真核细胞中支持ATP浓度梯度的物理条件的估计。

IF 3.2 3区 生物学 Q2 BIOPHYSICS
Rajneesh Kumar, Iain G Johnston
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引用次数: 0

摘要

ATP分子在真核生物(和所有生命)中充当能量货币,为许多基本的细胞过程提供所需的能量。但细胞内ATP浓度存在的空间差异的程度仍不完全清楚。有各种各样的争论认为,ATP扩散太快,无法建立大的梯度,或者ATP的高生产和使用速率(源和汇)即使在快速扩散的情况下也可以支持大的梯度——微观模型和不同具体情况下的详细实验支持这两种情况。在这里,我们尝试进行介观研究,在细胞的简单生物物理图像中使用反应扩散模型,试图询问,通常,哪些条件会导致真核细胞内出现实质性的ATP梯度。如果ATP源(如线粒体)或汇(如细胞核)在空间上聚集,则整个细胞的浓度会发生大的折叠变化;如果源和汇分布更广,那么快速扩散确实会阻止大梯度的建立。这种依赖性存在于不同大小的模型细胞中,表明它在细胞类型之间具有普遍性。我们的理论工作将补充研究真核细胞内ATP浓度的细胞内方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Estimating physical conditions supporting gradients of ATP concentration in the eukaryotic cell.

The ATP molecule serves as an energy currency in eukaryotes (and all life), providing the energy needed for many essential cellular processes. But the extent to which substantial spatial differences exist in ATP concentration in the cell remains incompletely known. It is variously argued that ATP diffuses too quickly for large gradients to be established, or that the high rates of ATP production and use (sources and sinks) can support large gradients even with rapid diffusion-and microscopic models and detailed experiments in different specific cases support both pictures. Here, we attempt a mesoscopic investigation, using reaction-diffusion modeling in a simple biophysical picture of the cell to attempt to ask, generally, which conditions cause substantial ATP gradients to emerge within eukaryotic cells. If ATP sources (like mitochondria) or sinks (like the nucleus) are spatially clustered, large fold changes in concentration can exist across the cell; if sources and sinks are more spread, then rapid diffusion indeed prevents large gradients from being established. This dependence holds in model cells of different sizes, suggesting its generality across cell types. Our theoretical work will complement developing intracellular approaches exploring ATP concentration inside eukaryotic cells.

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来源期刊
Biophysical journal
Biophysical journal 生物-生物物理
CiteScore
6.10
自引率
5.90%
发文量
3090
审稿时长
2 months
期刊介绍: BJ publishes original articles, letters, and perspectives on important problems in modern biophysics. The papers should be written so as to be of interest to a broad community of biophysicists. BJ welcomes experimental studies that employ quantitative physical approaches for the study of biological systems, including or spanning scales from molecule to whole organism. Experimental studies of a purely descriptive or phenomenological nature, with no theoretical or mechanistic underpinning, are not appropriate for publication in BJ. Theoretical studies should offer new insights into the understanding ofexperimental results or suggest new experimentally testable hypotheses. Articles reporting significant methodological or technological advances, which have potential to open new areas of biophysical investigation, are also suitable for publication in BJ. Papers describing improvements in accuracy or speed of existing methods or extra detail within methods described previously are not suitable for BJ.
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