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母体胆汁淤积并不影响胎鼠和新生鼠肝脏中钠/牛磺胆酸盐共转运多肽(ntcp)的个体发育表达模式。

Maternal cholestasis does not affect the ontogenic pattern of expression of the Na+/taurocholate cotransporting polypeptide (ntcp) in the fetal and neonatal rat liver.

作者信息

Arrese M, Trauner M, Ananthanarayanan M, Boyer J L, Suchy F J

机构信息

Liver Center and Department of Pediatrics, Yale University School of Medicine, New Haven, CT, USA.

出版信息

Hepatology. 1998 Sep;28(3):789-95. doi: 10.1002/hep.510280328.

Abstract

To assess the effects of cholestasis during pregnancy on fetal and neonatal mRNA expression, protein mass, and function of the Na+/taurocholate cotransporting polypeptide (Ntcp), common bile duct ligation (BDL) was performed in pregnant rats on day 14 of pregnancy (maternal cholestasis [MC] group), and livers were harvested at days 20 and 21 of fetal life, as well as at days 4, 7, 14, 21, and 28 after birth. Sham-operated rats and their litters were used as controls. Ntcp steady-state mRNA levels, protein mass, and function were determined by Northern blotting, immunoblotting, and taurocholate (TC) transport studies in isolated short-term cultured hepatocytes, respectively. In addition, protein mass and function of the organic anion transporting polypeptide (Oatp1), another sinusoidal bile acid transporter, were studied at 4 weeks of age. The majority of pregnant cholestatic rats (94%) were able to carry pregnancy to term. Body and liver weights of the offspring from the MC group were lower than those from sham-operated animals at all postnatal time points. Ntcp steady-state mRNA levels, protein mass, and function were unaffected by MC. The ontogenic pattern of expression was identical in offspring from MC and controls with detection of the Ntcp mRNA at day 21 of fetal life. There was a significant increase in mRNA postnatally, reaching adult levels by 7 days of age. Protein mass and function of Ntcp as well as of Oatp1 were similar in offspring from MC and control groups at 4 weeks of age. In conclusion, maternal obstructive cholestasis during the last third of pregnancy does not affect the fetal/neonatal expression of the basolateral bile acid transporters, Ntcp and Oatp1. This suggests that the impaired bile acid excretion described in this experimental model is not related to altered uptake of bile acids in the affected neonate.

摘要

为评估孕期胆汁淤积对胎儿及新生儿mRNA表达、蛋白质含量以及牛磺胆酸钠共转运多肽(Ntcp)功能的影响,在妊娠第14天对孕鼠进行胆总管结扎(BDL)手术(母体胆汁淤积[MC]组),并在胎儿期第20天和21天以及出生后第4、7、14、21和28天采集肝脏。假手术的大鼠及其幼崽用作对照。分别通过Northern印迹法、免疫印迹法以及在分离的短期培养肝细胞中进行牛磺胆酸盐(TC)转运研究来测定Ntcp稳态mRNA水平、蛋白质含量及功能。此外,在4周龄时研究了另一种窦状隙胆汁酸转运体——有机阴离子转运多肽(Oatp1)的蛋白质含量及功能。大多数妊娠胆汁淤积大鼠(94%)能够足月分娩。在所有出生后时间点,MC组后代的体重和肝脏重量均低于假手术动物的后代。MC对Ntcp稳态mRNA水平、蛋白质含量及功能无影响。MC组和对照组后代的个体发育表达模式相同,在胎儿期第21天可检测到Ntcp mRNA。出生后mRNA显著增加,到7日龄时达到成年水平。在4周龄时,MC组和对照组后代的Ntcp以及Oatp1的蛋白质含量和功能相似。总之,妊娠最后三个月的母体梗阻性胆汁淤积不影响基底外侧胆汁酸转运体Ntcp和Oatp1的胎儿/新生儿表达。这表明该实验模型中描述的胆汁酸排泄受损与受影响新生儿胆汁酸摄取改变无关。

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