首页> 外文期刊>Pharmaceutical research >Rectal absorption of vigabatrin, a substrate of the proton coupled amino acid transporter (PAT1, Slc36a1), in rats.
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Rectal absorption of vigabatrin, a substrate of the proton coupled amino acid transporter (PAT1, Slc36a1), in rats.

机译:大鼠在直肠中吸收了vigabatrin(质子偶联氨基酸转运蛋白(PAT1,Slc36a1)的底物)。

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To investigate the rectal absorption of vigabatrin in rats, based on the hypothesis that PAT1 (Slc36a1) is involved.Male Sprague-Dawley rats were dosed rectally with five different gels, varying in buffer capacity, the amount of vigabatrin, and co-administration of proline or tryptophan. Western blotting was used to detect rPAT1 in rat rectal epithelium. X. Laevis oocytes were injected with SLC36A1 cRNA for the expression of hPAT1, prior to two-electrode voltage clamp measurements.rPAT1 protein was present in rat rectal epithelium. Approximately 7%-9% of a 1?mg/kg vigabatrin dose was absorbed after rectal administration, regardless of the formulation used. Increasing the dose of vigabatrin 10-fold decreased the absolute bioavailability to 4.2%. Co-administration of proline or tryptophan changed the pharmacokinetic profile, indicating a role of PAT1 in the rectal absorption of vigabatrin. Transport of vigabatrin via hPAT1 expressed in X. Laevis oocytes had a K(m) of 5.2?±?0.6?mM and was almost completely inhibited by tryptophan.Although vigabatrin is a PAT1 substrate and the rPAT1 protein is expressed in the rectum epithelium, vigabatrin has low rectal absorption in rats.
机译:根据涉及PAT1(Slc36a1)的假说,研究大鼠vigabatrin的直肠吸收情况。对雄性Sprague-Dawley大鼠进行直肠给药五种不同的凝胶,缓冲液容量,vigabatrin的量和共同给药脯氨酸或色氨酸。 Western印迹用于检测大鼠直肠上皮中的rPAT1。 X.在两电极电压钳测量之前,向Laevis卵母细胞注射SLC36A1 cRNA表达hPAT1。大鼠直肠上皮中存在rPAT1蛋白。直肠给药后,无论使用哪种制剂,大约吸收1?mg / kg维加巴特林剂量的7%-9%。将Vigabatrin的剂量增加10倍会使绝对生物利用度降低至4.2%。脯氨酸或色氨酸的共同给药改变了药代动力学特征,表明PAT1在维加巴特林的直肠吸收中具有作用。 vigabatrin通过X上表达的hPAT1转运。Laevis卵母细胞的K(m)为5.2?±?0.6?mM,几乎完全被色氨酸抑制。尽管vigabatrin是PAT1底物,rPAT1蛋白在直肠上皮中表达, Vigabatrin在大鼠中的直肠吸收低。

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