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Sensitivity analysis of programmed cell death and implications for crosstalk phenomena during Tumor Necrosis Factor stimulation

机译:肿瘤坏死因子刺激期间编程细胞死亡的敏感性分析及串扰现象的影响

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Different methods for analyzing the sensitivity of the direct signal transduction pathway of receptor-induced apoptosis to parameter changes are presented. Apoptosis is a form of programmed cell death, removing unwanted cells within multicellular organisms to maintain a proper balance between cell reproduction and death. The results indicate the importance of controlling activated caspases by direct inhibition to prevent apoptosis. A misregulation of IAP molecules, one of the main inhibitors, appears to be especially critical. The results indicate how an increased production of this molecule promotes survival and might promote cancer progression, while a reduced degradation might not, thereby providing insight of potential pharmaceutical relevance and also stimulating experimental verification. The different engineering methods applied, nicely complement each other to provide valuable insight into this important process. Because IAPs, among others, are also an important connection to other signaling pathways, the results will enable a more efficient extension of the current model. This is outlined at the example of Tumor Necrosis Factor induced signaling pathways.
机译:提出了分析受体诱导的凋亡直接信号转导通路对参数变化的直接信号转导通路的敏感性的不同方法。细胞凋亡是一种编程细胞死亡的形式,除去多细胞生物体内的不需要的细胞,以保持细胞繁殖和死亡之间的适当平衡。结果表明通过直接抑制来控制活化的胱天膜酶以防止细胞凋亡的重要性。 IAP分子的误解是主要抑制剂之一,似乎是特别关键的。结果表明,该分子的产量增加促进存活,并且可能促进癌症进展,而降低可能不会,从而提供潜在的药物相关性和刺激实验验证的洞察力。应用的不同工程方法,很好地相互补充,以提供有价值的洞察力。因为IAP等也是与其他信令途径的重要联系,结果将实现当前模型的更有效的扩展。这在肿瘤坏死因子诱导的信号通路的实施例中概述。

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