首页> 外文期刊>Development >The Drosophila kinesin-like protein KLP3A is required for proper behavior of male and female pronuclei at fertilization.
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The Drosophila kinesin-like protein KLP3A is required for proper behavior of male and female pronuclei at fertilization.

机译:果蝇驱动蛋白样蛋白KLP3A是受精时男性和女性前核正常行为所必需的。

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摘要

Drosophila melanogaster females homozygous for mutations in the gene encoding the kinesin-like protein KLP3A are sterile (Williams et al., 1995). We have investigated the basis of this sterility. The eggs produced by KLP3A mutant mothers are fertilized by sperm, and female meiosis appears to occur normally. However, the large majority of these embryos arrest their development soon thereafter with a characteristic phenotype. The four nuclei produced by female meiosis associate together in a polar body-like structure, while a bipolar spindle is established around the metaphase-arrested male pronucleus. Thus, the major defect caused by depletion of the KLP3A protein is either in specification of the female pronucleus, or in migration of the male and female pronuclei toward each other. We have also found that the KLP3A protein is located throughout the metaphase spindle during meiosis and the early embryonic mitotic divisions, but later accumulates specifically at the midzone of these same spindles during telophase. The protein is also present on two other microtubule structures: the sperm aster; and the radial, monastral array of microtubules established between the two meiosis II spindles. We discuss these results in light of possible functions of the KLP3A protein in pronuclear specification and migration.
机译:果蝇的果蝇雌性在编码驱动蛋白样蛋白KLP3A的基因中是纯合的(Williams等,1995)。我们已经研究了这种无菌性的基础。由KLP3A突变母亲生产的卵子受精后受精,雌性减数分裂似乎正常发生。然而,这些胚胎中的绝大多数在此后不久便以特征表型停止了它们的发育。雌性减数分裂产生的四个核以极体状结构结合在一起,而双极纺锤体则建立在中期停滞的雄性原核周围。因此,由KLP3A蛋白的消耗引起的主要缺陷在于雌性原核的规格或雄性和雌性原核彼此之间的迁移。我们还发现,KLP3A蛋白在减数分裂和早期胚胎有丝分裂分裂的整个中期纺锤体中定位,但后来在末期特异性地聚集在这些纺锤体的中部区域。该蛋白质还存在于另外两个微管结构上:精子;以及在两个减数分裂II纺锤之间建立的放射状,微通道的微管阵列。我们根据KLP3A蛋白在核前规格和迁移中的可能功能来讨论这些结果。

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