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麻醉诱导莫能菌素和尼日利亚菌素介导的H⁺/M⁺跨磷脂囊泡膜交换速率增加中的金属离子特异性

Metal ion specificity in anaesthetic induced increase in the rate of monensin and nigericin mediated H+/M+ exchange across phospholipid vesicular membranes.

作者信息

Prabhananda B S, Kombrabail M H

机构信息

Department of Chemical Sciences, Tata Institute of Fundamental Research, Mumbai, India.

出版信息

Indian J Biochem Biophys. 1999 Dec;36(6):415-21.

Abstract

From a study of the decay of the pH difference across vesicular membranes (delta pH) it has been possible to show that H+ and alkali metal ion (M+) concentration gradients across bilayer membranes (which are responsible for driving important biochemical processes) can be selectively perturbed by anaesthetics such as chloroform and benzyl alcohol by combining them with a suitable exchange ionophore. On adding the anaesthetic to the membrane in an environment containing metal ions M+ = K+, the rate of delta pH decay by H+/M+ exchange increases by a larger factor or by a smaller factor (when compared to that in a membrane environment with M+ = Na+) depending on whether the exchange ionophore chosen is monensin or nigericin. A rational explanation of this "metal ion specificity" can be given using the exchange ionophore mediated ion transport scheme in which the equilibrations at the "interfaces" are fast compared to the "translocation equilibration" between the species in the two layers of the membrane. The following three factors are responsible for the observed "specificity": On adding the anaesthetic (i) translocation rate constants increase, (ii) the concentrations of the M+ bound ionophores increase at the expense of H+ bound ionophores. (iii) Under our experimental conditions the rate determining species are the complexes monensin-K (Mon-K) and nigericin-H (Nig-H) for M+ = K+ whereas they are monensin-H (Mon-H) and nigericin-Na (Nig-Na) for M+ = Na+. Possible anaesthetic induced membrane perturbations contributing to the above mentioned changes in the membrane are (A), the loosening of the membrane structure and (B), an associated increase in the membrane hydration (and membrane dielectric constant). An analysis of the consequent changes in the various transport step shows the following: (a), The anaesthetic induced changes in the translocation rates of electrically charged species are not relevant in the explanation of the observed changes in the delta pH decay rates. (b), Changes in the rates of fast equilibria at the interface contribute to changes in KH and KM. (c), A suggestion made in the literature, that a significant interaction between the dipole moment of the monensin-K complex and the membrane slows down its translocation, is not valid. (d), The ability to explain rationally all the delta pH decay data confirms the validity of the transport scheme used. In our experiments delta pH across the vesicular membrane was created by pH jump coming from a temperature jump.

摘要

通过对囊泡膜两侧pH差值(ΔpH)衰减的研究,已经能够表明,通过将氯仿和苄醇等麻醉剂与合适的交换离子载体相结合,可以选择性地扰动双层膜两侧的H⁺和碱金属离子(M⁺)浓度梯度(这是驱动重要生化过程的原因)。在含有金属离子M⁺ = K⁺的环境中,将麻醉剂添加到膜中时,与M⁺ = Na⁺的膜环境相比,H⁺/M⁺交换导致的ΔpH衰减速率增加的倍数更大或更小,这取决于所选择的交换离子载体是莫能菌素还是尼日利亚菌素。利用交换离子载体介导的离子转运方案可以对这种“金属离子特异性”给出合理的解释,在该方案中,与膜两层中物种之间的“易位平衡”相比,“界面”处的平衡很快。观察到的“特异性”由以下三个因素导致:添加麻醉剂后,(i)易位速率常数增加,(ii)与H⁺结合的离子载体浓度降低,M⁺结合的离子载体浓度增加。(iii)在我们的实验条件下,对于M⁺ = K⁺,速率决定物种是莫能菌素 - K(Mon - K)和尼日利亚菌素 - H(Nig - H)复合物,而对于M⁺ = Na⁺,它们是莫能菌素 - H(Mon - H)和尼日利亚菌素 - Na(Nig - Na)。可能导致上述膜变化的麻醉剂诱导的膜扰动是(A)膜结构的松弛和(B)膜水合作用(以及膜介电常数)的相关增加。对各种转运步骤随之而来的变化进行分析表明:(a)麻醉剂诱导的带电物种易位速率变化与观察到的ΔpH衰减速率变化的解释无关。(b)界面处快速平衡速率的变化导致KH和KM的变化。(c)文献中提出的莫能菌素 - K复合物的偶极矩与膜之间存在显著相互作用会减慢其易位的观点是无效的。(d)能够合理解释所有ΔpH衰减数据证实了所使用的转运方案的有效性。在我们的实验中,囊泡膜两侧的ΔpH是由温度跃迁引起的pH跃变产生的。

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