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极化上皮细胞中管腔ATP激活氯离子分泌的机制。

Mechanism of luminal ATP activated chloride secretion in a polarized epithelium.

作者信息

Keating N, Dev K, Hynes A C, Quinlan L R

机构信息

Physiology, School of Medicine, National University of Ireland, Galway, University Road, Galway, Ireland.

CÚRAM, Centre for Research in Medical Devices, NUI Galway, University Road, Galway, Ireland.

出版信息

J Physiol Sci. 2019 Jan;69(1):85-95. doi: 10.1007/s12576-018-0623-7. Epub 2018 Jun 14.

Abstract

There are both secretory and absorptive pathways working in tandem to support ionic movement driving fluid secretion across epithelia. The mechanisms exerting control of fluid secretion in the oviduct is yet to be fully determined. This study explored the role of apical or luminal extracellular ATP (ATPe)-stimulated ion transport in an oviduct epithelium model, using the Ussing chamber short-circuit current (Isc) technique. Basal Isc in oviduct epithelium in response to apical ATPe comprises both chloride secretion and sodium absorption and has distinct temporal phases. A rapid transient peak followed by a sustained small increase above baseline. Both phases of the apical ATPe Isc response are sensitive to anion (HCO, Cl) and cation (Na) replacement. Additionally, the role of apical chloride channels, basolateral potassium channels and intracellular calcium in supporting the peak Isc current was confirmed. The role of ATP breakdown to adenosine resulting in the activation of P2 receptors was supported by examining the effects of non-hydrolyzable forms of ATP. A P2YR2 potency profile of ATP = UTP > ADP was generated for the apical membrane, suggesting the involvement of the P2YR2 subtype of purinoceptor. A P2X potency profile of ATP = 2MeSATP > alpha,beta-meATP > BzATP was also generated for the apical membrane. In conclusion, these results provide strong evidence that purinergic activation of apical P2YR2 promotes chloride secretion and is thus an important factor in fluid formation by the oviduct.

摘要

分泌途径和吸收途径协同作用,以支持离子运动,驱动液体通过上皮细胞分泌。输卵管中控制液体分泌的机制尚未完全确定。本研究使用尤斯灌流室短路电流(Isc)技术,在输卵管上皮模型中探讨了顶端或管腔细胞外ATP(ATPe)刺激的离子转运作用。输卵管上皮对顶端ATPe反应的基础Isc包括氯离子分泌和钠离子吸收,且具有不同的时间阶段。先是快速短暂的峰值,随后是在基线之上持续的小幅增加。顶端ATPe Isc反应的两个阶段对阴离子(HCO、Cl)和阳离子(Na)替代均敏感。此外,还证实了顶端氯离子通道、基底外侧钾离子通道和细胞内钙在支持峰值Isc电流中的作用。通过研究不可水解形式的ATP的作用,支持了ATP分解为腺苷从而激活P2受体的作用。为顶端膜生成了ATP = UTP > ADP的P2YR2效价谱,表明嘌呤受体的P2YR2亚型参与其中。也为顶端膜生成了ATP = 2MeSATP > α,β-meATP > BzATP的P2X效价谱。总之,这些结果提供了有力证据,即顶端P2YR2的嘌呤能激活促进氯离子分泌,因此是输卵管液体形成的一个重要因素。

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本文引用的文献

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Small conductance potassium channels drive ATP-activated chloride secretion in the oviduct.
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