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不同的细胞状态决定钙信号反应。

Distinct cellular states determine calcium signaling response.

作者信息

Yao Jason, Pilko Anna, Wollman Roy

机构信息

Departments of Chemistry and Biochemistry, Integrative Biology and Physiology, and Institute for Quantitative and Computational Biosciences (QCB), UCLA, Los Angeles, CA, USA.

Departments of Chemistry and Biochemistry, Integrative Biology and Physiology, and Institute for Quantitative and Computational Biosciences (QCB), UCLA, Los Angeles, CA, USA

出版信息

Mol Syst Biol. 2016 Dec 15;12(12):894. doi: 10.15252/msb.20167137.

Abstract

The heterogeneity in mammalian cells signaling response is largely a result of pre-existing cell-to-cell variability. It is unknown whether cell-to-cell variability rises from biochemical stochastic fluctuations or distinct cellular states. Here, we utilize calcium response to adenosine trisphosphate as a model for investigating the structure of heterogeneity within a population of cells and analyze whether distinct cellular response states coexist. We use a functional definition of cellular state that is based on a mechanistic dynamical systems model of calcium signaling. Using Bayesian parameter inference, we obtain high confidence parameter value distributions for several hundred cells, each fitted individually. Clustering the inferred parameter distributions revealed three major distinct cellular states within the population. The existence of distinct cellular states raises the possibility that the observed variability in response is a result of structured heterogeneity between cells. The inferred parameter distribution predicts, and experiments confirm that variability in IP3R response explains the majority of calcium heterogeneity. Our work shows how mechanistic models and single-cell parameter fitting can uncover hidden population structure and demonstrate the need for parameter inference at the single-cell level.

摘要

哺乳动物细胞信号反应的异质性很大程度上是细胞间预先存在的变异性的结果。细胞间变异性是源于生化随机波动还是不同的细胞状态尚不清楚。在这里,我们利用对三磷酸腺苷的钙反应作为模型来研究细胞群体内异质性的结构,并分析不同的细胞反应状态是否共存。我们使用基于钙信号传导机制动力学系统模型的细胞状态功能定义。通过贝叶斯参数推断,我们获得了数百个细胞各自单独拟合的高置信度参数值分布。对推断出的参数分布进行聚类揭示了群体内三种主要的不同细胞状态。不同细胞状态的存在增加了这样一种可能性,即观察到的反应变异性是细胞间结构化异质性的结果。推断出的参数分布进行了预测,实验证实肌醇三磷酸受体(IP3R)反应的变异性解释了大部分钙异质性。我们的工作展示了机制模型和单细胞参数拟合如何能够揭示隐藏的群体结构,并证明了单细胞水平参数推断的必要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a744/5199124/1bd6d3a014f3/MSB-12-894-g002.jpg

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