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瘦素调节与吸收和分泌相关的胆囊基因。

Leptin regulates gallbladder genes related to absorption and secretion.

作者信息

Swartz-Basile Deborah A, Lu Debao, Basile David P, Graewin Shannon J, Al-Azzawi Hayder, Kiely James M, Mathur Abhishek, Yancey Kyle, Pitt Henry A

机构信息

Department of Surgery, Indiana University School of Medicine, 535 Barnhill Drive, RT 130D, Indianapolis, IN 46202, USA.

出版信息

Am J Physiol Gastrointest Liver Physiol. 2007 Jul;293(1):G84-90. doi: 10.1152/ajpgi.00389.2006. Epub 2007 Apr 26.

Abstract

Dysregulation of gallbladder ion and water absorption and/or secretion has been linked to cholesterol crystal and gallstone formation. We have recently demonstrated that obese, leptin-deficient (Lep(ob)) mice have enlarged gallbladder volumes and decreased gallbladder contractility and that leptin administration to these mice normalizes gallbladder function. However, the effect of leptin on gallbladder absorption/secretion is not known. Therefore, we sought to determine whether leptin would alter the expression of genes involved in water and ion transport across the gallbladder epithelium. Affymetrix oligonucleotide microarrays representing 39,000 transcripts were used to compare gallbladder gene-expression profiles from 12-wk-old control saline-treated Lep(ob) and from leptin-treated Lep(ob) female mice. Leptin administration to Lep(ob) mice decreased gallbladder volume, bile sodium concentration, and pH. Leptin repletion upregulated the expression of aquaporin 1 water channel by 1.3-fold and downregulated aquaporin 4 by 2.3-fold. A number of genes involved in sodium transport were also influenced by leptin replacement. Epithelial sodium channel-alpha and sodium hydrogen exchangers 1 and 3 were moderately downregulated by 2.0-, 1.6-, and 1.3-fold, respectively. Carbonic anhydrase-IV, which plays a role in the acidification of bile, was upregulated 3.7-fold. In addition, a number of inflammatory cytokines that are known to influence gallbladder epithelial cell absorption and secretion were upregulated. Thus leptin, an adipocyte-derived cytokine involved with satiety and energy balance, influences gallbladder bile volume, sodium, and pH as well as multiple inflammatory cytokine genes and genes related to water, sodium, chloride, and bicarbonate transport.

摘要

胆囊离子和水吸收及/或分泌的失调与胆固醇结晶和胆结石形成有关。我们最近证明,肥胖、缺乏瘦素的(Lep(ob))小鼠胆囊体积增大,胆囊收缩力下降,给这些小鼠注射瘦素可使胆囊功能恢复正常。然而,瘦素对胆囊吸收/分泌的影响尚不清楚。因此,我们试图确定瘦素是否会改变参与胆囊上皮水和离子转运的基因表达。使用代表39000个转录本的Affymetrix寡核苷酸微阵列,比较12周龄对照盐水处理的Lep(ob)雌性小鼠和瘦素处理的Lep(ob)雌性小鼠的胆囊基因表达谱。给Lep(ob)小鼠注射瘦素可降低胆囊体积、胆汁钠浓度和pH值。补充瘦素使水通道蛋白1水通道的表达上调1.3倍,使水通道蛋白4下调2.3倍。一些参与钠转运的基因也受到瘦素替代的影响。上皮钠通道-α以及钠氢交换体1和3分别中度下调2.0倍、1.6倍和1.3倍。在胆汁酸化中起作用的碳酸酐酶-IV上调了3.7倍。此外,一些已知会影响胆囊上皮细胞吸收和分泌的炎性细胞因子也上调了。因此,瘦素作为一种与饱腹感和能量平衡有关的脂肪细胞衍生细胞因子,会影响胆囊胆汁体积、钠和pH值,以及多种炎性细胞因子基因和与水、钠、氯和碳酸氢盐转运相关的基因。

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