通过 OATP2B1 将奥美沙坦转化为奥美沙坦美多索米，这是一种可改善肠道吸收的原药，可被 OATP2B1 识别为底物。

IF 3.5 3区医学 Q2 CHEMISTRY, MULTIDISCIPLINARY Pharmaceutical Research Pub Date : 2024-05-01 Epub Date: 2024-03-14 DOI:10.1007/s11095-024-03687-1

Naomi Fukazawa, Tomohiro Nishimura, Keisuke Orii, Saki Noguchi, Masatoshi Tomi

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引用次数: 0

摘要

目的：奥美沙坦酯（奥美沙坦-MX）是血管紧张素 II 受体阻滞剂（ARB）奥美沙坦的酯类原药，在肠道 pH 值下主要呈阴离子型。人类有机阴离子转运多肽 2B1 （OATP2B1）在小肠中表达，并参与各种酸性药物的吸收。本研究旨在验证一个假设，即尽管奥美沙坦本身不是 OATP2B1 的底物，但 OATP2B1 介导的吸收有助于促进奥美沙坦-MX 的肠道吸收：方法：建立了四环素诱导的人 OATP2B1 和大鼠 Oatp2b1 外表达 HEK 293 细胞系（分别为 hOATP2B1/T-REx-293 和 rOatp2b1/T-REX-293），以描述 OATP2B1 介导的吸收。大鼠空肠通透性用乌星室测量。采用液相色谱-串联质谱法对 ARB 进行定量：结果：在hOATP2B1/T-REX-293和rOatp2b1/T-REX-293细胞中观察到了明显的奥美沙坦-MX摄取，而奥美沙坦的摄取量则无法检测到或远远低于奥美沙坦-MX的摄取量。此外，与奥美沙坦相比，奥美沙坦-MX 在 Caco-2 细胞中的吸收率高出数倍，在大鼠空肠中的渗透性也更高。奥美沙坦-MX在hOATP2B1/T-REX-293细胞和Caco-2细胞中的摄取量在OATP2B1底物/抑制剂（如1 mM 3-硫酸雌酮、100 µM 利福霉素SV和100 µM氟伐他汀等）的作用下显著降低。OATP2B1 抑制剂 50 µM 柚皮甙能显著降低大鼠 Oatp2b1 介导的奥美沙坦-MX 吸收和大鼠空肠渗透性。大鼠口服含 50 µM 柚皮甙的奥美沙坦-MX 后，奥美沙坦的血浆浓度-时间曲线下面积明显降低至 76.9%：奥美沙坦-MX是OATP2B1的底物，与母药奥美沙坦相比，柚皮苷敏感转运系统有助于改善奥美沙坦-MX的肠道吸收。

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Conversion of Olmesartan to Olmesartan Medoxomil, A Prodrug that Improves Intestinal Absorption, Confers Substrate Recognition by OATP2B1.

Purpose: Olmesartan medoxomil (olmesartan-MX), an ester-type prodrug of the angiotensin II receptor blocker (ARB) olmesartan, is predominantly anionic at intestinal pH. Human organic anion transporting polypeptide 2B1 (OATP2B1) is expressed in the small intestine and is involved in the absorption of various acidic drugs. This study was designed to test the hypothesis that OATP2B1-mediated uptake contributes to the enhanced intestinal absorption of olmesartan-MX, even though olmesartan itself is not a substrate of OATP2B1.

Methods: Tetracycline-inducible human OATP2B1- and rat Oatp2b1-overexpressing HEK 293 cell lines (hOATP2B1/T-REx-293 and rOatp2b1/T-REx-293, respectively) were established to characterize OATP2B1-mediated uptake. Rat jejunal permeability was measured using Ussing chambers. ARBs were quantified by liquid chromatography-tandem mass spectrometry.

Results: Significant olmesartan-MX uptake was observed in hOATP2B1/T-REx-293 and rOatp2b1/T-REx-293 cells, whereas olmesartan uptake was undetectable or much lower than olmesartan-MX uptake, respectively. Furthermore, olmesartan-MX exhibited several-fold higher uptake in Caco-2 cells and greater permeability in rat jejunum compared to olmesartan. Olmesartan-MX uptake in hOATP2B1/T-REx-293 cells and in Caco-2 cells was significantly decreased by OATP2B1 substrates/inhibitors such as 1 mM estrone-3-sulfate, 100 µM rifamycin SV, and 100 µM fluvastatin. Rat Oatp2b1-mediated uptake and rat jejunal permeability of olmesartan-MX were significantly decreased by 50 µM naringin, an OATP2B1 inhibitor. Oral administration of olmesartan-MX with 50 µM naringin to rats significantly reduced the area under the plasma concentration-time curve of olmesartan to 76.9%.

Conclusion: Olmesartan-MX is a substrate for OATP2B1, and the naringin-sensitive transport system contributes to the improved intestinal absorption of olmesartan-MX compared with its parent drug, olmesartan.

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来源期刊

Pharmaceutical Research 医学-化学综合

CiteScore

6.60

自引率

5.40%

发文量

276

审稿时长

3.4 months

期刊介绍： Pharmaceutical Research, an official journal of the American Association of Pharmaceutical Scientists, is committed to publishing novel research that is mechanism-based, hypothesis-driven and addresses significant issues in drug discovery, development and regulation. Current areas of interest include, but are not limited to: -(pre)formulation engineering and processing- computational biopharmaceutics- drug delivery and targeting- molecular biopharmaceutics and drug disposition (including cellular and molecular pharmacology)- pharmacokinetics, pharmacodynamics and pharmacogenetics. Research may involve nonclinical and clinical studies, and utilize both in vitro and in vivo approaches. Studies on small drug molecules, pharmaceutical solid materials (including biomaterials, polymers and nanoparticles) biotechnology products (including genes, peptides, proteins and vaccines), and genetically engineered cells are welcome.