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Evolving gene regulation networks into cellular networks guiding adaptive behavior: an outline how single cells could have evolved into a centralized neurosensory system

机译:将基因调控网络演变为指导适应性行为的细胞网络:概述单细胞如何演变为集中式神经感觉系统

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摘要

Understanding the evolution of the neurosensory system of man, able to reflect on its own origin, is one of the major goals of comparative neurobiology. Details of the origin of neurosensory cells, their aggregation into central nervous systems and associated sensory organs, their localized patterning into remarkably different cell types aggregated into variably sized parts of the central nervous system begin to emerge. Insights at the cellular and molecular level begin to shed some light on the evolution of neurosensory cells, partially covered in this review. Molecular evidence suggests that high mobility group (HMG) proteins of pre-metazoans evolved into the definitive Sox [SRY (sex determining region Y)-box] genes used for neurosensory precursor specification in metazoans. Likewise, pre-metazoan basic helix-loop-helix (bHLH) genes evolved in metazoans into the group A bHLH genes dedicated to neurosensory differentiation in bilaterians. Available evidence suggests that the Sox and bHLH genes evolved a cross-regulatory network able to synchronize expansion of precursor populations and their subsequent differentiation into novel parts of the brain or sensory organs. Molecular evidence suggests metazoans evolved patterning gene networks early and not dedicated to neuronal development. Only later in evolution were these patterning gene networks tied into the increasing complexity of diffusible factors, many of which were already present in pre-metazoans, to drive local patterning events. It appears that the evolving molecular basis of neurosensory cell development may have led, in interaction with differentially expressed patterning genes, to local network modifications guiding unique specializations of neurosensory cells into sensory organs and various areas of the central nervous system.
机译:了解人类的神经感觉系统的进化,能够反思其起源,是比较神经生物学的主要目标之一。有关神经感觉细胞起源,它们聚集到中枢神经系统和相关感觉器官中,它们的局部模式化为聚集到中枢神经系统大小各异的不同细胞类型中的详细信息开始出现。在细胞和分子水平上的见识开始为神经感觉细胞的进化提供一些启示,本篇综述对此进行了部分介绍。分子证据表明,前metazoans的高迁移率族(HMG)蛋白演变成确定的Sox [SRY(性别决定区域Y)-box]基因,用于后生动物的神经感觉前体指标。同样,前metazoan基本螺旋-环-螺旋(bHLH)基因在后生动物中进化成A组bHLH基因,专门用于在双边生物中进行神经感觉分化。现有证据表明,Sox和bHLH基因进化出了一种交叉调节网络,能够使前体种群的扩展及其随后分化为大脑或感觉器官的新部分同步化。分子证据表明,后生动物早期进化了模式基因网络,并不致力于神经元发育。只是在进化的后期,这些模式基因网络才与不断增加的扩散因子的复杂性联系在一起,其中许多因素已经存在于前metazoans中,以驱动局部模式事件。看起来,神经感觉细胞发展的不断发展的分子基础可能与差异表达的模式基因相互作用,导致了局部网络修饰,从而引导神经感觉细胞的独特专业进入感觉器官和中枢神经系统的各个区域。

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