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Computational insights into Caenorhabditis elegans vulval development.

机译:对秀丽隐杆线虫外阴发育的计算见解。

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Studies of Caenorhabditis elegans vulval development provide a paradigm for pattern formation during animal development. The fates of the six vulval precursor cells are specified by the combined action of an inductive signal that activates the EGF receptor mitogen-activated PK signaling pathway (specifying a primary fate) and a lateral signal mediated by LIN-12/Notch (specifying a secondary fate). Here we use methods devised for the engineering of complex reactive systems to model a biological system. We have chosen the visual formalism of statecharts and use it to formalize Sternberg and Horvitz's 1989 model [Sternberg, P. W. & Horvitz, H. R. (1989) Cell 58, 679-693], which forms the basis for our current understanding of the interaction between these two signaling pathways. The construction and execution of our model suggest that different levels of the inductive signal induce a temporally graded response of the EGF receptor mitogen-activated PK pathway and make explicit the importance of this temporal response. Our model also suggests the existence of an additional mechanism operating during lateral specification that prohibits neighboring vulval precursor cells from assuming the primary fate.
机译:秀丽隐杆线虫外阴发育的研究为动物发育过程中的模式形成提供了范例。六个外阴前体细胞的命运通过激活EGF受体促分裂原激活的PK信号通路(指定主要命运)的诱导信号和LIN-12 / Notch介导的横向信号(指定次要信号)的联合作用来确定。命运)。在这里,我们使用为复杂反应系统工程设计的方法来对生物系统进行建模。我们选择了状态图的视觉形式主义,并将其用于形式化Sternberg和Horvitz的1989年模型[Sternberg,PW&Horvitz,HR(1989)Cell 58,679-693],这构成了我们当前了解这些状态之间相互作用的基础两个信号通路。我们模型的构建和执行表明,不同水平的诱导信号会诱导EGF受体促分裂原激活的PK途径的时间分级响应,并明确了这种时间响应的重要性。我们的模型还表明,存在一种在横向规范期间运行的其他机制,该机制可防止相邻的外阴前体细胞承担主要命运。

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