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大鼠肝再生过程中参与胆汁分泌的肝脏转运系统的调节

Regulation of hepatic transport systems involved in bile secretion during liver regeneration in rats.

作者信息

Vos T A, Ros J E, Havinga R, Moshage H, Kuipers F, Jansen P L, Müller M

机构信息

Groningen Institute for Drug Studies, University Hospital Groningen, The Netherlands.

出版信息

Hepatology. 1999 Jun;29(6):1833-9. doi: 10.1002/hep.510290638.

Abstract

We investigated the expression of hepatic transport systems involved in bile secretion during liver regeneration after partial hepatectomy (PH) in rats. Initial studies showed maximal BrdU incorporation 24 hours after PH. Therefore, transporter expression and bile secretion were analyzed in detail at this time. The mRNA levels of the multidrug resistance genes mdr1a and mrp1 slightly increased, whereas mdr1b mRNA levels showed an extensive increase after PH. The mRNA levels of the conjugate transporter, mrp2, decreased slightly, whereas mrp2 protein levels did not change. Bilirubin secretion did not change, but the biliary glutathione secretion markedly decreased and the hepatic GSH content increased. The messenger RNA levels of the bile salt uptake transporters ntcp, oatp1, and oatp2 and the bile salt exporter, bsep/spgp, all decreased with ntcp showing the most prominent decrease. Protein levels of ntcp dramatically decreased whereas oatp2 only slightly decreased. Oatp1 protein expression slightly increased and bsep/spgp protein levels did not change. Decreased levels of bile salt uptake systems were associated with a 10-fold increase in the plasma bile salt concentration, yet, bile flow and bile salt secretion were increased when expressed per gram liver and unaffected when expressed on the basis of body weight. In conclusion, during the initial phase of rat liver regeneration ntcp is down-regulated whereas other transporter proteins involved in bile secretion are only slightly affected. Despite increased serum bile salt levels the remnant liver is not cholestatic: bile flow is maintained by uptake of bile salts probably via oatp isoforms and their secretion via bsep/spgp.

摘要

我们研究了大鼠部分肝切除(PH)后肝再生过程中参与胆汁分泌的肝脏转运系统的表达。初步研究显示,PH后24小时5-溴脱氧尿苷(BrdU)掺入量达到最大值。因此,此时对转运体表达和胆汁分泌进行了详细分析。多药耐药基因mdr1a和mrp1的mRNA水平略有升高,而PH后mdr1b mRNA水平显著升高。结合转运体mrp2的mRNA水平略有下降,而mrp2蛋白水平未发生变化。胆红素分泌未改变,但胆汁谷胱甘肽分泌显著减少,肝脏谷胱甘肽(GSH)含量增加。胆盐摄取转运体ntcp、oatp1和oatp2以及胆盐外排转运体bsep/spgp的信使RNA水平均下降,其中ntcp下降最为显著。ntcp蛋白水平显著下降,而oatp2仅略有下降。Oatp1蛋白表达略有增加,bsep/spgp蛋白水平未发生变化。胆盐摄取系统水平的降低与血浆胆盐浓度升高10倍相关,然而,以每克肝脏计算时胆汁流量和胆盐分泌增加,而以体重为基础计算时则未受影响。总之,在大鼠肝再生的初始阶段,ntcp下调,而其他参与胆汁分泌的转运蛋白仅受到轻微影响。尽管血清胆盐水平升高,但残余肝脏并未发生胆汁淤积:胆汁流量可能通过oatp异构体摄取胆盐并通过bsep/spgp分泌胆盐来维持。

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