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Abcg2 转运体影响美洛昔康的血浆、乳中和组织水平。

Abcg2 transporter affects plasma, milk and tissue levels of meloxicam.

机构信息

Department of Biomedical Sciences-Physiology, Veterinary Faculty, Instituto de Desarrollo Ganadero y Sanidad Animal (INDEGSAL), Universidad de León, Campus de Vegazana, León, Spain.

Department of Biomedical Sciences-Physiology, Veterinary Faculty, Instituto de Desarrollo Ganadero y Sanidad Animal (INDEGSAL), Universidad de León, Campus de Vegazana, León, Spain.

出版信息

Biochem Pharmacol. 2020 May;175:113924. doi: 10.1016/j.bcp.2020.113924. Epub 2020 Mar 23.

DOI:10.1016/j.bcp.2020.113924
PMID:32217099
Abstract

ATP-binding cassette (ABCG2) is an efflux transporter that extrudes xenotoxins from cells in liver, intestine, mammary gland, brain and other organs, affecting the pharmacokinetics, brain accumulation and secretion into milk of several compounds, including antitumoral, antimicrobial and anti-inflammatory drugs. The aim of this study was to investigate whether the widely used anti-inflammatory drug meloxicam is an Abcg2 sustrate, and how this transporter affects its systemic distribution. Using polarized ABCG2-transduced cell lines, we found that meloxicam is efficiently transported by murine Abcg2 and human ABCG2. After oral administration of meloxicam, the area under the plasma concentration-time curve in Abcg2 mice was 2-fold higher than in wild type mice (146.06 ± 10.57 µg·h/ml versus 73.80 ± 10.00 µg·h/ml). Differences in meloxicam distribution were reported for several tissues after oral and intravenous administration, with a 20-fold higher concentration in the brain of Abcg2 after oral administration. Meloxicam secretion into milk was also affected by the transporter, with a 2-fold higher milk-to-plasma ratio in wild-type compared with Abcg2 lactating female mice after oral and intravenous administration. We conclude that Abcg2 is an important determinant of the plasma and brain distribution of meloxicam and is clearly involved in its secretion into milk.

摘要

三磷酸腺苷结合盒(ABCG2)是一种外排转运体,可将肝脏、肠道、乳腺、大脑和其他器官中的外源性毒素排出细胞,影响多种化合物的药代动力学、脑内蓄积和分泌入乳汁,包括抗肿瘤、抗菌和抗炎药物。本研究旨在探讨广泛使用的抗炎药美洛昔康是否为 Abcg2 的底物,以及该转运体如何影响其全身分布。使用极化 ABCG2 转染细胞系,我们发现美洛昔康可被鼠源性 Abcg2 和人源性 ABCG2 有效转运。美洛昔康经口给药后,Abcg2 小鼠的血浆浓度-时间曲线下面积(AUC)是野生型小鼠的 2 倍(146.06 ± 10.57 µg·h/ml 比 73.80 ± 10.00 µg·h/ml)。口服和静脉给药后,几种组织中美洛昔康的分布存在差异,口服给药后 Abcg2 小鼠的脑内浓度高 20 倍。转运体也影响美洛昔康分泌入乳汁,口服和静脉给药后,野生型小鼠的乳汁-血浆比是 Abcg2 泌乳雌鼠的 2 倍。我们的结论是,Abcg2 是美洛昔康的血浆和脑内分布的重要决定因素,并且明显参与其分泌入乳汁。

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