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在小型猪中,Roux-en-Y胃旁路术通过降低肝脏对胆汁酸的摄取,增加了全身胆汁酸浓度,但门静脉胆汁酸浓度未增加。

Roux-en-Y gastric bypass increases systemic but not portal bile acid concentrations by decreasing hepatic bile acid uptake in minipigs.

作者信息

Chávez-Talavera O, Baud G, Spinelli V, Daoudi M, Kouach M, Goossens J-F, Vallez E, Caiazzo R, Ghunaim M, Hubert T, Lestavel S, Tailleux A, Staels B, Pattou F

机构信息

Université de Lille, U1011 - EGID, Lille, France.

Inserm, U1011, Lille, France.

出版信息

Int J Obes (Lond). 2017 Apr;41(4):664-668. doi: 10.1038/ijo.2017.7. Epub 2017 Jan 17.

Abstract

Roux-en-Y gastric bypass (RYGB) surgery is widely used in the management of morbid obesity. RYGB improves metabolism independently of weight loss by still unknown mechanisms. Bile acids (BAs) are good candidates to explain this benefit, since they regulate metabolic homeostasis and their systemic concentrations increase upon RYGB. Here we analyzed the mechanisms underlying the increase in systemic BA concentrations after RYGB and the role of the liver therein. To this aim, we used the Göttingen-like minipig, a human-size mammalian model, which allows continuous sampling and simultaneous analysis of pre-hepatic portal and systemic venous blood. BA concentrations and pool composition were measured in portal blood, containing intestinal reabsorbed BAs and compared to systemic blood during a standardized meal test before and after RYGB. Systemic total BA concentrations increased after RYGB, due to an increase in conjugated BAs. Interestingly, the ratio of portal:systemic conjugated BAs decreased after RYGB, indicating a role for the liver in systemic BA concentrations changes. In line, hepatic expression of BA transporter genes decreased after RYGB. Our results show that the increase in systemic BAs after surgery is due to decreased selective hepatic recapture. Thus, alterations in hepatic function contribute to the increase in systemic BAs after RYGB.

摘要

Roux-en-Y胃旁路术(RYGB)在病态肥胖的治疗中被广泛应用。RYGB通过尚不清楚的机制独立于体重减轻改善代谢。胆汁酸(BAs)是解释这种益处的良好候选因素,因为它们调节代谢稳态且其全身浓度在RYGB后会升高。在此,我们分析了RYGB后全身BA浓度升高的潜在机制以及肝脏在其中的作用。为此,我们使用了类似哥廷根小型猪这种与人类大小相似的哺乳动物模型,它允许对肝前门静脉血和全身静脉血进行连续采样和同步分析。在RYGB前后的标准化进餐试验期间,测量门静脉血(含有肠道重吸收的BAs)中的BA浓度和池组成,并与全身血液进行比较。RYGB后全身总BA浓度升高,这是由于结合型BAs增加所致。有趣的是,RYGB后门静脉:全身结合型BAs的比率降低,表明肝脏在全身BA浓度变化中起作用。同样,RYGB后BA转运蛋白基因的肝脏表达降低。我们的结果表明,手术后全身BAs的增加是由于肝脏选择性重摄取减少所致。因此,肝功能的改变促成了RYGB后全身BAs的增加。

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