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溶剂通过细胞间连接的拖曳作用对大鼠小肠营养物质吸收的贡献。

Contribution of solvent drag through intercellular junctions to absorption of nutrients by the small intestine of the rat.

作者信息

Pappenheimer J R, Reiss K Z

机构信息

Department of Physiology and Biophysics, Harvard Medical School, Boston, Massachusetts.

出版信息

J Membr Biol. 1987;100(2):123-36. doi: 10.1007/BF02209145.

Abstract

The lumen of the small intestine in anesthetized rats was recirculated with 50 ml perfusion fluid containing normal salts, 25 mM glucose and low concentrations of hydrophilic solutes ranging in size from creatinine (mol wt 113) to Inulin (mol wt 5500). Ferrocyanide, a nontoxic, quadrupally charged anion was not absorbed; it could therefore be used as an osmotically active solute with reflection coefficient of 1.0 to adjust rates of fluid absorption, Jv, and to measure the coefficient of osmotic flow, Lp. The clearances from the perfusion fluid of all other test solutes were approximately proportional to Jv. From Lp and rates of clearances as a function of Jv and molecular size we estimate (a) the fraction of fluid absorption which passes paracellularly (approx. 50%), (b) coefficients of solvent drag of various solutes within intercellular junctions, (c) the equivalent pore radius of intercellular junctions (50 A) and their cross sectional area per unit path length (4.3 cm per cm length of intestine). Glucose absorption also varied as a function of Jv. From this relationship and the clearances of inert markers we calculate the rate of active transport of glucose, the amount of glucose carried paracellularly by solvent drag or back-diffusion at any given Jv and luminal glucose concentration and the concentration of glucose in the absorbate. The results indicate that solvent drag through paracellular channels is the principal route for intestinal transport of glucose or amino acids at physiological rates of fluid absorption and concentration. In the absence of luminal glucose the rate of fluid absorption and the clearances of all inert hydrophilic solutes were greatly reduced. It is proposed that Na-coupled transport of organic solutes from lumen to intercellular spaces provides the principal osmotic force for fluid absorption and triggers widening of intercellular junctions, thus promoting bulk absorption of nutrients by solvent drag. Further evidence for regulation of channel width is provided in accompanying papers on changes in electrical impedance and ultrastructure of junctions during Na-coupled solute transport.

摘要

在麻醉大鼠中,用含有生理盐水、25 mM葡萄糖和低浓度亲水性溶质(分子量范围从肌酐(113道尔顿)到菊粉(5500道尔顿))的50 ml灌注液对小肠腔进行再循环。亚铁氰化物是一种无毒的四价阴离子,不被吸收;因此它可以用作反射系数为1.0的渗透活性溶质,以调节液体吸收速率Jv,并测量渗透流系数Lp。所有其他测试溶质从灌注液中的清除率大致与Jv成正比。根据Lp以及清除率与Jv和分子大小的函数关系,我们估计:(a)通过细胞旁途径吸收的液体比例(约50%);(b)细胞间连接内各种溶质的溶剂拖曳系数;(c)细胞间连接的等效孔径半径(50 Å)及其每单位路径长度的横截面积(每厘米肠长度4.3平方厘米)。葡萄糖吸收也随Jv而变化。根据这种关系和惰性标记物的清除率,我们计算出葡萄糖的主动转运速率、在任何给定Jv和管腔葡萄糖浓度下通过溶剂拖曳或反向扩散细胞旁携带的葡萄糖量以及吸收物中葡萄糖的浓度。结果表明,在生理液体吸收速率和浓度下,通过细胞旁通道的溶剂拖曳是葡萄糖或氨基酸肠道转运的主要途径。在没有管腔葡萄糖的情况下,液体吸收速率和所有惰性亲水性溶质的清除率大大降低。有人提出,有机溶质从管腔到细胞间隙的钠偶联转运为液体吸收提供了主要的渗透力,并触发细胞间连接变宽,从而促进营养物质通过溶剂拖曳的大量吸收。关于钠偶联溶质转运过程中连接的电阻抗和超微结构变化的相关论文提供了通道宽度调节的进一步证据。

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