Green Center for Systems Biology, Department of Pharmacology, Simmons Cancer Center, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.
Cell Rep. 2013 May 30;3(5):1607-16. doi: 10.1016/j.celrep.2013.04.009. Epub 2013 May 9.
Neutrophil polarity relies on local, mutual inhibition to segregate incompatible signaling circuits to the leading and trailing edges. Mutual inhibition alone should lead to cells having strong fronts and weak backs or vice versa. However, analysis of cell-to-cell variation in human neutrophils revealed that back polarity remains consistent despite changes in front strength. How is this buffering achieved? Pharmacological perturbations and mathematical modeling revealed a functional role for microtubules in buffering back polarity by mediating positive, long-range crosstalk from front to back; loss of microtubules inhibits buffering and results in anticorrelation between front and back signaling. Furthermore, a systematic, computational search of network topologies found that a long-range, positive front-to-back link is necessary for back buffering. Our studies suggest a design principle that can be employed by polarity networks: short-range mutual inhibition establishes distinct signaling regions, after which directed long-range activation insulates one region from variations in the other.
中性粒细胞的极性依赖于局部的相互抑制,以将不兼容的信号通路分隔到前导和尾随边缘。仅相互抑制应该导致细胞具有强前沿和弱后缘,或者反之亦然。然而,对人类中性粒细胞的细胞间变异性的分析表明,尽管前沿强度发生变化,但后极性仍然保持一致。这种缓冲是如何实现的?药理学扰动和数学建模揭示了微管在缓冲后极性方面的功能作用,通过介导从前到后的正向、长程串扰;微管的缺失抑制了缓冲作用,导致前后信号之间的反相关。此外,对网络拓扑结构的系统、计算搜索发现,长程正向的前后连接对于后缓冲是必要的。我们的研究表明了一种可以被极性网络采用的设计原则:短程相互抑制建立了不同的信号区域,之后定向的长程激活将一个区域与另一个区域的变化隔离开来。