Liu Julia J, Glickman Jonathan N, Masyuk Anatoliy I, Larusso Nicholas F
Division of Gastroenterology, Department of Medicine, University of Alberta Hospital, Edmonton, Alberta, Canada.
J Gastroenterol Hepatol. 2008 Oct;23(10):1596-602. doi: 10.1111/j.1440-1746.2008.05500.x. Epub 2008 Aug 20.
We investigated the dietary and gender influences on the expression and functionality of cholangiocyte bile salt transporters and development of biliary hyperplasia in cholesterol gallstone-susceptible C57L/J and resistant AKR/J mice.
C57L and AKR mice were fed chow, a lithogenic diet, or a cholic acid-containing diet for 14 days. Expression of cholangiocyte bile salt transporter proteins ASBT (SLC10A2), ILBP (FABP6), and MRP3 (ABCC3) were studied by Western blot analysis. Taurocholate uptake studies were performed using microperfusion of isolated bile duct units. The pre- and post-perfusion taurocholate concentrations were analyzed by high performance liquid chromatography. Biliary proliferation in liver sections was scored.
The lithogenic diet induced ductular proliferation in C57L mice. On chow, SLC10A2 and ABCC3 were overexpressed in male and female C57L compared to AKR mice. A lithogenic diet reduced the expressions of FABP6 in both male and female C57L mice, SLC10A2 in female C57L mice, and ABCC3 in male C57L mice. These alterations in transporter expressions were not associated with changes in taurocholate uptake. The lithogenic diet induced biliary hyperplasia and reduced bile salt transporter expressions in C57L mice.
Although bile salt uptake was not increased in the bile duct unit, we speculate that the biliary hyperplasia on the lithogenic diet may lead to an increase in intrahepatic bile salt recycling during cholesterol cholelithogenesis.
我们研究了饮食和性别对胆固醇结石易感的C57L/J小鼠及抗性AKR/J小鼠胆管细胞胆盐转运体表达和功能以及胆管增生发展的影响。
给C57L和AKR小鼠喂食普通饲料、致石性饮食或含胆酸的饮食14天。通过蛋白质免疫印迹分析研究胆管细胞胆盐转运体蛋白ASBT(SLC10A2)、ILBP(FABP6)和MRP3(ABCC3)的表达。使用分离的胆管单位微灌注进行牛磺胆酸盐摄取研究。通过高效液相色谱分析灌注前后的牛磺胆酸盐浓度。对肝脏切片中的胆管增殖进行评分。
致石性饮食诱导C57L小鼠胆管增生。与AKR小鼠相比,在普通饲料喂养下,C57L小鼠的雄性和雌性中SLC10A2和ABCC3均过表达。致石性饮食降低了C57L小鼠雄性和雌性中的FABP6表达、雌性C57L小鼠中的SLC10A2表达以及雄性C57L小鼠中的ABCC3表达。这些转运体表达的改变与牛磺胆酸盐摄取的变化无关。致石性饮食诱导C57L小鼠胆管增生并降低胆盐转运体表达。
尽管胆管单位中的胆盐摄取没有增加,但我们推测致石性饮食引起的胆管增生可能导致胆固醇结石形成过程中肝内胆盐循环增加。