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Functional studies of a LIM-homeodomain transcription factor lmx1b in murine mid-hindbrain and limb development.

机译:LIM-同源域转录因子lmx1b在小鼠中脑和肢体发育中的功能研究。

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摘要

This thesis is centered on applying molecular genetics to study pattern formation during animal development. More specifically, this thesis describes the functional studies of a LIM-homeodomain gene called lmx1b during murine embryogenesis. Lmx1b expression is restricted to the mid-hindbrain junction as well as to the dorsal mesenchyme of the limb, suggesting important functions during mid-hindbrain and limb development. To test these possibilities, lmx1b homozygous mutant mice were generated and their limb and CNS phenotypes examined. Lmx1b homozygous mutant mice exhibit a large reduction of mid-hindbrain structures, and that their limbs are symmetrical along the dorsal-ventral axis as the result of a dorsal to ventral transformation. Taken together, these studies define essential functions for lmx1b in mid-hindbrain patteming and in dorsal limb cell fate determination. However, the molecular mechanisms which accounts for these phenotypes are unknown, and whether lmx1b has same or distinctive functions during the mid-hindbrain and limb development is also unclear.; Recently, insight into molecular mechanisms of mid-hindbrain patterning and limb development has resulted from the identification of several factors with restricted expression patterns within these regions. These include the secreted factors wnt-1, fgf-8, wnt-7a and the transcription factors pax-2, and en-1. Targeted disruption of any of these genes in mice suggests that these genes might be involved in similar regulatory pathways. Analysis of the expression of these genes in lmx1b mutants demonstrates that lmxlb is not required for the initiation, but is required to maintain their expression at the mid-hindbrain junction. Thus, lmxlb is not required for specifying mid-hindbrain cell fates, rather, it functions to ensure the establishment or maintenance of a proper organizing center at the mid-hindbrain junction. Interestingly, lmxlb functions cell non-autonomously in chimera analysis, which indicates that lmx1b might regulate the expression of secreted factors such as wnt-1 and/or fgf-8 in the organizing center. In contrast, lmx1b functions cell autonomously in the dorsal limb to govern dorsal ventral limb development and its expression is regulated by with wnt-7a and en-1. However, single and double mutant analysis suggest that all three genes have partially overlapping functions as well as independent functions. The results point toward a complicated network of cross-talks among all three limb axes.
机译:本文的重点是应用分子遗传学研究动物发育过程中的模式形成。更具体地说,本论文描述了在小鼠胚胎发生过程中称为lmx1b的LIM同源域基因的功能研究。 Lmx1b的表达被限制在肢体的中枢神经交界处和背侧间充质,提示在中枢神经和肢体发育过程中的重要功能。为了测试这些可能性,生成了lmx1b纯合突变小鼠,并检查了其肢体和CNS表型。 Lmx1b纯合突变小鼠表现出大幅度的中脑后脑结构减少,并且由于背侧向腹侧转化,其四肢沿着背腹轴对称。综上所述,这些研究定义了lmx1b在中脑后区拍打和背肢细胞命运测定中的基本功能。然而,导致这些表型的分子机制尚不清楚,lmx1b在中脑和肢体发育过程中是否具有相同或独特的功能也不清楚。近来,由于鉴定了在这些区域内表达模式受限的几个因素,导致了对中脑后部模式和肢体发育的分子机制的了解。这些包括分泌因子wnt-1,fgf-8,wnt-7a和转录因子pax-2和en-1。这些基因在小鼠中的靶向破坏表明这些基因可能参与了类似的调控途径。对lmx1b突变体中这些基因表达的分析表明,lmxlb并不是启动所必需的,而是维持中后脑交界处其表达所必需的。因此,lmxlb不需要指定中脑干细胞的命运,而是起到确保在中脑干结处建立或维持适当的组织中心的作用。有趣的是,在嵌合体分析中,lmxlb不自主地发挥细胞功能,这表明lmx1b可能调节组织中心中诸如wnt-1和/或fgf-8等分泌因子的表达。相反,lmx1b在背肢中自主发挥功能,以控制背腹肢发育,其表达受wnt-7a和en-1调节。但是,单突变和双突变分析表明,所有三个基因都具有部分重叠的功能以及独立的功能。结果表明,所有三个肢体轴之间都存在复杂的串扰网络。

著录项

  • 作者

    Chen, Haixu.;

  • 作者单位

    The University of Texas Health Science Center at Houston Graduate School of Biomedical Sciences.;

  • 授予单位 The University of Texas Health Science Center at Houston Graduate School of Biomedical Sciences.;
  • 学科 Biology Molecular.; Biology Genetics.
  • 学位 Ph.D.
  • 年度 2000
  • 页码 141 p.
  • 总页数 141
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子遗传学;遗传学;
  • 关键词

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