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犬肺中带电大分子的间质分布:一种动力学模型。

Interstitial distribution of charged macromolecules in the dog lung: a kinetic model.

作者信息

Parker J C, Miniati M, Pitt R, Taylor A E

出版信息

Ann Biomed Eng. 1987;15(2):157-72. doi: 10.1007/BF02364051.

Abstract

A mathematic model was constructed to investigate conflicting physiologic data concerning the charge effect of continuous capillaries to macromolecules in the lung. We simulated the equilibration kinetics of lactate dehydrogenase (MR 4.2 nM) isozymes LDH 1 (pI = 5.0) and LDH 5 (pI = 7.9) between plasma and lymph using previously measured permeability coefficients, lung tissue distribution volumes (VA) and plasma concentrations (CP) in lung tissue. Our hypothesis is that the fixed anionic charges in interstitium, basement membrane, and cell surfaces determine equilibration rather than charged membrane effects at the capillary barrier, so the same capillary permeability coefficients were used for both isozymes. Capillary filtration rates and protein fluxes were calculated using conventional flux equations. Initial conditions at baseline and increased left atrial pressures (PLA) were those measured in animal studies. Simulated equilibration of isozymes over 30 h in the model at baseline capillary pressures accurately predicted the observed differences in lymph/plasma concentration ratios (CL/CP) between isotopes at 4 h and equilibration of these ratios at 24 h. Quantitative prediction of isozyme CL/CP ratios was also obtained at increased PLA. However, an additional cation selective compartment representing the surface glycocalyx was required to accurately simulate the initial higher transcapillary clearances of cationic LDH 5. Thus experimental data supporting the negative barrier, positive barrier, and no charge barrier hypotheses were accurately reproduced by the model using only the observed differences in interstitial partitioning of isozymes without differences in capillary selectivity.

摘要

构建了一个数学模型,以研究关于肺中连续毛细血管对大分子电荷效应的相互矛盾的生理学数据。我们使用先前测量的通透性系数、肺组织分布容积(VA)和肺组织中的血浆浓度(CP),模拟了乳酸脱氢酶(分子量4.2 nM)同工酶LDH 1(pI = 5.0)和LDH 5(pI = 7.9)在血浆和淋巴之间的平衡动力学。我们的假设是,间质、基底膜和细胞表面的固定阴离子电荷决定平衡,而不是毛细血管屏障处的电荷膜效应,因此两种同工酶使用相同的毛细血管通透性系数。使用传统的通量方程计算毛细血管滤过率和蛋白质通量。基线和左心房压力升高(PLA)时的初始条件是在动物研究中测量的那些条件。在基线毛细血管压力下,模型中同工酶在30小时内的模拟平衡准确预测了4小时时同位素之间观察到的淋巴/血浆浓度比(CL/CP)差异以及24小时时这些比值的平衡。在PLA升高时也获得了同工酶CL/CP比值的定量预测。然而,需要一个额外的代表表面糖萼的阳离子选择性隔室来准确模拟阳离子LDH 5最初较高的跨毛细血管清除率。因此,该模型仅使用同工酶间质分配的观察差异而无毛细血管选择性差异,就准确再现了支持负屏障、正屏障和无电荷屏障假设的实验数据。

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