Nucleocytoplasmic transport: a thermodynamic mechanism.

Hfsp Journal Pub Date : 2009-01-01 Epub Date: 2009-03-18 DOI:10.2976/1.3080807
Ronen Benjamine Kopito, Michael Elbaum
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引用次数: 31

Abstract

The nuclear pore supports molecular communication between cytoplasm and nucleus in eukaryotic cells. Selective transport of proteins is mediated by soluble receptors, whose regulation by the small GTPase Ran leads to cargo accumulation in, or depletion from, the nucleus, i.e., nuclear import or nuclear export. We consider the operation of this transport system by a combined analytical and experimental approach. Provocative predictions of a simple model were tested using cell-free nuclei reconstituted in Xenopus egg extract, a system well suited to quantitative studies. We found that accumulation capacity is limited, so that introduction of one import cargo leads to egress of another. Clearly, the pore per se does not determine transport directionality. Moreover, different cargo reach a similar ratio of nuclear to cytoplasmic concentration in steady-state. The model shows that this ratio should in fact be independent of the receptor-cargo affinity, though kinetics may be strongly influenced. Numerical conservation of the system components highlights a conflict between the observations and the popular concept of transport cycles. We suggest that chemical partitioning provides a framework to understand the capacity to generate concentration gradients by equilibration of the receptor-cargo intermediary.

核细胞质运输:一种热力学机制。
真核细胞的核孔支持细胞质和细胞核之间的分子通讯。蛋白质的选择性运输是由可溶性受体介导的,其由小GTPase Ran调控,导致货物在细胞核中积累或消耗,即核输入或核输出。我们用分析和实验相结合的方法来考虑这个输运系统的运行。对一个简单模型的挑衅性预测进行了测试,使用在爪蟾卵提取物中重建的无细胞核,这是一个非常适合定量研究的系统。我们发现积累能力是有限的,因此一种进口货物的引入导致另一种进口货物的出口。显然,孔隙本身并不能决定输运方向。此外,不同的货物在稳定状态下达到相似的核与细胞质浓度比。该模型表明,该比率实际上应该独立于受体-货物亲和力,尽管动力学可能受到强烈影响。系统成分的数值守恒突出了观测结果与流行的输运周期概念之间的冲突。我们认为,化学分配提供了一个框架,以了解产生浓度梯度的能力,通过平衡的受体-货物中介。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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Hfsp Journal
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