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指定错误的细胞通过一个活跃的基因导向过程死亡,并且对这种死亡的抑制会导致果蝇中的细胞命运转变。

Mis-specified cells die by an active gene-directed process, and inhibition of this death results in cell fate transformation in Drosophila.

作者信息

Werz Christian, Lee Tom V, Lee Peter L, Lackey Melinda, Bolduc Clare, Stein David S, Bergmann Andreas

机构信息

The University of Texas M.D. Anderson Cancer Center, Department of Biochemistry and Molecular Biology, 1515 Holcombe Boulevard, Unit 1000, Houston, TX 77030, USA.

出版信息

Development. 2005 Dec;132(24):5343-52. doi: 10.1242/dev.02150. Epub 2005 Nov 9.

Abstract

Incorrectly specified or mis-specified cells often undergo cell death or are transformed to adopt a different cell fate during development. The underlying cause for this distinction is largely unknown. In many developmental mutants in Drosophila, large numbers of mis-specified cells die synchronously, providing a convenient model for analysis of this phenomenon. The maternal mutant bicoid is particularly useful model with which to address this issue because its mutant phenotype is a combination of both transformation of tissue (acron to telson) and cell death in the presumptive head and thorax regions. We show that a subset of these mis-specified cells die through an active gene-directed process involving transcriptional upregulation of the cell death inducer hid. Upregulation of hid also occurs in oskar mutants and other segmentation mutants. In hid bicoid double mutants, mis-specified cells in the presumptive head and thorax survive and continue to develop, but they are transformed to adopt a different cell fate. We provide evidence that the terminal torso signaling pathway protects the mis-specified telson tissue in bicoid mutants from hid-induced cell death, whereas mis-specified cells in the head and thorax die, presumably because equivalent survival signals are lacking. These data support a model whereby mis-specification can be tolerated if a survival pathway is provided, resulting in cellular transformation.

摘要

在发育过程中,指定错误或错误指定的细胞通常会经历细胞死亡,或者被转化以采用不同的细胞命运。这种差异的根本原因在很大程度上尚不清楚。在果蝇的许多发育突变体中,大量错误指定的细胞会同步死亡,为分析这一现象提供了一个方便的模型。母体突变体双尾是解决这个问题特别有用的模型,因为它的突变表型是组织转化(触角到尾节)和假定的头部和胸部区域细胞死亡的组合。我们表明,这些错误指定的细胞的一个子集通过一个活跃的基因导向过程死亡,该过程涉及细胞死亡诱导因子hid的转录上调。hid的上调也发生在osk突变体和其他节段突变体中。在hid双尾双突变体中,假定的头部和胸部中错误指定的细胞存活并继续发育,但它们被转化以采用不同的细胞命运。我们提供的证据表明,末端躯干信号通路保护双尾突变体中错误指定的尾节组织免受hid诱导的细胞死亡,而头部和胸部中错误指定的细胞死亡,大概是因为缺乏等效的存活信号。这些数据支持了一个模型,即如果提供了存活途径,错误指定可以被容忍,从而导致细胞转化。

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