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在不同钠浓度下[3H]苯扎明的摄取。关于钠通透性调节的推论。

Uptake of [3H]benzamil at different sodium concentrations. Inferences regarding the regulation of sodium permeability.

作者信息

Aceves J, Cuthbert A W

出版信息

J Physiol. 1979 Oct;295:491-504. doi: 10.1113/jphysiol.1979.sp012982.

Abstract
  1. The effect of benzamil on short-circuit current in frog skin was measured at different external sodium concentrations. A linear relationship exists between the concentration of benzamil reducing short-circuit current by 50% and the external sodium concentration, indicative of some form of competitive antagonism between sodium and benzamil. 2. Uptake of [3H]benzamil into isolated frog skin epithelium and whole skin (0.95 cm2 pieces) was measured at different external sodium concentrations. With a sodium concentration of 111 mM in the external medium the uptake of [3H]benzamil is linear with concentration. Uptake amounted to 8.8 f-mole nM-1, a value similar to the linear component of the uptake measured at low (1.1 mM) sodium concentration. 3. Using a variety of other conditions the maximal number of specific binding sites for [3H]benzamil was calculated from displaceable binding and the fractional occupancy, the latter being derived from the inhibition of short-circuit current. This approach gave similar binding site densities to those reported previously at low sodium concentrations. 4. The reduction in specific [3H]benzamil uptake at high sodium may result from two mechanisms, competition of sodium with the ligand for an external binding site and a reduction in the site density as the intracellular sodium concentration increases. 5. It is concluded that the saturation of sodium transport which occurs at high sodium concentration is likely a consequence of the reduced availability of entry sites, rather than saturation of the uptake process.
摘要
  1. 在不同的外部钠浓度下测量了苯扎米尔对蛙皮短路电流的影响。使短路电流降低50%的苯扎米尔浓度与外部钠浓度之间存在线性关系,这表明钠与苯扎米尔之间存在某种形式的竞争性拮抗作用。2. 在不同的外部钠浓度下测量了[³H]苯扎米尔在分离的蛙皮上皮和全皮(0.95平方厘米切片)中的摄取情况。当外部介质中的钠浓度为111 mM时,[³H]苯扎米尔的摄取与浓度呈线性关系。摄取量为8.8飞摩尔/纳摩尔,该值与在低(1.1 mM)钠浓度下测量的摄取线性成分相似。3. 使用各种其他条件,根据可置换结合和占据分数计算[³H]苯扎米尔的特异性结合位点的最大数量,后者来自短路电流的抑制。这种方法得到的结合位点密度与先前在低钠浓度下报道的相似。4. 在高钠条件下特异性[³H]苯扎米尔摄取的减少可能由两种机制导致,钠与配体竞争外部结合位点以及随着细胞内钠浓度增加位点密度降低。5. 得出的结论是,在高钠浓度下发生的钠转运饱和可能是进入位点可用性降低的结果,而不是摄取过程的饱和。

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