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首页> 外文期刊>American Journal of Physiology >Phosphatidylinositol 3-kinase facilitates bile acid-induced Ca(2+) responses in pancreatic acinar cells.
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Phosphatidylinositol 3-kinase facilitates bile acid-induced Ca(2+) responses in pancreatic acinar cells.

机译:磷脂酰肌醇3-激酶促进胆汁酸诱导胰腺腺泡细胞中的Ca(2+)反应。

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Bile acids are known to induce Ca(2+) signals in pancreatic acinar cells. We have recently shown that phosphatidylinositol 3-kinase (PI3K) regulates changes in free cytosolic Ca(2+) concentration ([Ca(2+)](i)) elicited by CCK by inhibiting sarco(endo)plasmic reticulum Ca(2+)-ATPase (SERCA). The present study sought to determine whether PI3K regulates bile acid-induced [Ca(2+)](i) responses. In pancreatic acinar cells, pharmacological inhibition of PI3K with LY-294002 or wortmannin inhibited [Ca(2+)](i) responses to taurolithocholic acid 3-sulfate (TLC-S) and taurochenodeoxycholate (TCDC). Furthermore, genetic deletion of the PI3K gamma-isoform also decreased [Ca(2+)](i) responses to bile acids. Depletion of CCK-sensitive intracellular Ca(2+) pools or application of caffeine inhibited bile acid-induced [Ca(2+)](i) signals, indicating that bile acids release Ca(2+) from agonist-sensitive endoplasmic reticulum (ER) stores via an inositol (1,4,5)-trisphosphate-dependent mechanism. PI3K inhibitors increasedthe amount of Ca(2+) in intracellular stores during the exposure of acinar cells to bile acids, suggesting that PI3K negatively regulates SERCA-dependent Ca(2+) reloading into the ER. Bile acids inhibited Ca(2+) reloading into ER in permeabilized acinar cells. This effect was augmented by phosphatidylinositol (3,4,5)-trisphosphate (PIP(3)), suggesting that both bile acids and PI3K act synergistically to inhibit SERCA. Furthermore, inhibition of PI3K by LY-294002 completely inhibited trypsinogen activation caused by the bile acid TLC-S. Our results indicate that PI3K and its product, PIP(3), facilitate bile acid-induced [Ca(2+)](i) responses in pancreatic acinar cells through inhibition of SERCA-dependent Ca(2+) reloading into the ER and that bile acid-induced trypsinogen activation is mediated by PI3K. The findings have important implications for the mechanism of acute pancreatitis since [Ca(2+)](i) increases and trypsinogen activation mediate key pathological processes in this disorder.
机译:胆汁酸已知在胰腺腺泡细胞中诱导Ca(2+)信号。我们最近显示,磷脂酰肌醇3-激酶(PI3K)调节CCK通过抑制肌(内)质网Ca(2+)调节游离胞质Ca(2+)浓度([Ca(2 +)](i))的变化。 )-ATPase(SERCA)。本研究试图确定PI3K是否调节胆汁酸诱导的[Ca(2 +)](i)反应。在胰腺腺泡细胞中,用LY-294002或渥曼青霉素对PI3K进行药理学抑制可抑制[Ca(2 +)](i)对牛磺石酸3-硫酸盐(TLC-S)和牛磺去氧胆酸(TCDC)的反应。此外,PI3Kγ亚型的基因删除也降低了[Ca(2 +)](i)对胆汁酸的反应。 CCK敏感细胞内Ca(2+)池的耗尽或咖啡因的应用抑制胆汁酸诱导的[Ca(2 +)](i)信号,表明胆汁酸从激动剂敏感的内质网释放Ca(2+)( ER)通过肌醇(1,4,5)-三磷酸依赖性机制进行存储。 PI3K抑制剂增加了腺泡细胞暴露于胆汁酸的过程中细胞内存储的Ca(2+)的量,表明PI3K负调节SERCA依赖的Ca(2+)重新加载到ER。胆汁酸抑制透化的腺泡细胞中的Ca(2+)重新加载到ER。磷脂酰肌醇(3,4,5)-三磷酸(PIP(3))增强了这种作用,表明胆汁酸和PI3K协同作用来抑制SERCA。此外,LY-294002对PI3K的抑制作用完全抑制了由胆汁酸TLC-S引起的胰蛋白酶原激活。我们的结果表明,PI3K及其产物PIP(3)通过抑制SERCA依赖性Ca(2+)重新加载到ER中,促进胆汁酸诱导的胰腺腺泡细胞中的[Ca(2 +)](i)反应。胆汁酸诱导的胰蛋白酶原激活是由PI3K介导的。该发现对急性胰腺炎的机制具有重要意义,因为[Ca(2 +)](i)增加并且胰蛋白酶原激活介导了该疾病的关键病理过程。

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