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毛细血管壁小分子溶质交换双途径模型的测试。

Test of a two-pathway model for small-solute exchange across the capillary wall.

作者信息

Fu B M, Adamson R H, Curry F E

机构信息

Dept. of Human Physiology, School of Medicine, University of California at Davis, Davis, California 95616, USA.

出版信息

Am J Physiol. 1998 Jun;274(6):H2062-73. doi: 10.1152/ajpheart.1998.274.6.H2062.

Abstract

We previously proposed a two-pathway model for solute and water transport across vascular endothelium (Fu, B. M., R. Tsay, F. E. Curry, and S. Weinbaum. J. Biomech. Eng. 116: 502-513, 1994) that hypothesized the existence of a continuous slit 2 nm wide along tight junction strands within the interendothelial cleft in parallel with 20 x 150-nm breaks in tight junctions. We tested this model by measuring capillary permeability coefficients (P) to a small solute (sodium fluorescein, radius 0.45 nm), assumed to permeate primarily the 2-nm small pore, and an intermediate-sized solute (FITC-alpha-lactalbumin, radius 2.01 nm) excluded from the small pore. Mean values of the paired diffusive permeability coefficients, Psodium fluorescein and PFITC-alpha-lactalbumin, were 34.4 and 2.9 x 10(-6) cm/s, respectively, after corrections for solvent drag and free dye (n = 26). These permeabilities were accounted for by transport through the large-break pathway without the additional capacity of the hypothetical 2-nm pathway. As a further test we examined the relative reductions of Psodium fluorescein and PFITC-alpha-lactalbumin produced by elevated intracellular cAMP. Within 20 min after the introduction of rolipram and forskolin, Psodium fluorescein and PFITC-alpha-lactalbumin decreased to 0.67 and 0.64 times their respective baseline values. These similar responses to permeability decrease were evidence that the two solutes were carried by a common pathway. Combined results in both control and reduced permeability states did not support the hypothesis that a separate pathway across tight junctions is available for solutes with a radius as large as 0.75 nm. If such a pathway is present, then its size must be smaller than that of sodium fluorescein.

摘要

我们之前提出了一个溶质和水跨血管内皮运输的双途径模型(傅,B.M.,R.蔡,F.E.库里,和S.温鲍姆。《生物医学工程杂志》116: 502 - 513,1994),该模型假设在内皮细胞间裂隙内紧密连接链上存在一条2纳米宽的连续缝隙,与紧密连接中20×150纳米的断裂处平行。我们通过测量毛细血管对一种小溶质(荧光素钠,半径0.45纳米)和一种中等大小溶质(异硫氰酸荧光素 - α - 乳白蛋白,半径2.01纳米)的渗透系数(P)来测试这个模型,假设小溶质主要通过2纳米的小孔渗透,而中等大小溶质被排除在小孔之外。在校正溶剂拖曳和游离染料后(n = 26),荧光素钠和异硫氰酸荧光素 - α - 乳白蛋白的成对扩散渗透系数的平均值分别为34.4和2.9×10⁻⁶厘米/秒。这些渗透率是通过大断裂途径的运输来解释的,而无需假设的2纳米途径的额外容量。作为进一步的测试,我们研究了细胞内cAMP升高导致的荧光素钠和异硫氰酸荧光素 - α - 乳白蛋白相对降低的情况。在引入咯利普兰和福斯高林后20分钟内,荧光素钠和异硫氰酸荧光素 - α - 乳白蛋白分别降至各自基线值的0.67和0.64倍。这些对渗透率降低的相似反应证明这两种溶质是通过共同途径运输的。对照和低渗透率状态下的综合结果不支持这样的假设,即对于半径高达0.75纳米的溶质,存在一条独立的跨紧密连接途径。如果存在这样一条途径,那么它的大小必须小于荧光素钠的大小。

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