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No major effects of vitamin D3 (1,25 dihydroxyvitamin D3) on absorption and pharmacokinetics of folic acid and fexofenadine in healthy volunteers

机译:维生素D3(1,25二羟基维生素D3)对健康志愿者体内叶酸和非索非那定的吸收和药代动力学没有重大影响

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摘要

PURPOSE: In Caco-2 cells, folate uptake via the proton-coupled folate transporter (PCFT) increases significantly by a 3-day treatment with 1,25-dihydroxyvitamin D3 (1,25(OH)2D3). Additionally, mRNA content and protein expression of the transporter OATP1A2 were increased up to ninefold with 1,25(OH)2D3. We investigated whether these in vitro findings can be confirmed in humans in vivo.\udMETHODS: Ten healthy volunteers (six women) received 5 mg folic acid orally once before and once together with the last intake of a 10-day course of 0.5 μg 1,25(OH)2D3 orally. One hundred twenty milligrams fexofenadine, an OATP1A2 substrate, was taken in 1 day before the first folic acid intake, and again on the ninth day of 1,25(OH)2D3 intake. Duodenal biopsies were taken for transporter mRNA assessments once before and once on the ninth or tenth day of the vitamin D3 course. Serum folic acid and fexofenadine concentrations were quantified with a chemiluminescence immunoassay and LC-MS/MS, respectively. Pharmacokinetics were compared between periods with standard bioequivalence approaches.\udRESULTS: While geometric mean folic acid AUC0-2h, which mainly reflects absorption, was 0.403 and 0.414 mg/L·h before and after the vitamin D3 course (geometric mean ratio (GMR), 1.027; 90 % confidence interval (90 % CI), 0.788-1.340), the geometric mean fexofenadine AUC0-2h was 1.932 and 2.761 mg/L·h, respectively (GMR, 1.429; 90 % CI, 0.890-2.294). PCFT- and OATP1A2-mRNA expressions in duodenal biopsies were essentially unchanged.\udCONCLUSIONS: No significant changes in folic acid and fexofenadine absorption were observed after a 10-day course of 1,25(OH)2D3 in humans in vivo. This study underlines the importance of confirming in vitro findings in vivo in humans.
机译:目的:在Caco-2细胞中,通过1,25-二羟基维生素D3(1,25(OH)2D3)处理3天,通过质子偶联叶酸转运蛋白(PCFT)吸收的叶酸显着增加。此外,转运蛋白OATP1A2的mRNA含量和蛋白表达与1,25(OH)2D3相比增加了9倍。我们调查了这些体外发现是否可以在人体中得到证实。\ udMethods:十名健康志愿者(六名女性)之前和之后一次口服了5 mg叶酸,最后一次摄入的是为期10天的0.5μg疗程1口服25,OH(OH)2D3。在第一次摄入叶酸之前的1天,然后在摄入1,25(OH)2D3的第9天,服用了120毫克非索非那定(OATP1A2底物)。在维生素D3疗程的第9天或第10天进行一次十二指肠活检以评估转运蛋白mRNA。血清叶酸和非索非那定的浓度分别用化学发光免疫分析法和LC-MS / MS定量。结果:虽然主要反映吸收的叶酸几何平均数AUC0-2h(主要反映吸收)在维生素D3疗程前后分别为0.403和0.414 mg / L·h(几何平均比(GMR)) ,1.027; 90%置信区间(90%CI),0.788-1.340),非索非那定AUC0-2h的几何平均数分别为1.932和2.761 mg / L·h(GMR,1.429; 90%CI,0.890-2.294)。结论:在人体内1,25(OH)2D3的10天疗程后,叶酸和非索非那定的吸收未见明显变化。这项研究强调了确认人类体内体外发现的重要性。

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