Death ligand concentration and the membrane proximal signaling module regulate the type 1/type 2 choice in apoptotic death signaling.

Systems and Synthetic Biology Pub Date : 2014-03-01 Epub Date: 2013-09-19 DOI:10.1007/s11693-013-9124-4
Subhadip Raychaudhuri, Somkanya C Raychaudhuri
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引用次数: 5

Abstract

Apoptotic death pathways are frequently activated by death ligand induction and subsequent activation of the membrane proximal signaling module. Death receptors cluster upon binding to death ligands, leading to formation of a membrane proximal death-inducing-signaling-complex (DISC). In this membrane proximal signalosome, initiator caspases (caspase 8) are processed resulting in activation of both type 1 and type 2 pathways of apoptosis signaling. How the type 1/type 2 choice is made is an important question in the systems biology of apoptosis signaling. In this study, we utilize a Monte Carlo based in silico approach to elucidate the role of membrane proximal signaling module in the type 1/type 2 choice of apoptosis signaling. Our results provide crucial mechanistic insights into the formation of DISC signalosome and caspase 8 activation. Increased concentration of death ligands was shown to correlate with increased type 1 activation. We also study the caspase 6 mediated system level feedback activation of apoptosis signaling and its role in the type 1/type 2 choice. Our results clarify the basis of cell-to-cell stochastic variability in apoptosis activation and ramifications of this issue is further discussed in the context of therapies for cancer and neurodegenerative disorders.

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死亡配体浓度和膜近端信号模块调节凋亡死亡信号的1型/ 2型选择。
凋亡死亡途径经常被死亡配体诱导和随后的膜近端信号模块激活。死亡受体在与死亡配体结合时聚集,导致膜近端死亡诱导信号复合物(DISC)的形成。在这个膜近端信号小体中,引发caspase (caspase 8)被加工,导致1型和2型凋亡信号通路的激活。如何选择1型或2型是凋亡信号系统生物学中的一个重要问题。在这项研究中,我们利用基于蒙特卡罗的方法来阐明膜近端信号模块在细胞凋亡信号的1型/ 2型选择中的作用。我们的研究结果为DISC信号体的形成和caspase 8的激活提供了重要的机制见解。死亡配体浓度的增加与1型活化的增加相关。我们还研究了caspase 6介导的细胞凋亡信号的系统水平反馈激活及其在1/ 2型选择中的作用。我们的研究结果阐明了细胞间细胞凋亡激活的随机变异的基础,并在癌症和神经退行性疾病的治疗背景下进一步讨论了这一问题的后果。
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