The bumetanide-resistant part of forskolin-induced anion secretion in rat colon.

Acta physiologica Scandinavica Pub Date : 1998-10-01
G Schultheiss, S Hörger, M Diener
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Abstract

In order to reveal the contribution of the Na(+)-K(+)-2 Cl(-)- cotransporter to forskolin-induced anion secretion, the inhibition of forskolin-stimulated short-circuit current (Isc) by bumetanide, furosemide, azosemide and piretanide was investigated. In the distal colon, all blockers inhibited the forskolin-stimulated Isc with a maximal efficiency of 70%. In contrast, in the proximal colon, bumetanide and furosemide inhibited only about 40% of the forskolin response, whereas piretanide and azosemide were ineffective. A similar result was observed, when Na+ was replaced by impermeant cations suggesting especially in the proximal colon a great part of forskolin-induced anion secretion to be independent of the Na(+)-K(+)-2 Cl(-)-cotransporter. In anion substitution experiments the forskolin-induced increase in Isc was reduced by 70-80%, if either Cl- or HCO3- were omitted from the buffer solution, whereas in the combined absence of both anions the response was nearly suppressed. Measurement of the mucosal alkalinization revealed that forskolin stimulated a HCO3- secretion, which was, however, too weak to explain the bumetanide-insensitive Isc induced by forskolin. Bumetanide inhibited the serosa-to-mucosa flux of Cl- (JsmCl) stimulated by forskolin; an effect, which was strongly enhanced by subsequent administration of the anion exchange inhibitor, SITS. These data suggest that the bumetanide-resistant part of the forskolin-induced Isc is mainly mediated by a basolateral anion exchanger, probably a Cl(-)-HCO3- exchanger, which contributes to forskolin-evoked Cl- secretion, and in addition by a small HCO3- secretion stimulated by the drug.

福斯柯林诱导大鼠结肠阴离子分泌布美他尼耐药部分。
为了揭示Na(+)- k (+)-2 Cl(-)-共转运体对福斯克林诱导的阴离子分泌的贡献,研究了布美他尼、呋塞米、阿唑塞米和吡雷他尼对福斯克林刺激的短路电流(Isc)的抑制作用。在远端结肠,所有阻滞剂抑制福斯克林刺激的Isc的最高效率为70%。相比之下,在近端结肠,布美他尼和呋塞米仅抑制约40%的福斯克林反应,而吡雷他尼和阿唑塞米无效。当Na+被不正常的阳离子取代时,观察到类似的结果,特别是在近端结肠中,福斯克林诱导的阴离子分泌的很大一部分独立于Na(+)- k (+)-2 Cl(-)-共转运体。在阴离子替代实验中,如果从缓冲溶液中省略Cl-或HCO3-,则福斯克林诱导的Isc增加减少了70-80%,而在同时缺少这两种阴离子时,反应几乎被抑制。对粘膜碱化的测量显示,福斯克林刺激了HCO3-的分泌,但这种作用太弱,无法解释福斯克林诱导的布美他尼不敏感的Isc。布美他尼抑制福斯克林刺激的血清到粘膜的Cl- (JsmCl)通量;这一效应被随后的阴离子交换抑制剂(sit)强化。这些数据表明,福斯柯林诱导的Isc中布美他尼耐药部分主要是由一个基底侧阴离子交换剂介导的,可能是一个Cl(-)-HCO3-交换剂,它有助于福斯柯林诱导的Cl-分泌,此外,福斯柯林还能刺激少量HCO3-分泌。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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