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Investigation of the role of programmed cell death in pattern formation in the Drosophila embryo.

机译:研究果蝇胚胎中程序性细胞死亡在模式形成中的作用。

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摘要

Pattern formation in Drosophila embryogenesis can be defined as the processes which transform a single-celled, fertilized egg into a multi-tissued larva. An essential element of Drosophila embryonic pattern formation is cell number regulation. Specific numbers of cells are needed to form individual embryonic tissues. Required cell numbers are obtained through a balance of cell division, cell allocation and cell death. Cell division and allocation often result in more than the requisite number of cells in some tissues. Excess cells may be removed by the genetically controlled process of programmed cell death or apoptosis. Although programmed cell death occurs in numerous embryonic Drosophila tissues, its role in abdominal development has not been investigated. We found that cell death is important for normal germband retraction and patterning of epidermal fates in the abdomen. In another set of experiments, regulation was examined in embryos with expansions or compressions of normal cell numbers. An increase in cell removal was observed in expanded regions, as evidenced by a normalization of cell numbers and an increase in apoptosis. However, compressed regions were not as efficient in normalizing cell numbers as seen by defects in tissues derived from condensed regions.;Identifying the mechanisms that specify which cells live or die in a particular tissue is paramount to understanding how regulation occurs in wild-type and mispatterned embryos. A model tissue to study the events which singled-out doomed cells is the embryonic epidermis. Apoptosis is relatively abundant in the epidermis and numerous mutants exist that affect normal patterning of this tissue. In order to facilitate cell death analyses, we developed a procedure to generate spatial and temporal maps of apoptotic cells throughout development. Comparison of cell death maps between wild-type and epidermal mutant embryos revealed that segment polarity genes are essential for viability of rows of cells in the developing embryonic epidermis. The loss of cells in segment polarity mutants may contribute to segment polarity phenotypes. The outcome from this work provides a novel cell death mapping procedure, sheds new light on the role of cell death in embryonic regulation, provides a starting point to understanding the determinants of the cell death fate in the epidermis and demonstrates that apoptosis is essential for normal embryonic abdominal development.
机译:果蝇胚胎发生中的模式形成可以定义为将单细胞受精卵转化为多组织幼虫的过程。果蝇胚胎模式形成的基本要素是细胞数量调节。需要特定数量的细胞来形成单个胚胎组织。通过平衡细胞分裂,细胞分配和细胞死亡获得所需的细胞数。细胞分裂和分配通常会导致某些组织中细胞的数量超出所需数量。多余的细胞可以通过程序控制的细胞死亡或凋亡的遗传控制过程去除。尽管程序性细胞死亡发生在许多胚胎果蝇组织中,但尚未研究其在腹部发育中的作用。我们发现细胞死亡对于正常的生殖带收缩和腹部表皮命运的模式很重要。在另一组实验中,检查了正常细胞数量的膨胀或压缩对胚胎的调节作用。细胞数量的正常化和细胞凋亡的增加证明了在扩大区域中细胞去除的增加。然而,压缩区在标准化细胞数量方面不如从压缩区获得的组织缺陷所见的那样有效。确定特定细胞在特定组织中存活或死亡的机制,对于理解野生型和野生型调控如何发生至关重要。胚胎图案错误。一个模型组织,用于研究那些注定失败的细胞是胚胎表皮的事件。表皮中的细胞凋亡相对丰富,并且存在许多影响该组织正常模式的突变体。为了促进细胞死亡分析,我们开发了一种程序,可在整个发育过程中生成凋亡细胞的时空图。野生型和表皮突变型胚胎之间细胞死亡图的比较表明,区段极性基因对于发育中的胚胎表皮中的成排细胞的活力至关重要。节段极性突变体中细胞的丢失可能有助于节段极性表型。这项工作的结果提供了一种新颖的细胞死亡作图程序,阐明了细胞死亡在胚胎调控中的作用,为了解表皮中细胞死亡命运的决定因素提供了一个起点,并证明了凋亡对于正常人至关重要。胚胎腹部发育。

著录项

  • 作者

    Pazdera, Todd Matthew.;

  • 作者单位

    Carnegie Mellon University.;

  • 授予单位 Carnegie Mellon University.;
  • 学科 Cellular biology.;Animal Physiology.
  • 学位 Ph.D.
  • 年度 1998
  • 页码 235 p.
  • 总页数 235
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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