首页> 美国卫生研究院文献>Journal of the Royal Society Interface >Secreted receptor-associated bone morphogenetic protein regulators reduce stochastic noise intrinsic to many extracellular morphogen distributions
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Secreted receptor-associated bone morphogenetic protein regulators reduce stochastic noise intrinsic to many extracellular morphogen distributions

机译:受体相关的分泌型骨形态发生蛋白调节剂可减少许多细胞外形态发生素分布固有的随机噪声

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摘要

Morphogens are secreted molecules that specify cell-fate organization in developing tissues. Patterns of gene expression or signalling immediately downstream of many morphogens such as the bone morphogenetic protein (BMP) decapentaplegic (Dpp) are highly reproducible and robust to perturbations. This contrasts starkly with our expectation of a noisy interpretation that would arise out of the experimentally determined low concentration (approximately picomolar) range of Dpp activity, tight receptor binding and very slow kinetic rates. To investigate mechanisms by which the intrinsic noise can be attenuated in Dpp signalling, we focus on a class of secreted proteins that bind to Dpp in the extracellular environment and play an active role in regulating Dpp/receptor interactions. We developed a stochastic model of Dpp signalling in Drosophila melanogaster and used the model to quantify the extent that stochastic fluctuations would lead to errors in spatial patterning and extended the model to investigate how a surface-associated BMP-binding protein (SBP) such as Crossveinless-2 (Cv-2) may buffer out signalling noise. In the presence of SBPs, fluctuations in the level of ligand-bound receptor can be reduced by more than twofold depending on parameter values for the intermediate transition states. Regulation of receptor–ligand interactions by SBPs may also increase the frequency of stochastic fluctuations providing a separation of timescales between high-frequency receptor equilibration and slower morphogen patterning. High-frequency noise generated by SBP regulation is easily attenuated by the intracellular network creating a system that imitates the performance of a simple low-pass filter common in audio and communication applications. Together, these data indicate that one of the benefits of receptor–ligand regulation by secreted non-receptors may be greater reliability of morphogen patterning mechanisms.
机译:形态发生素是一种分泌的分子,可以在发育中的组织中确定细胞命运的组织。基因表达或信号传导模式直接在许多形态发生子的下游,例如骨形态发生蛋白(BMP)去功能化(Dpp),具有很高的再现性,并且对扰动具有鲁棒性。这与我们期望的嘈杂解释形成鲜明对比,这是由实验确定的Dpp活性的低浓度(约皮摩尔)范围,紧密的受体结合和非常慢的动力学速率引起的。为了研究在Dpp信号传导中可以减弱固有噪声的机制,我们集中于一类分泌蛋白,这些蛋白与细胞外环境中的Dpp结合并在调节Dpp /受体相互作用中发挥积极作用。我们开发了果蝇中Dpp信号的随机模型,并使用该模型量化了随机波动将导致空间模式错误的程度,并扩展了该模型以研究与表面相关的BMP结合蛋白(SBP),例如Crossveinless -2(Cv-2)可以缓冲信令噪声。在存在SBP的情况下,取决于中间过渡态的参数值,配体结合受体水平的波动可以减少两倍以上。 SBP对受体-配体相互作用的调节也可能会增加随机波动的频率,从而在高频受体平衡和较慢的形态发生模式之间提供时间尺度上的分离。由SBP调节产生的高频噪声很容易被细胞内网络衰减,从而创建了一个模仿音频和通信应用中常见的简单低通滤波器的性能的系统。总之,这些数据表明,分泌型非受体调节受体-配体的好处之一可能是形态发生子构图机制的更高可靠性。

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