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氯苯丁胺预处理对离体灌注大鼠肺摄取氯苯丁胺的影响。

Effect of chlorphentermine pretreatment on chlorphentermine uptake by isolated perfused rat lung.

作者信息

Angevine L S, Ohmiya Y, Mehendale H M

出版信息

Drug Metab Dispos. 1982 Jan-Feb;10(1):68-73.

PMID:6124387
Abstract

Chlorphentermine (CP), an anorectic agent currently in use, is known to be highly accumulated in the lung, causes pulmonary phospholipidosis, and has been suspected of causing pulmonary hypertension. These studies were undertaken to characterize the uptake and accumulation processes and to examine the effect of subacute CP treatment on the uptake kinetics of CP in the rat lung. Animals were treated po with a saline solution of CP (50 mg/kg/day) for 7 days and the controls received the vehicle only. Artificially ventilated isolated rat lung preparations were perfused with Krebs-Ringer bicarbonate buffer containing bovine serum albumin. CP was not metabolized by control or pretreated perfused lungs or by their 9000g supernatant or microsomal fractions. In recirculating perfusion experiments, steady-state uptake was reached after 20 min of perfusion with 0.17 mM CP. Lungs from rats treated with CP as described above accumulated CP to a greater extent and more rapidly than did lungs from control rats. Similarly, lungs from rats treated with CP accumulated significantly greater quantities of CP than control lungs during single-pass perfusion experiments. Whereas control lungs reached a steady state uptake within 7 min, lungs from CP treated animals failed to reach a steady-state uptake during a 10-min perfusion. The lungs from CP-treated rats retained most of the accumulated CP and exhibited a significantly increased half life of efflux in comparison to control rats. Removal of Na+ from the perfusion medium or the addition of harmaline significantly decreased the half-life of CP uptake and the amount of CP accumulated by the lung.

摘要

氯苯丁胺(CP)是一种目前正在使用的食欲抑制剂,已知其在肺中高度蓄积,可导致肺磷脂沉积症,并且一直被怀疑会引起肺动脉高压。开展这些研究旨在表征摄取和蓄积过程,并研究亚急性CP处理对大鼠肺中CP摄取动力学的影响。动物经口给予CP盐溶液(50mg/kg/天),持续7天,对照组仅接受赋形剂。用含牛血清白蛋白的 Krebs-Ringer 碳酸氢盐缓冲液灌注人工通气的离体大鼠肺制剂。CP在对照或预处理的灌注肺及其9000g上清液或微粒体组分中均未代谢。在循环灌注实验中,用0.17mM CP灌注20分钟后达到稳态摄取。如上所述用CP处理的大鼠的肺比对照大鼠的肺蓄积CP的程度更大且更迅速。同样,在单次灌注实验中,用CP处理的大鼠的肺比对照肺蓄积的CP量显著更多。对照肺在7分钟内达到稳态摄取,而用CP处理的动物的肺在10分钟灌注期间未达到稳态摄取。与对照大鼠相比,用CP处理的大鼠的肺保留了大部分蓄积的CP,并且外排半衰期显著延长。从灌注培养基中去除Na+或添加哈尔满可显著降低CP摄取的半衰期以及肺蓄积的CP量。

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