大鼠肾小管中左旋多巴内向转运的药理学研究。

Studies on the pharmacology of the inward transport of L-DOPA in rat renal tubules.

作者信息

Pinto-do-O P C, Soares-da-Silva P

机构信息

Institute of Pharmacology and Therapeutics, Faculty of Medicine, Porto, Portugal.

出版信息

Br J Pharmacol. 1996 Jun;118(3):741-7. doi: 10.1111/j.1476-5381.1996.tb15462.x.

DOI:10.1111/j.1476-5381.1996.tb15462.x

PMID:8762102

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1909740/

Abstract

The accumulation of L-DOPA in suspensions of renal tubules obtained from male Wistar rats occurred through non-saturable and saturable mechanisms. The kinetics of the saturable component of L-DOPA uptake in renal tubules was as follows: Vmax = 46.3 +/- 2.8 nmol mg-1 protein h-1 and Km = 114.4 (95% confidence limits; 83.8, 156.2) microM (n = 5). The diffusion constant (in nmol-1) of the non-saturable component for the accumulation of L-DOPA was 1.3 (1.1, 1.6; n = 8). 2. The effect of 2,4-dinitrophenol was a marked reduction in the tubular uptake of L-DOPA, with an IC50 value of 12.1 (4.0, 36.9) microM. Cocaine produced a slight (P = 0.08) decrease (22% reduction at 50 microM) in the tubular uptake of L-DOPA. Corticosterone produced a considerable inhibitory effect on the uptake of L-DOPA with an IC50 value of 11.0 (3.6, 33.5) microM. The maximal inhibitory effect of probenecid was a 24% decrease in the uptake of L-DOPA; however, the more selective organic anion transport inhibitor 4,4'-diisothiocyantostilbene-2,2'-disulphonic acid (DIDS) was, found not to affect the tubular uptake of L-DOPA. The organic cation transport inhibitor, cyanine 863, was found to produce a marked decrease in the uptake of L-DOPA (IC50 = 2.02 [1.07, 3.79]). The cyanine derivatives 1,1'-diethyl-2,2'-cyanine (decynium 22) and 1,1'-diethyl-2,4'-cyanine (decynium 24) also potently inhibited L-DOPA uptake with IC50 values (in microM) of 0.63 (0.39, 1.01) and 0.10 (0.08, 0.13), respectively, both compounds were found to be more potent than cyanine 863. 3. The inhibitory effect of decynium 24 (0.2 microM) on the tubular uptake of L-DOPA was dependent on the pH of the incubation medium; at pH = 6.5 the accumulation of L-DOPA was reduced up to 37 +/- 2% of control values, whereas at pH = 7.4 and pH = 8.2 the accumulation of L-DOPA was reduced by 56 +/- 1% and 60 +/- 6%, respectively. Cyanine 863 (2 microM), decynium 22 (1 microM) and decynium 24 (0.2 microM) were found to decrease the Vmax values for the saturable component of L-DOPA uptake without changes in Km values. 4. It is concluded that the tubular uptake of L-DOPA might be promoted through a mechanism which is dependent on the activity of the organic cation transport system.

摘要

从雄性Wistar大鼠获得的肾小管悬浮液中L - DOPA的积累通过非饱和和饱和机制发生。肾小管中L - DOPA摄取的饱和成分动力学如下：Vmax = 46.3±2.8 nmol mg-1蛋白质 h-1，Km = 114.4（95%置信限；83.8，156.2）μM（n = 5）。L - DOPA积累的非饱和成分的扩散常数（以nmol-1计）为1.3（1.1，1.6；n = 8）。2. 2,4 - 二硝基苯酚的作用是显著降低L - DOPA的肾小管摄取，IC50值为12.1（4.0，36.9）μM。可卡因使L - DOPA的肾小管摄取略有（P = 0.08）下降（50μM时降低22%）。皮质酮对L - DOPA的摄取产生相当大的抑制作用，IC50值为11.0（3.6，33.5）μM。丙磺舒的最大抑制作用是使L - DOPA的摄取降低24%；然而，发现更具选择性的有机阴离子转运抑制剂4,4'-二异硫氰基芪 - 2,2'-二磺酸（DIDS）不影响L - DOPA的肾小管摄取。有机阳离子转运抑制剂花青863被发现使L - DOPA的摄取显著降低（IC50 = 2.02 [1.07，3.79]）。花青衍生物1,1'-二乙基 - 2,2'-花青（癸花青22）和1,1'-二乙基 - 2,4'-花青（癸花青24）也强烈抑制L - DOPA摄取，IC50值（以μM计）分别为0.63（0.39，1.01）和0.10（0.08，0.13），发现这两种化合物比花青863更有效。3. 癸花青24（0.2μM）对L - DOPA肾小管摄取的抑制作用取决于孵育介质的pH；在pH = 6.5时，L - DOPA的积累减少至对照值的37±2%，而在pH = 7.4和pH = 8.2时，L - DOPA的积累分别减少56±1%和60±6%。发现花青863（2μM）、癸花青22（1μM）和癸花青24（0.2μM）降低L - DOPA摄取的饱和成分的Vmax值，而Km值不变。4. 得出结论，L - DOPA的肾小管摄取可能通过一种依赖于有机阳离子转运系统活性的机制来促进。