190;

    NCMIS Academy of Mathematics and Systems Science Chinese Academy of Sciences Beijing 100190;

    CAS Key Laboratory for Biomedical Effects of Nanomaterials and Nanosafety Key Laboratory for;

    NCMIS Academy of Mathematics and Systems Science Chinese Academy of Sciences Beijing 100190;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

    Apoptosis; ER stress; Microarray normalization; Nanoparticle; TP53; Transcriptional inference;

    机译:细胞凋亡;ER应激;微阵列归一化;纳米粒子;TP53;转录推断;

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