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Variable stoichiometry in active ion transport: theoretical analysis of physiological consequences.

机译:活性离子传输中的可变化学计量:生理后果的理论分析。

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摘要

Active ion transport systems with fixed stoichiometry are subject to a thermodynamic limit on the ion concentration gradients that they can generate and maintain, and their net rates of transport must inevitably decrease as this limit is approached. The capability to vary stoichiometry might thus be physiologically advantageous: a shift to lower stoichiometry (fewer ions pumped per reaction cycle) at increasing thermodynamic load could increase the limit on the supportable concentration gradient and could accelerate the rate of transport under high-load conditions. Here we present a theoretical and numerical analysis of this possibility, using the sarcoplasmic reticulum ATP-driven Ca pump as the example. It is easy to introduce alternate pathways into the reaction cycle for this system to shift the stoichiometry (Ca2+/ATP) from the normal value of 2:1 to 1:1, but it cannot be done without simultaneous generation of a pathway for uncoupled leak of Ca2+ across the membrane. This counteracts the advantageous effect of the change in transport stoichiometry and a physiologically useful rate acceleration cannot be obtained. This result is likely to be generally applicable to most active transport systems.
机译:具有固定化学计量比的主动离子传输系统会受到其可以生成和维持的离子浓度梯度的热力学限制,并且随着接近该限制,其净传输速率必定会降低。因此,改变化学计量比的能力在生理上可能是有利的:在热力学负荷增加时转向较低的化学计量比(每个反应周期泵送的离子较少)会增加对可支持的浓度梯度的限制,并可能加快高负荷条件下的传输速率。在这里,我们以肌浆网ATP驱动的Ca泵为例,对这种可能性进行了理论和数值分析。对于该系统而言,很容易在反应周期中引入替代途径,以使化学计量比(Ca2 + / ATP)从正常值2:1变为1:1,但是,如果没有同时产生非耦合泄漏的途径,就无法做到这一点。跨膜的Ca2 +含量。这抵消了运输化学计量变化的有利效果,并且无法获得生理学上有用的速率加速。该结果可能普遍适用于大多数主动运输系统。

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