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基于微西方点阵法的表皮生长因子受体信号转导动力学系统分析。

Systems analysis of EGF receptor signaling dynamics with microwestern arrays.

机构信息

The Ben May Department for Cancer Research and the Institute for Genomics and Systems Biology, The University of Chicago, Chicago, Illinois, USA.

出版信息

Nat Methods. 2010 Feb;7(2):148-55. doi: 10.1038/nmeth.1418. Epub 2010 Jan 24.

Abstract

We describe microwestern arrays, which enable quantitative, sensitive and high-throughput assessment of protein abundance and modifications after electrophoretic separation of microarrayed cell lysates. This method allowed us to measure 91 phosphosites on 67 proteins at six time points after stimulation with five epidermal growth factor (EGF) concentrations in A431 human carcinoma cells. We inferred the connectivities among 15 phosphorylation sites in 10 receptor tyrosine kinases (RTKs) and two sites from Src kinase using Bayesian network modeling and two mutual information-based methods; the three inference methods yielded substantial agreement on the network topology. These results imply multiple distinct RTK coactivation mechanisms and support the notion that small amounts of experimental data collected from phenotypically diverse network states may enable network inference.

摘要

我们描述了微西方阵列,该阵列可在微阵列细胞裂解物电泳分离后,对蛋白质丰度和修饰进行定量、敏感和高通量的评估。该方法使我们能够在 A431 人癌细胞中用五种表皮生长因子 (EGF) 浓度刺激后,在六个时间点测量 67 种蛋白质上的 91 个磷酸化位点。我们使用贝叶斯网络建模和两种基于互信息的方法推断了 10 个受体酪氨酸激酶 (RTK) 和 2 个来自Src 激酶的 15 个磷酸化位点之间的连通性;这三种推断方法在网络拓扑上得出了实质性的一致。这些结果表明存在多种不同的 RTK 共激活机制,并支持这样一种观点,即从表型多样的网络状态中收集少量的实验数据可能可以进行网络推断。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fcb6/2881471/0263c8d75040/nihms-186334-f0001.jpg

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