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巯基试剂对家兔降结肠阳离子通透性的影响

Modification of cation permeability of rabbit descending colon by sulphydryl reagents.

作者信息

Luger A, Turnheim K

出版信息

J Physiol. 1981 Aug;317:49-66. doi: 10.1113/jphysiol.1981.sp013813.

Abstract
  1. Addition of the organic mercurials mersalyl, p-chloromercuribenzoate, and p-chloromercuribenzene sulphonate to the Ringer solution (140 mM-Na) bathing the luminal side of isolated epithelia of rabbit descending colon increases short-circuit current (Isc) and tissue conductance (Gt) when the spontaneous Isc is below 2-3 muequiv/cm2 hr. 2. The stimulation of Isc by mersalyl is due to an increase in Na absorption, simultaneously K secretion is induced, whereas Cl absorption is not affected. 3. Mersalyl inhibits Isc at Na concentrations below 50 mM. The Na concentration at which Isc is half-maximal (KNa) is shifted by mersalyl from 25 to 133 mM. The overshoot in Isc to a peak volume of 5 muequiv/cm2 hr observed when Na-depleted tissues are suddenly exposed to Na is markedly depressed by mersalyl. 4. Mersalyl inhibits non-competitively the blocking effect of amiloride on Isc. Both the stimulation of Isc and the inhibition of the amiloride effect by mersalyl have the same time course (half-time of the effects 30-40 min) and similar concentration-response curve (half-maximal effects with 2.0-2.6 x 10(-4) M), indicating a common mechanism. 5. The mersalyl effects on Isc and on the amiloride action are only partially reversed by dimercaptopropanol. p-Chloromercuribenzoate conjugated with dextran (mol. wt. 10,000) elicited the same effects as mersalyl. 6. The stoichiometry of the mersalyl-amiloride interaction, estimated by use of the Hill plot, is 1:1; a Hill coefficient of 1 was also obtained for the stimulating effect of mersalyl on Isc. 7. It is concluded that one sulphydryl group per luminal Na entry site controls both its Na conductance and cation selectivity. Titration of these sulphydryl groups by organic mercurials appear to fix the conductance of the luminal Na entry mechanism in a submaximal position and prevent its modulation by amiloride or variations in intra- and/or extracellular Na concentrations.
摘要
  1. 当兔降结肠孤立上皮管腔侧浸泡的林格液(140 mM - Na)中添加有机汞制剂汞撒利、对氯汞苯甲酸和对氯汞苯磺酸盐时,若自发短路电流(Isc)低于2 - 3 μeq/cm²·hr,会增加短路电流(Isc)和组织电导(Gt)。2. 汞撒利对Isc的刺激作用是由于钠吸收增加,同时诱导钾分泌,而氯吸收不受影响。3. 在钠浓度低于50 mM时,汞撒利会抑制Isc。汞撒利使Isc达到最大值一半时的钠浓度(KNa)从25 mM变为133 mM。当缺钠组织突然暴露于钠时观察到的Isc超射到峰值5 μeq/cm²·hr的现象会被汞撒利显著抑制。4. 汞撒利非竞争性抑制氨氯地平对Isc的阻断作用。汞撒利对Isc的刺激作用和对氨氯地平作用的抑制具有相同的时间进程(效应半衰期为30 - 40分钟)和相似的浓度 - 反应曲线(半数最大效应浓度为2.0 - 2.6×10⁻⁴ M),表明存在共同机制。5. 二巯丙醇只能部分逆转汞撒利对Isc和氨氯地平作用的影响。与葡聚糖(分子量10,000)结合的对氯汞苯甲酸产生的效应与汞撒利相同。6. 通过希尔图估算,汞撒利 - 氨氯地平相互作用的化学计量比为1:1;汞撒利对Isc的刺激作用也得到了希尔系数为1的结果。7. 得出的结论是,每个管腔钠进入位点的一个巯基控制其钠电导和阳离子选择性。有机汞制剂对这些巯基的滴定似乎将管腔钠进入机制的电导固定在次最大位置,并阻止其被氨氯地平或细胞内和/或细胞外钠浓度变化所调节。

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