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应激和衰老卵母细胞中 RNP 颗粒的组装需要核孔蛋白,并与核膜起泡相协调。

Assembly of RNP granules in stressed and aging oocytes requires nucleoporins and is coordinated with nuclear membrane blebbing.

机构信息

Central Michigan University, Department of Biology, Mount Pleasant, MI 48859, USA.

出版信息

Dev Biol. 2011 May 15;353(2):173-85. doi: 10.1016/j.ydbio.2011.02.028. Epub 2011 Mar 5.

Abstract

Protective cellular responses to stress and aging in the germline are essential for perpetuation of a species; however, relatively few studies have focused on how germ cells respond to stress and aging. We have previously shown that large ribonucleoprotein (RNP) complexes assemble in oocytes of Caenorhabditis during extended meiotic arrest or after environmental stress. Here we explore the regulation of these dynamic RNPs and demonstrate their assembly is coordinated with dramatic, nuclear membrane blebbing in oocytes. Our ultrastructural analyses reveal distinct changes in the endoplasmic reticulum, and the first evidence for the assembly of stacked annulate lamellae in Caenorhabditis. We further show several nucleoporins are required for the complete assembly of RNP granules, and a disruption in RNP granule assembly coupled with a low frequency of nuclear blebbing in arrested oocytes negatively impacts embryonic viability. Our observations support a model where nuclear membrane blebbing is required to increase the trafficking of nucleoporins to the cell cortex in stressed or meiotically arrested cells and to facilitate the recruitment of RNA and protein components of RNPs into large complexes. These new insights may have general implications for better understanding how germ cells preserve their integrity when fertilization is delayed and how cells respond to stress.

摘要

保护生殖细胞免受应激和衰老的影响对于物种的延续至关重要;然而,很少有研究关注生殖细胞如何应对应激和衰老。我们之前已经表明,在延长减数分裂停滞或环境应激后,大型核糖核蛋白(RNP)复合物会在秀丽隐杆线虫的卵母细胞中组装。在这里,我们探索了这些动态 RNP 的调节,并证明它们的组装与卵母细胞中剧烈的核膜起泡协调一致。我们的超微结构分析揭示了内质网的明显变化,以及在秀丽隐杆线虫中组装堆叠的环层小体的第一个证据。我们进一步表明,几个核孔蛋白对于 RNP 颗粒的完全组装是必需的,而 RNP 颗粒组装的破坏以及停滞卵母细胞中核起泡频率的降低会对胚胎活力产生负面影响。我们的观察结果支持这样一种模型,即核膜起泡是必需的,以增加应激或减数分裂停滞细胞中核孔蛋白向细胞皮质的运输,并促进 RNA 和 RNP 蛋白成分招募到大型复合物中。这些新的见解可能对更好地理解生殖细胞在受精延迟时如何保持其完整性以及细胞如何应对应激具有普遍意义。

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