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胆管结扎后大鼠胆管细胞中液泡H⁺-ATP酶和钠/氢交换体3的差异调节

Differential regulation of vacuolar H+ -ATPase and Na+/H+ exchanger 3 in rat cholangiocytes after bile duct ligation.

作者信息

Roussa Eleni, Bertram Jasmin, Berge Knut Erik, Labori Knut Jørgen, Thévenod Frank, Raeder Morten G

机构信息

Department of Neuroanatomy, Center for Anatomy, University of Göttingen, Kreuzbergring 36, 37075, Göttingen, Germany.

出版信息

Histochem Cell Biol. 2006 Apr;125(4):419-28. doi: 10.1007/s00418-005-0082-0. Epub 2005 Nov 3.

Abstract

The cholangiocytes lining the intrahepatic bile ducts modify the primary secretion from the hepatocytes. The cholangiocytes secrete HCO (3)(-) into bile when stimulated with secretin in many species, including man. However, in rats, secretin stimulation neither affects biliary HCO (3)(-) concentration nor bile flow, whereas following bile duct ligation (BDL) it induces hypercholeresis with significant increase of NaHCO(3) concentration. We hypothesized that BDL might affect the expression of cholangiocyte H(+) transporters and thereby choleresis, and determined the expression and localization of the 31 kDa vacuolar type H(+)-ATPase (V-ATPase) subunit and of Na(+)/H(+) exchanger NHE3 in the livers of control and BDL rats by real-time PCR, in situ hybridization, immunoblotting, and immunohistochemistry. In controls, secretin had no effect on bile flow, whereas following BDL, secretin increased bile flow approximately threefold. V-ATPase and NHE3 were expressed in control cholangiocytes showing intracellular and apical distribution, respectively. BDL significantly up-regulated V-ATPase mRNA and protein expression and was associated with redistribution to the apical pole in approximately 60% of the cholangiocytes lining the small bile ductules. In contrast, NHE3 expression was significantly down-regulated by BDL at the mRNA and protein level. The data demonstrate expression of V-ATPase in rat cholangiocytes. BDL-induced down-regulation of NHE3 may contribute to a reduction of Na(+) and HCO (3)(-) reabsorption and thus to their net secretion into bile. Apical localization of V-ATPase in cholangiocytes may indicate its involvement in pH regulation and/or HCO (3)(-) salvage to compensate for NHE3 down-regulation in BDL.

摘要

肝内胆管内衬的胆管细胞会改变肝细胞的初始分泌。在包括人类在内的许多物种中,胆管细胞在受到促胰液素刺激时会向胆汁中分泌HCO₃⁻。然而,在大鼠中,促胰液素刺激既不影响胆汁中HCO₃⁻的浓度,也不影响胆汁流量,而在胆管结扎(BDL)后,它会诱导胆汁分泌过多,同时NaHCO₃浓度显著增加。我们推测BDL可能会影响胆管细胞H⁺转运体的表达,进而影响胆汁分泌,并通过实时PCR、原位杂交、免疫印迹和免疫组织化学方法,确定了对照大鼠和BDL大鼠肝脏中31 kDa液泡型H⁺ - ATP酶(V - ATP酶)亚基和Na⁺/H⁺交换体NHE3的表达及定位。在对照大鼠中,促胰液素对胆汁流量没有影响,而在BDL后,促胰液素使胆汁流量增加了约三倍。V - ATP酶和NHE3分别在对照胆管细胞中表达,呈现细胞内和顶端分布。BDL显著上调了V - ATP酶的mRNA和蛋白质表达,并与约60%的小胆管内衬胆管细胞顶端极的重新分布有关。相比之下,BDL在mRNA和蛋白质水平上显著下调了NHE3的表达。数据表明V - ATP酶在大鼠胆管细胞中表达。BDL诱导的NHE3下调可能导致Na⁺和HCO₃⁻重吸收减少,从而导致它们向胆汁中的净分泌增加。胆管细胞中V - ATP酶的顶端定位可能表明其参与pH调节和/或HCO₃⁻回收,以补偿BDL中NHE3的下调。

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