首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >Maelstrom coordinates microtubule organization during Drosophila oogenesis through interaction with components of the MTOC.
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Maelstrom coordinates microtubule organization during Drosophila oogenesis through interaction with components of the MTOC.

机译:Maelstrom通过与MTOC的相互作用来协调果蝇卵子发生过程中的微管组织。

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摘要

The establishment of body axes in multicellular organisms requires accurate control of microtubule polarization. Mutations in Drosophila PIWI-interacting RNA (piRNA) pathway genes often disrupt the axes of the oocyte. This results from the activation of the DNA damage checkpoint factor Checkpoint kinase 2 (Chk2) due to transposon derepression. A piRNA pathway gene, maelstrom (mael), is critical for the establishment of oocyte polarity in the developing egg chamber during Drosophila oogenesis. We show that Mael forms complexes with microtubule-organizing center (MTOC) components, including Centrosomin, Mini spindles, and gammaTubulin. We also show that Mael colocalizes with alphaTubulin and gammaTubulin to centrosomes in dividing cyst cells and follicle cells. MTOC components mislocalize in mael mutant germarium and egg chambers, leading to centrosome migration defects. During oogenesis, the loss of mael affects oocyte determination and induces egg chamber fusion. Finally, we show that the axis specification defects in mael mutants are not suppressed by a mutation in mnk, which encodes a Chk2 homolog. These findings suggest a model in which Mael serves as a platform that nucleates other MTOC components to form a functional MTOC in early oocyte development, which is independent of Chk2 activation and DNA damage signaling.
机译:多细胞生物体轴的建立需要精确控制微管极化。果蝇PIWI相互作用RNA(piRNA)途径基因中的突变通常会破坏卵母细胞的轴。这是由于转座子抑制所致的DNA损伤检查点因子Checkpoint激酶2(Chk2)的激活所致。 piRNA通路基因,漩涡(mael),对于果蝇卵子发生期间在发育中的卵腔中建立卵母细胞极性至关重要。我们显示,Mael与微管组织中心(MTOC)组分形成复合物,包括Centrosomin,Mini Spins和gammaTubulin。我们还显示,Mael与alphaTubulin和gammaTubulin共同定位在分裂囊肿细胞和卵泡细胞的中心体。 MTOC成分在梅尔突变菌和卵室中定位不正确,导致中心体迁移缺陷。在卵子发生过程中,黄液的损失影响卵母细胞的确定并诱导卵室融合。最后,我们表明,mael突变体中的轴规格缺陷不会被编码Chk2同源物的mnk突变所抑制。这些发现提示了一种模型,其中Mael作为平台,在早期卵母细胞发育中使其他MTOC成分成核,从而形成功能性MTOC,该平台独立于Chk2激活和DNA损伤信号传导。

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