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Endothelial cells decode VEGF-mediated Ca2+ signaling patterns to produce distinct functional responses

机译:内皮细胞解码VEGF介导的Ca2 +信号传导模式以产生不同的功能反应

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摘要

A single extracellular stimulus can promote diverse behaviors among isogenic cells by differentially regulated signaling networks. We examined Ca2+ signaling in response to VEGF (vascular endothelial growth factor), a growth factor that can stimulate different behaviors in endothelial cells. We found that altering the amount of VEGF signaling in endothelial cells by stimulating them with different VEGF concentrations triggered distinct and mutually exclusive dynamic Ca2+ signaling responses that correlated with different cellular behaviors. These behaviors were cell proliferation involving the transcription factor NFAT (nuclear factor of activated T cells) and cell migration involving MLCK (myosin light chain kinase). Further analysis suggested that this signal decoding was robust to the noisy nature of the signal input. Using probabilistic modeling, we captured both the stochastic and deterministic aspects of Ca2+ signal decoding and accurately predicted cell responses in VEGF gradients, which we used to simulate different amounts of VEGF signaling. Ca2+ signaling patterns associated with proliferation and migration were detected during angiogenesis in developing zebrafish.
机译:单个细胞外刺激可以通过差异调节的信号网络促进等基因细胞之间的多种行为。我们检查了Ca 2 + 信号对VEGF(血管内皮生长因子)的反应,VEGF是一种可以刺激内皮细胞不同行为的生长因子。我们发现,通过以不同的VEGF浓度刺激内皮细胞来改变VEGF信号传导的数量,会触发与细胞行为相关的独特且相互排斥的动态Ca 2 + 信号传导反应。这些行为是涉及转录因子NFAT(活化的T细胞的核因子)的细胞增殖和涉及MLCK(肌球蛋白轻链激酶)的细胞迁移。进一步的分析表明,这种信号解码对于信号输入的噪声性质是鲁棒的。使用概率建模,我们捕获了Ca 2 + 信号解码的随机和确定性方面,并准确地预测了VEGF梯度中的细胞反应,我们用来模拟不同量的VEGF信号传导。在发育中的斑马鱼的血管生成过程中检测到与增殖和迁移相关的Ca 2 + 信号模式。

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