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首页> 外文期刊>American Journal of Physiology >Functional map of TEA transport activity in isolated rabbit renal proximal tubules.
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Functional map of TEA transport activity in isolated rabbit renal proximal tubules.

机译:分离的兔肾近端小管中TEA转运活性的功能图。

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The organic cation (OC) transporters OCT1 and OCT2 are suspected of mediating substrate entry from the blood into proximal tubule cells as the first step in renal secretion of OCs. We examined the contribution of each process in different rabbit renal proximal tubule (RPT) segments, taking advantage of the fact that rabbit orthologs of OCT1 and OCT2 can be distinguished by the high affinity of the former for tyramine (TYR) and of the latter for cimetidine (CIM). We verified that TEA uptake, for which both transporters share a similar affinity, is relatively constant in all three segments (apparent inhibitory constant of 33, 74, and 30 microM and maximal rate of mediated TEA uptake of 0.8, 1.0, and 1.2 pmol x mm(-1) x min(-1) in S1, S2, and S3, respectively). In the S1 segment, TYR was a more effective inhibitor of TEA uptake than CIM (IC50 values of 39 and 328 microM, respectively), implicating OCT1 as the predominant pathway for TEA transport. The opposite profiles were noted in the S2 segment (IC50 values of 302 and 20 microM for TYR and CIM, respectively) and S3 segment (IC50 values of 2,900 and 54 microM for TYR and CIM, respectively), suggesting that OCT2 is the predominant TEA transporter in the later portion of RPT. TEA sufficient to saturate OCT1 and OCT2 blocked only 37% of mediated amantadine transport in the S2 segment, confirming the functional presence of at least one additional OC transporter (perhaps OCT3). These data indicate that renal OC transport involves the concerted activity of a suite of transport processes.
机译:怀疑有机阳离子(OC)转运蛋白OCT1和OCT2介导底物从血液进入近端小管细胞,这是OCs肾分泌的第一步。我们利用OCT1和OCT2的兔直系同源物可以通过前者对酪胺(TYR)的高亲和力和后者对TYR的高亲和力来区分这一事实,检查了每个过程在不同的兔肾近端小管(RPT)段中的作用。西咪替丁(CIM)。我们验证了两个转运蛋白都具有相似亲和力的TEA吸收在所有三个区段中都相对恒定(表观抑制常数分别为33、74和30 microM,介导的TEA吸收的最大速率为0.8、1.0和1.2 pmol x在S1,S2和S3中分别为mm(-1)x min(-1))。在S1区段中,TYR比CIM(分别为39和328 microM的IC50值)更有效地抑制TEA摄取,暗示OCT1是TEA转运的主要途径。在S2段(TYR和CIM的IC50值分别为302和20 microM)和S3段(TYR和CIM的IC50值分别为2,900和54 microM)中注意到了相反的曲线,这表明OCT2是主要的TEA。 RPT后期的运输工具。足以使OCT1和OCT2饱和的TEA只能阻止S2段中介导的金刚烷胺转运的37%,从而确认至少存在一种额外的OC转运蛋白(也许是OCT3)的功能存在。这些数据表明,肾OC运输涉及一系列运输过程的协调活动。

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