Effect of SLCO1B1 polymorphism on the plasma concentrations of bile acids and bile acid synthesis marker in humans.

Xiang X; Han Y; Neuvonen M; Pasanen MK; Kalliokoski A; Backman JT; Laitila J; Neuvonen PJ; Niemi M

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Effect of SLCO1B1 polymorphism on the plasma concentrations of bile acids and bile acid synthesis marker in humans.

机译：SLCO1B1多态性对人血浆中胆汁酸浓度和胆汁酸合成标记物的影响。

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BACKGROUND AND OBJECTIVE: Organic anion transporting polypeptide 1B1 (OATP1B1, encoded by SLCO1B1) is a sinusoidal influx transporter of human hepatocytes. Our aim was to characterize the role of OATP1B1 in the hepatic uptake of bile acids in vivo. METHODS: Fasting blood samples were drawn from 24 healthy volunteers with SLCO1B1 c.388AA-c.521TT (*1A/*1A) genotype, eight with c.388GG-c.521TT (*1B/*1B) genotype, 24 with c.521TC genotype, and nine with c.521CC genotype. Plasma concentrations of 15 endogenous bile acids, their synthesis marker, and cholesterol were determined by liquid chromatography-tandem mass spectrometry. RESULTS: The concentrations of ursodeoxycholic acid, glycoursodeoxycholic acid, chenodeoxycholic acid, and glycochenodeoxycholic acid were approximately 50-240% higher in individuals with the SLCO1B1 c.521CC, c.521TC, or c.388AA-c.521TT genotype than in those with the c.388GG-c.521TT genotype (P<0.05), with the largest differences seen between the c.521CC and c.388GG-c.521TT individuals. The concentration of tauroursodeoxycholic acid was approximately 120% higher in individuals with the c.521TC genotype and that of taurochenodeoxycholic acid 110% higher in individuals with the c.521CC or c.521TC genotype than in those with the c.388GG-c.521TT genotype (P<0.05). The cholic acid concentration was approximately 30% higher in individuals with the c.521CC or c.388AA-c.521TT genotype than in those with the c.388GG-c.521TT genotype (P<0.05), but its conjugates remained unaffected by the genotype. The bile acid synthesis marker 7alpha-hydroxy-4-cholesten-3-one/cholesterol concentration ratio was 62 or 45% higher in the c.388AA-c.521TT participants than in the c.388GG-c.521TT or c.521TC participants, respectively (P<0.05). CONCLUSION: SLCO1B1 polymorphism considerably affects the disposition of several endogenous bile acids and bile acid synthesis marker, indicating that OATP1B1 plays an important role in the hepatic uptake of bile acids in vivo in humans.

机译：背景与目的：有机阴离子转运多肽1B1（OATP1B1，由SLCO1B1编码）是人肝细胞的正弦流入转运蛋白。我们的目的是表征OATP1B1在体内胆汁酸肝吸收中的作用。方法：从24名健康志愿者的SLCO1B1 c.388AA-c.521TT（* 1A / * 1A）基因型，八名c.388GG-c.521TT（* 1B / * 1B）基因型，24名c。 .521TC基因型，其中九个具有c.521CC基因型。通过液相色谱-串联质谱法测定15种内源性胆汁酸的血浆浓度，它们的合成标记物和胆固醇。结果：SLCO1B1 c.521CC，c.521TC或c.388AA-c.521TT基因型的个体中熊去氧胆酸，糖去氧胆酸，鹅去氧胆酸和糖去氧胆酸的浓度比那些具有基因型的人高约50-240％ c.388GG-c.521TT基因型（P <0.05），在c.521CC和c.388GG-c.521TT个人之间发现的差异最大。与具有c.388GG-c.521TT基因型的个体相比，具有c.521TC基因型的个体中的tauroursodeoxycholic acid的浓度大约高120％，而具有c.521CC或c.521TC基因型的个体中taurochenodeoxycholic acid的浓度高110％。基因型（P <0.05）。具有c.521CC或c.388AA-c.521TT基因型的个体的胆酸浓度比具有c.388GG-c.521TT基因型的个体的胆酸浓度高约30％（P <0.05），但其结合物仍不受其影响基因型。与c.388GG-c.521TT或c.521TC相比，c.388AA-c.521TT参与者的胆汁酸合成标记物7alpha-羟基-4-胆甾烯3-胆固醇/胆固醇浓度比高62或45％。参与者，分别为（P <0.05）。结论：SLCO1B1基因多态性极大地影响了几种内源性胆汁酸和胆汁酸合成标记的分布，表明OATP1B1在人体内胆汁酸肝吸收中起重要作用。

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《Pharmacogenetics and genomics》 |2009年第6期|共11页
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Xiang X; Han Y; Neuvonen M; Pasanen MK; Kalliokoski A; Backman JT; Laitila J; Neuvonen PJ; Niemi M;
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1. Effect of SLCO1B1 polymorphism on the plasma concentrations of bile acids and bile acid synthesis marker in humans. [J] . Xiang X, Han Y, Neuvonen M, Pharmacogenetics and genomics . 2009,第6期

机译：SLCO1B1多态性对人血浆中胆汁酸浓度和胆汁酸合成标记物的影响。
2. Gender, but not CYP7A1 or SLCO1B1 polymorphism, affects the fasting plasma concentrations of bile acids in human beings. [J] . Xiaoqiang Xiang, Janne T Backman, Pertti J Neuvonen, Basic & clinical pharmacology & toxicology. . 2012,第3期

机译：性别而非CYP7A1或SLCO1B1多态性会影响人体内空腹胆汁酸的血浆浓度。
3. Significance of plasma 7alpha-hydroxy-4-cholesten-3-one and 27-hydroxycholesterol concentrations as markers for hepatic bile acid synthesis in cholesterol-fed rabbits. [J] . Honda A, Yoshida T, Xu G, Metabolism: Clinical and Experimental . 2004,第1期

机译：血浆7α-羟基-4-胆甾烯3-1和27-羟基胆固醇浓度作为胆固醇喂养的兔肝胆汁酸合成的标志物的意义。
4. Metabolic Phenotyping of Bile Acids - Standardized quantitative bile acids analysis in human plasma/serum and mouse plasma on different (U)HPLC-MS/MS platforms. [C] . Hai Pham Tuan, Doreen Kirchberg, Ines Zitturi, International Mass Spectrometry Conference . 2014

机译：胆汁酸的代谢表型 - 在不同（U）HPLC-MS / MS平台上的人血浆/血清和小鼠血浆中标准化的定量胆汁酸分析。
5. Effect of dietary conjugated linoleic acid on molecular markers for bile acid metabolism, cholesterol synthesis and inflammation in rats. [D] . Matutes, Katherine Wright. 2005

机译：日粮共轭亚油酸对大鼠胆汁酸代谢，胆固醇合成和炎症分子标记的影响。
6. Bile acid N-acetylglucosaminidation. In vivo and in vitro evidence for a selective conjugation reaction of 7 beta-hydroxylated bile acids in humans. [O] . H U Marschall, H Matern, H Wietholtz, 1992

机译：胆汁酸N-乙酰氨基葡糖化。体内和体外证据表明人类中7种β-羟基化胆汁酸的选择性结合反应。
7. Bile acid N-acetylglucosaminidation. In vivo and in vitro evidence for a selective conjugation reaction of 7 beta-hydroxylated bile acids in humans. [O] . Marschall, H U, Matern, H, Wietholtz, H, 1992

机译：胆汁酸N-乙酰氨基葡糖化。体内和体外证据表明人类中7种β-羟基化胆汁酸的选择性结合反应。

Effect of SLCO1B1 polymorphism on the plasma concentrations of bile acids and bile acid synthesis marker in humans.

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