兔皮质集合管中流量刺激的钾分泌的个体发生:功能和分子方面

Ontogeny of flow-stimulated potassium secretion in rabbit cortical collecting duct: functional and molecular aspects.

作者信息

Woda Craig B, Miyawaki Nobuyuki, Ramalakshmi Santhanam, Ramkumar Mohan, Rojas Raul, Zavilowitz Beth, Kleyman Thomas R, Satlin Lisa M

机构信息

Department of Pediatrics, Mount Sinai School of Medicine, New York, NY 10029, USA.

出版信息

Am J Physiol Renal Physiol. 2003 Oct;285(4):F629-39. doi: 10.1152/ajprenal.00191.2003. Epub 2003 Jun 24.

Abstract

High urinary flow rates stimulate K secretion in the fully differentiated but not neonatal or weanling rabbit cortical collecting duct (CCD). Both small-conductance secretory K and high-conductance Ca2+/stretch-activated maxi-K channels have been identified in the apical membrane of the mature CCD by patch-clamp analysis. We reported that flow-stimulated net K secretion in the adult rabbit CCD is 1) blocked by TEA and charybdotoxin, inhibitors of intermediate- and high-conductance (maxi-K) Ca2+-activated K channels, and 2) associated with increases in net Na absorption and intracellular Ca2+ concentration ([Ca2+]i). The present study examined whether the absence of flow-stimulated K secretion early in life is due to a 1) limited flow-induced rise in net Na absorption and/or [Ca2+]i and/or 2) paucity of apical maxi-K channels. An approximately sixfold increase in tubular fluid flow rate in CCDs isolated from 4-wk-old rabbits and microperfused in vitro led to an increase in net Na absorption and [Ca2+]i, similar in magnitude to the response observed in 6-wk-old tubules, but it failed to generate an increase in net K secretion. By 5 wk of age, there was a small, but significant, flow-stimulated rise in net K secretion that increased further by 6 wk of life. Luminal perfusion with iberiotoxin blocked the flow stimulation of net K secretion in the adult CCD, confirming the identity of the maxi-K channel in this response. Maxi-K channel alpha-subunit message was consistently detected in single CCDs from animals >/=4 wk of age by RT-PCR. Indirect immunofluorescence microscopy using antibodies directed against the alpha-subunit revealed apical labeling of intercalated cells in cryosections from animals >/=5 wk of age; principal cell labeling was generally intracellular and punctate. We speculate that the postnatal appearance of flow-dependent K secretion is determined by the transcriptional/translational regulation of expression of maxi-K channels. Furthermore, our studies suggest a novel function for intercalated cells in mediating flow-stimulated K secretion.

摘要

高尿流率刺激完全分化的兔皮质集合管(CCD)分泌钾,但对新生或断奶兔的皮质集合管无此作用。通过膜片钳分析已在成熟CCD的顶端膜中鉴定出小电导分泌性钾通道和高电导Ca2+/牵张激活的大电导钾通道。我们报道,成年兔CCD中流量刺激的净钾分泌:1)被TEA和美洲商陆毒素阻断,这两种物质是中电导和高电导(大电导钾)Ca2+激活钾通道的抑制剂;2)与净钠吸收增加和细胞内Ca2+浓度([Ca2+]i)升高有关。本研究探讨了生命早期缺乏流量刺激的钾分泌是否是由于:1)流量诱导的净钠吸收和/或[Ca2+]i升高受限,和/或2)顶端大电导钾通道缺乏。从4周龄兔分离并在体外进行微灌注的CCD中,肾小管液流速增加约6倍,导致净钠吸收和[Ca2+]i增加,其幅度与在6周龄肾小管中观察到的反应相似,但未能使净钾分泌增加。到5周龄时,流量刺激使净钾分泌有小幅但显著的增加,到6周龄时进一步增加。用埃博毒素进行管腔灌注可阻断成年CCD中流量对净钾分泌的刺激,证实了该反应中存在大电导钾通道。通过RT-PCR在≥4周龄动物的单个CCD中始终检测到大电导钾通道α亚基的信息。使用针对α亚基的抗体进行间接免疫荧光显微镜检查显示,≥5周龄动物的冷冻切片中闰细胞顶端有标记;主细胞标记通常在细胞内且呈点状。我们推测,出生后流量依赖性钾分泌的出现是由大电导钾通道表达的转录/翻译调控决定的。此外,我们的研究提示闰细胞在介导流量刺激的钾分泌中具有新功能。

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