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Transmembrane flux and receptor desensitization measured with membrane vesicles. Homogeneity of vesicles investigated by computer simulation.

机译:用膜囊泡测量跨膜通量和受体脱敏。通过计算机模拟研究了囊泡的均质性。

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摘要

The use of membrane vesicles to make quantitative studies of transmembrane transport and exchange processes involves an assumption of homogeneity of the membrane vesicles. In studies of 86Rb+ exchange mediated by acetylcholine receptor from the electric organ of Electrophorus electricus and of 36Cl- exchange mediated by GABA receptor from rat brain, measurements of ion exchange and receptor desensitization precisely followed first order kinetics in support of this assumption. In other measurements a biphasic decay of receptor activity was seen. To elucidate the molecular properties of receptors from such measurements it is important to appreciate what the requirements of vesicle monodispersity are for meaningful results and what the effect of vesicle heterogeneity would be. The experiments were simulated with single vesicle populations with variable defined size distributions as well as with mixtures of different populations of vesicles. The properties of the receptors and their density in the membrane could be varied. Different receptors could be present on the same or different membrane vesicles. The simulated measurements were not very sensitive to size dispersity. A very broad size distribution of a single vesicle population was necessary to give rise to detectable deviations from first order kinetics or errors in the determined kinetic constants. Errors could become significant with mixtures of different vesicle populations, where the dispersity in initial ion exchange rate constant, proportional to the receptor concentration per internal volume, became large. In this case the apparent rate of receptor desensitization would diverge in opposite directions from the input value when measured by two different methods, suggesting an experimental test for such kinetic heterogeneity. A biphasic decrease of receptor activity could not be attributed to vesicle heterogeneity and must be due to desensitization processes with different rates. Significant errors would not arise from the size dispersity apparent in subpopulations of vesicles seen by imaging techniques in membrane preparations.
机译:使用膜囊泡进行跨膜运输和交换过程的定量研究涉及膜囊泡同质性的假设。在对电的电器官的乙酰胆碱受体介导的86Rb +交换和对大鼠脑的GABA受体介导的36Cl-交换的研究中,离子交换和受体脱敏的测量正好遵循一阶动力学来支持这一假设。在其他测量中,发现受体活性双相衰减。为了从此类测量中阐明受体的分子特性,重要的是要了解囊泡单分散性对于有意义的结果的要求以及囊泡异质性的影响。用具有可变的定义的大小分布的单个囊泡种群以及不同囊泡种群的混合物模拟了实验。受体的性质及其在膜中的密度可以改变。不同的受体可以存在于相同或不同的膜囊泡上。模拟的测量结果对尺寸分散度不是很敏感。为了引起与一级动力学的可检测偏差或确定的动力学常数的误差,单个囊泡群体的非常宽的尺寸分布是必要的。在不同囊泡群体的混合物中,误差可能会变得很显着,其中初始离子交换速率常数的分散度与每单位内部体积的受体浓度成比例,因此变得很大。在这种情况下,当通过两种不同的方法进行测量时,受体脱敏的表观速率与输入值的方向相反,这表明对这种动力学异质性进行了实验测试。受体活性的双相下降不能归因于囊泡异质性,必须归因于具有不同速率的脱敏过程。在膜制备中通过成像技术观察到的囊泡亚群中明显的大小分散性不会引起明显的误差。

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