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细胞周期中细胞内密度的变化源于裂殖酵母尖端生长的调节。

Variations of intracellular density during the cell cycle arise from tip-growth regulation in fission yeast.

机构信息

Department of Cell and Tissue Biology, University of California, San Francisco, San Francisco, United States.

Department of Bioengineering, Stanford University, Stanford, United States.

出版信息

Elife. 2021 Jun 8;10:e64901. doi: 10.7554/eLife.64901.

Abstract

Intracellular density impacts the physical nature of the cytoplasm and can globally affect cellular processes, yet density regulation remains poorly understood. Here, using a new quantitative phase imaging method, we determined that dry-mass density in fission yeast is maintained in a narrow distribution and exhibits homeostatic behavior. However, density varied during the cell cycle, decreasing during G2, increasing in mitosis and cytokinesis, and dropping rapidly at cell birth. These density variations were explained by a constant rate of biomass synthesis, coupled to slowdown of volume growth during cell division and rapid expansion post-cytokinesis. Arrest at specific cell-cycle stages exacerbated density changes. Spatially heterogeneous patterns of density suggested links between density regulation, tip growth, and intracellular osmotic pressure. Our results demonstrate that systematic density variations during the cell cycle are predominantly due to modulation of volume expansion, and reveal functional consequences of density gradients and cell-cycle arrests.

摘要

细胞内密度会影响细胞质的物理性质,并可能会对细胞过程产生全局性影响,但目前人们对其调控机制仍知之甚少。在这里,我们使用一种新的定量相位成像方法发现,裂殖酵母的干物质密度保持在较窄的分布范围内,并表现出自身稳态行为。然而,密度在细胞周期中会发生变化,在 G2 期下降,在有丝分裂和胞质分裂过程中增加,并在细胞分裂后迅速下降。这些密度变化可以通过恒定的生物量合成率来解释,这种合成率与细胞分裂过程中体积生长速度的减慢以及胞质分裂后快速扩张有关。在特定的细胞周期阶段的停滞会加剧密度变化。密度的空间异质性模式表明,密度调节与尖端生长和细胞内渗透压之间存在联系。我们的研究结果表明,细胞周期过程中的系统性密度变化主要是由于体积扩张的调节所致,并揭示了密度梯度和细胞周期停滞的功能后果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/625e/8221806/8f460a2adc23/elife-64901-fig1.jpg

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