染色体的空间排列决定了二倍体芽殖酵母核仁的融合。

IF 2.7 3区 生物学 Q3 CELL BIOLOGY
Molecular Biology of the Cell Pub Date : 2025-11-01 Epub Date: 2025-09-17 DOI:10.1091/mbc.E25-08-0375
Philipp Girke, Simone Fabian, Leonie Aberle, Wolfgang Seufert
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引用次数: 0

摘要

核仁是一种非膜结合的隔室,在核糖体RNA基因(rDNA)串联阵列周围形成,并为细胞提供核糖体。同一核内的多个核仁聚合,核仁融合被认为主要是由核仁的固有特性引起的。然而,rDNA阵列大多是在染色体背景下,染色体不是随机组织的。染色体的空间排列如何影响核仁融合在很大程度上是未知的。利用荧光显微镜研究了二倍体芽殖酵母的核仁融合。在同源rDNA阵列周围形成的核仁在间期有效融合,但在后期往往个体化。虽然在间期核仁远离纺锤体,但在有丝分裂时它们靠得很近,这表明纺锤体依赖的定位可能影响核仁融合。事实上,诺可唑破坏微管依赖性着丝粒锚定在SPB上,促进了核仁的个别化。相比之下,rDNA粘附在核膜上的损伤几乎没有影响。因此,通过非rdna序列定位染色体有利于核仁融合。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The spatial arrangement of chromosomes determines fusion of nucleoli in diploid budding yeast.

The nucleolus is a nonmembrane-bound compartment that forms around tandem arrays of ribosomal RNA genes and provides the cell with ribosomes. Multiple nucleoli within the same nucleus coalesce, and fusion is thought to result mainly from intrinsic properties of nucleoli. However, ribosomal DNA (rDNA) arrays are mostly in chromosomal context, and chromosomes are not randomly organized. How the spatial arrangement of chromosomes affects nucleolar fusion is largely unknown. Using fluorescence microscopy, we investigated nucleolar fusion in diploid budding yeast. Nucleoli forming around homologous rDNA arrays efficiently fused during interphase but often individualized during late anaphase. Although nucleoli were far from the spindle pole body (SPB) in interphase, they came close during mitosis, suggesting that SPB-dependent positioning may affect nucleolar fusion. Indeed, disruption of microtubule-dependent centromere anchorage to the SPB by nocodazole promoted individualization of nucleoli. In contrast, impairment of rDNA tethering to the nuclear envelope had little or no effect. Hence, chromosome positioning by non-rDNA sequences facilitates nucleolar fusion.

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来源期刊
Molecular Biology of the Cell
Molecular Biology of the Cell 生物-细胞生物学
CiteScore
6.00
自引率
6.10%
发文量
402
审稿时长
2 months
期刊介绍: MBoC publishes research articles that present conceptual advances of broad interest and significance within all areas of cell, molecular, and developmental biology. We welcome manuscripts that describe advances with applications across topics including but not limited to: cell growth and division; nuclear and cytoskeletal processes; membrane trafficking and autophagy; organelle biology; quantitative cell biology; physical cell biology and mechanobiology; cell signaling; stem cell biology and development; cancer biology; cellular immunology and microbial pathogenesis; cellular neurobiology; prokaryotic cell biology; and cell biology of disease.
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