Mühlfeld Anja, Kubitz Ralf, Dransfeld Olaf, Häussinger Dieter, Wettstein Matthias
Clinic for Gastroenterology, Hepatology and Infectiology, Universitätsklinikum Düsseldorf, Moorenstrasse 5, Germany.
Arch Biochem Biophys. 2003 May 1;413(1):32-40. doi: 10.1016/s0003-9861(03)00098-5.
The effect of oral taurine supplementation on endotoxin-induced cholestasis was investigated in rat liver. At 12h following lipopolysaccharide (LPS) injection (4mg/kg body weight i.p.) bile flow and bromosulfophthalein (BSP) and taurocholate (TC) excretion were determined in the perfused liver and the expression of the canalicular transporters multidrug resistance protein 2 (Mrp2) and bile salt export pump (Bsep) was analyzed. Injection of LPS induced a significant decrease of bile flow ( 2.2+/-0.2 microl/g liver wet weight/min vs 3.3+/-0.1 microl/g liver wet weight in controls), biliary BSP excretion (10.8+/-2.2 nmol/g/min vs 21.0+/-3.8 nmol/g/min), and biliary TC excretion (114+/-23 nmol/g/min vs 228+/-8 nmol/g/min). These effects were due to transporter retrieval from the canalicular membrane and downregulation of Mrp2 and Bsep expression. In taurine-supplemented rats bile flow was 30% higher than that in untreated rats and the expression of Mrp2 and Bsep protein was increased two- to threefold. In taurine-supplemented rats there was no significant reduction of bile flow or of BSP and TC excretion at 12h following LPS injection. This protective effect of taurine was due to higher Mrp2 and Bsep protein levels compared to nonsupplemented LPS-treated rats, whereas relative Mrp2 retrieval from the canalicular membrane induced by LPS was not significantly different. LPS-induced tumor necrosis factor alpha and interleukin-1beta release were lower in taurine-fed rats; however, downregulation of Mrp2 and Bsep expression by LPS was delayed but not prevented. The data show that oral supplementation of taurine induces Mrp2 and Bsep expression and may prevent LPS-induced cholestasis.
在大鼠肝脏中研究了口服补充牛磺酸对内毒素诱导的胆汁淤积的影响。在腹腔注射脂多糖(LPS,4mg/kg体重)后12小时,测定灌注肝脏中的胆汁流量、溴磺酞钠(BSP)和牛磺胆酸盐(TC)排泄,并分析胆小管转运体多药耐药相关蛋白2(Mrp2)和胆盐输出泵(Bsep)的表达。注射LPS导致胆汁流量显著降低(2.2±0.2微升/克肝脏湿重/分钟,而对照组为3.3±0.1微升/克肝脏湿重)、胆汁BSP排泄(10.8±2.2纳摩尔/克/分钟,而对照组为21.0±3.8纳摩尔/克/分钟)和胆汁TC排泄(114±23纳摩尔/克/分钟,而对照组为228±8纳摩尔/克/分钟)。这些影响是由于转运体从小胆管膜回收以及Mrp2和Bsep表达下调所致。在补充牛磺酸的大鼠中,胆汁流量比未处理大鼠高30%,Mrp2和Bsep蛋白的表达增加了两到三倍。在补充牛磺酸的大鼠中,LPS注射后12小时胆汁流量、BSP和TC排泄没有显著降低。牛磺酸的这种保护作用是由于与未补充LPS处理的大鼠相比,Mrp2和Bsep蛋白水平更高,而LPS诱导的从小胆管膜回收Mrp2相对没有显著差异。LPS诱导的肿瘤坏死因子α和白细胞介素-1β释放在喂食牛磺酸的大鼠中较低;然而,LPS对Mrp2和Bsep表达的下调被延迟但未被阻止。数据表明,口服补充牛磺酸可诱导Mrp2和Bsep表达,并可能预防LPS诱导的胆汁淤积。
