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The molecular architecture of the meiotic spindle is remodeled during metaphase arrest in oocytes

机译:减数分裂纺锤体的分子结构在卵母细胞中期停滞期被重塑

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摘要

Before fertilization, oocytes of most species undergo a long, natural arrest in metaphase. Before this, prometaphase I is also prolonged, due to late stable kinetochore–microtubule attachment. How oocytes stably maintain the dynamic spindle for hours during these periods is poorly understood. Here we report that the bipolar spindle changes its molecular architecture during the long prometaphase/metaphase I in Drosophila melanogaster oocytes. By generating transgenic flies expressing GFP-tagged spindle proteins, we found that 14 of 25 spindle proteins change their distribution in the bipolar spindle. Among them, microtubule cross-linking kinesins, MKlp1/Pavarotti and kinesin-5/Klp61F, accumulate to the spindle equator in late metaphase. We found that the late equator accumulation of MKlp1/Pavarotti is regulated by a mechanism distinct from that in mitosis. While MKlp1/Pavarotti contributes to the control of spindle length, kinesin-5/Klp61F is crucial for maintaining a bipolar spindle during metaphase I arrest. Our study provides novel insight into how oocytes maintain a bipolar spindle during metaphase arrest.
机译:受精前,大多数物种的卵母细胞在中期会经历长时间的自然停滞。在此之前,由于后期稳定的动粒-微管附着,前中期I也被延长。在这些期间,卵母细胞如何稳定地维持动态纺锤达数小时的了解很少。在这里,我们报告双极纺锤体在果蝇黑卵母细胞的长前中期/中期I期间改变其分子结构。通过生成表达GFP标签的纺锤体蛋白的转基因果蝇,我们发现25个纺锤体蛋白中有14个改变了其在双极纺锤体中的分布。其中,微管交联的驱动蛋白,MKlp1 / Pavarotti和驱动蛋白-5 / Klp61F,在中期晚期积累到纺锤状赤道。我们发现,MKlp1 / Pavarotti的赤道后期积累受与有丝分裂不同的机制调控。虽然MKlp1 / Pavarotti有助于控制纺锤体的长度,但kinesin-5 / Klp61F对于在I期中期停搏期间维持双极纺锤体至关重要。我们的研究为卵母细胞在中期停滞期间如何维持双极纺锤体提供了新的见解。

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