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Quantitative insight into models of Hedgehog signal transduction.

机译:刺猬信号转导模型的定量见解。

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The Hedgehog (Hh) signaling pathway is an essential regulator of embryonic development and a key factor in carcinogenesis.(1,2) Hh, a secreted morphogen, activates intracellular signaling events via downstream effector proteins, which translate the signal to regulate target gene transcription.(3,4) In a recent publication, we quantitatively compared two commonly accepted models of Hh signal transduction.(5) Each model requires a different ratio of signaling components to be feasible. Thus, we hypothesized that knowing the steady-state ratio of core signaling components might allow us to distinguish between models. We reported vast differences in the molar concentrations of endogenous effectors of Hh signaling, with Smo present in limiting concentrations.(5) This extra view summarizes the implications of this endogenous ratio in relation to current models of Hh signaling and places our results in the context of recent work describing the involvement of guanine nucleotide binding protein Galphai and Cos2 motility.
机译:刺猬(Hh)信号通路是胚胎发育的重要调节剂,也是致癌作用的关键因素。(1,2)分泌的吗啡肽Hh通过下游效应蛋白激活细胞内信号传导事件,该效应蛋白将信号翻译为调控靶基因转录的信号。 。(3,4)在最近的出版物中,我们定量比较了两个普遍接受的Hh信号转导模型。(5)每个模型需要不同比例的信号传导才可行。因此,我们假设知道核心信令组件的稳态比率可能使我们能够区分模型。我们报道了Hh信号的内源性效应物摩尔浓度的巨大差异,Smo以极限浓度存在。(5)这种额外的观点总结了这种内源比与当前Hh信号模型之间的关系,并将我们的结果放在背景中描述鸟嘌呤核苷酸结合蛋白Galphai和Cos2运动的参与的最新研究。

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