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异丙托溴铵和左旋卡尼汀经离体鼠肺肺循环吸收是由被动过程驱动,而非由 OCT/OCTN 转运体的主动摄取所驱动。

Absorption of ipratropium and l-carnitine into the pulmonary circulation of the ex-vivo rat lung is driven by passive processes rather than active uptake by OCT/OCTN transporters.

机构信息

School of Pharmacy & Pharmaceutical Sciences, Cardiff University, Wales CF10 3NB, United Kingdom.

JPK Consulting, Hitchin, Hertfordshire, SG5 1XG, United Kingdom.

出版信息

Int J Pharm. 2015 Dec 30;496(2):834-41. doi: 10.1016/j.ijpharm.2015.10.036. Epub 2015 Oct 22.

DOI:10.1016/j.ijpharm.2015.10.036
PMID:26475971
Abstract

The organic cation transporters OCT and OCTN have been reported to play a significant role in the cellular uptake of substrates within in vitro lung cells. However, no studies to date have investigated the effect of these transporters upon transepithelial absorption of substrates into the pulmonary circulation. We investigated the contribution of OCT and OCTN transporters to total pulmonary absorption of l-carnitine and the anti-muscarinic drug, ipratropium, across an intact isolated perfused rat lung (IPRL). The results obtained from the IPRL were contrasted with active transport in vitro using three human pulmonary cell lines and primary rat alveolar epithelial cells. Ex-vivo studies showed that OCT/OCTN transporters do not play a role in the overall pulmonary absorption of l-carnitine or ipratropium, as evidenced by the effect of chemical inhibition of these transporters upon pulmonary absorption. In contrast, in vitro studies showed that OCT/OCTN transporters play a significant role in cellular accumulation of substrates with preferential uptake of ipratropium by OCTs, and of l-carnitine uptake by OCTNs. The results show that in vitro uptake studies cannot be predictive of airway to blood absorption in vivo. Nevertheless, localised submucosal pulmonary concentrations of inhaled drugs and their pulmonary pharmacodynamic profiles may be influenced by OCT/OCTN transport activity.

摘要

有机阳离子转运体 OCT 和 OCTN 已被报道在体外肺细胞中对底物的细胞摄取中发挥重要作用。然而,迄今为止,尚无研究探讨这些转运体对底物经肺上皮细胞向肺循环的跨上皮吸收的影响。我们研究了 OCT 和 OCTN 转运体对左旋肉碱和抗毒蕈碱药物异丙托溴铵经完整离体灌注大鼠肺(IPRL)的总肺吸收的贡献。通过使用三种人肺细胞系和原代大鼠肺泡上皮细胞进行体外主动转运,对 IPRL 获得的结果进行了对比。离体研究表明,OCT/OCTN 转运体在左旋肉碱或异丙托溴铵的整体肺吸收中不起作用,这表明这些转运体的化学抑制对肺吸收的影响。相比之下,体外研究表明,OCT/OCTN 转运体在底物的细胞积累中发挥重要作用,OCT 优先摄取异丙托溴铵,OCTN 摄取左旋肉碱。结果表明,体外摄取研究不能预测体内气道到血液的吸收。然而,吸入药物的局部黏膜下肺浓度及其肺药效学特征可能受 OCT/OCTN 转运活性的影响。

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