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前列腺素E2对猪子宫内膜上皮细胞氯分泌的调节

Regulation of chloride secretion across porcine endometrial epithelial cells by prostaglandin E2.

作者信息

Deachapunya C, O'Grady S M

机构信息

Department of Physiology, University of Minnesota, St Paul, MN 55108, USA.

出版信息

J Physiol. 1998 Apr 1;508 ( Pt 1)(Pt 1):31-47. doi: 10.1111/j.1469-7793.1998.031br.x.

Abstract
  1. The objective of this study was to investigate the mechanism of PGE2 regulation of Cl- transport across glandular endometrial cells grown in primary culture. 2. Most of the basal short circuit current (Isc) was inhibited by luminal addition of 5-nitro-2-(3-phenylpropylamino)benzoic acid (NPPB) or glibenclamide, suggesting the presence of a basally active Cl- conductance in the apical membrane. 3. Basolateral addition of 10 microM PGE2 increased Isc by 41 +/- 3 microA. A similar response was observed when cells were treated with 8-(4-chlorophenylthio) adenosine 3',5'-cyclic monophosphate (CPT-cAMP). Pretreatment of monolayers with NPPB and glibenclamide blocked the PGE2 and cAMP-mediated increase in Isc, suggesting that the effects of PGE2 and cAMP were dependent on the activity of an apical NPPB- and glibenclamide-sensitive conductance. 4. Addition of 50 nM antiPGE2 antibody to the basolateral bathing solution decreased basal Isc by 20 % and shifted the threshold response to exogenous PGE2. This result suggests autocrine regulation of electrogenic Cl- transport by PGE2. 5. Experiments with amphotericin B-permeabilized monolayers revealed that the apical PGE2-activated, NPPB- and glibenclamide-sensitive conductance was Cl- dependent and that the current-voltage relationship and anion permeation properties (SCN->Br- > Cl- > I-) were characteristic of the cystic fibrosis transmembrane conductance regulator (CFTR). 6. Cultured porcine endometrial epithelial cells were specifically labelled with an antibody to a peptide sequence within the regulatory domain of CFTR. 7. The effect of PGE2 was blocked by basolateral addition of bumetanide and furosemide at concentrations that are selective for inhibition of Na+-K+-2Cl-cotransport activity. The effect of bumetanide on Isc was Cl- dependent, suggesting a role for the bumetanide-sensitive transport pathway in Cl- secretion. 8. PGE2 and cAMP also activated an outwardly rectifying basolateral K+ channel which presumably sustains the driving force for electrogenic Cl- efflux across the apical membrane. 9. The concentration-conductance and concentration-Isc response relationships for PGE2 showed that basolateral K+ permeability was rate limiting with respect to transepithelial anion secretion and that activation of a basolateral K+ channel by PGE2 was necessary to achieve maximum rates of Cl- secretion.
摘要
  1. 本研究的目的是探讨前列腺素E2(PGE2)对原代培养的腺性子宫内膜细胞跨膜氯离子转运调节的机制。2. 管腔中添加5-硝基-2-(3-苯丙基氨基)苯甲酸(NPPB)或格列本脲可抑制大部分基础短路电流(Isc),提示顶端膜存在基础活性氯离子电导。3. 基底外侧添加10μM PGE2可使Isc增加41±3μA。用8-(4-氯苯硫基)腺苷3',5'-环磷酸(CPT-cAMP)处理细胞时观察到类似反应。用NPPB和格列本脲预处理单层细胞可阻断PGE2和cAMP介导的Isc增加,提示PGE2和cAMP的作用依赖于顶端NPPB和格列本脲敏感电导的活性。4. 向基底外侧浴液中添加50 nM抗PGE2抗体可使基础Isc降低20%,并改变对外源PGE2的阈值反应。该结果提示PGE2对电生性氯离子转运的自分泌调节作用。5. 两性霉素B通透单层细胞的实验表明,顶端PGE2激活的NPPB和格列本脲敏感电导依赖于氯离子,电流-电压关系和阴离子通透特性(SCN->Br->Cl->I-)具有囊性纤维化跨膜电导调节因子(CFTR)的特征。6. 培养的猪子宫内膜上皮细胞用针对CFTR调节域内肽序列的抗体进行特异性标记。7. 基底外侧添加布美他尼和呋塞米可阻断PGE2的作用,其浓度对抑制Na+-K+-2Cl-协同转运活性具有选择性。布美他尼对Isc的作用依赖于氯离子,提示布美他尼敏感转运途径在氯离子分泌中起作用。8. PGE2和cAMP还激活了外向整流性基底外侧钾通道,该通道可能维持了电生性氯离子通过顶端膜外流的驱动力。9. PGE2的浓度-电导和浓度-Isc反应关系表明,基底外侧钾通透性是跨上皮阴离子分泌的限速因素,PGE2激活基底外侧钾通道是实现最大氯离子分泌速率所必需的。

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