首页> 外文期刊>Developmental dynamics: an official publication of the American Association of Anatomists >Genetic inducible fate mapping in mouse: Establishing genetic lineages and defining genetic neuroanatomy in the nervous system.
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Genetic inducible fate mapping in mouse: Establishing genetic lineages and defining genetic neuroanatomy in the nervous system.

机译:小鼠中的遗传诱导命运定位:建立遗传谱系并定义神经系统中的遗传神经解剖结构。

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A fascinating aspect of developmental biology is how organs are assembled in three dimensions over time. Fundamental to understanding organogenesis is the ability to determine when and where specific cell types are generated, the lineage of each cell, and how cells move to reside in their final position. Numerous methods have been developed to mark and follow the fate of cells in various model organisms used by developmental biologists, but most are not readily applicable to mouse embryos in utero because they involve physical marking of cells through injection of tracers. The advent of sophisticated transgenic and gene targeting techniques, combined with the use of site-specific recombinases, has revolutionized fate mapping studies in mouse. Furthermore, using genetic fate mapping to mark cells has opened up the possibility of addressing fundamental questions that cannot be studied with traditional methods of fate mapping in other organisms. Specifically, genetic fate mapping allows both the relationship between embryonic gene expression and cell fate (genetic lineage) to be determined, as well as the link between gene expression domains and anatomy (genetic anatomy) to be established. In this review, we present the ever-evolving development of genetic fate mapping techniques in mouse, especially the recent advance of Genetic Inducible Fate Mapping. We then review recent studies in the nervous system (focusing on the anterior hindbrain) as well as in the limb and with adult stem cells to highlight fundamental developmental processes that can be discovered using genetic fate mapping approaches. We end with a look toward the future at a powerful new approach that combines genetic fate mapping with cellular phenotyping alleles to study cell morphology, physiology, and function using examples from the nervous system.
机译:发育生物学的一个令人着迷的方面是如何随着时间的推移在三个维度上组装器官。了解器官发生的基础是确定何时何地生成特定细胞类型,每个细胞的谱系以及细胞如何移动以驻留在其最终位置的能力。已经开发出许多方法来标记和跟踪发育生物学家使用的各种模型生物中细胞的命运,但是大多数方法都不容易应用于子宫内的小鼠胚胎,因为它们涉及通过注入示踪剂对细胞进行物理标记。复杂的转基因和基因靶向技术的出现,结合位点特异性重组酶的使用,彻底改变了小鼠的命运图谱研究。此外,使用遗传命运图谱标记细胞为解决其他生物无法通过传统的命运图谱方法研究的基本问题提供了可能性。具体而言,遗传命运图谱既可以确定胚胎基因表达与细胞命运(遗传谱系)之间的关系,也可以建立基因表达域与解剖结构(遗传解剖结构)之间的联系。在这篇综述中,我们介绍了小鼠遗传命运图谱技术的不断发展,特别是遗传诱导命运图谱的最新进展。然后,我们回顾了神经系统(侧重于前后脑)以及肢体以及成体干细胞的最新研究,以突出可以通过遗传命运图谱方法发现的基本发育过程。我们以一种强大的新方法来展望未来,该方法结合了遗传结局图谱与细胞表型等位基因,可使用神经系统的实例研究细胞形态,生理学和功能。

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