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消胆胺对犬体内替诺昔康消除的加速作用。

Acceleration of the elimination of tenoxicam by cholestyramine in the dog.

作者信息

Guentert T W, Schmitt M, Defoin R

出版信息

J Pharmacol Exp Ther. 1986 Jul;238(1):295-301.

PMID:3723402
Abstract

Two commonly used adsorbents, activated charcoal and cholestyramine, were evaluated in vitro for their ability to adsorb the nonsteroidal anti-inflammatory drug tenoxicam and in vivo for their use in influencing the elimination kinetics of this drug. The Langmuir binding isotherms determined in buffer solutions at pH 7.5 indicated a much greater adsorption capacity of cholestyramine (1.63 g of drug per g of resin) than of charcoal (0.18 g/g of adsorbent) for the acidic drug with a pKa of 5.3. When single i.v. tenoxicam administrations to dogs were followed by multiple p.o. cholestyramine doses the elimination rate of the drug was accelerated drastically. Due to an increased total body clearance (0.65 vs. 0.13 liters/hr), the elimination half-life was reduced from a median base-line value of 31 to 5.4 hr and the mean residence time of drug in the body was decreased from 41 to 7.9 hr. In contrast to cholestyramine, charcoal hardly increased the rate of elimination of tenoxicam over the base-line values determined in the same animals. Inasmuch as these results were similar in all three animals investigated and because the study design precluded an influence of the treatment sequence, it is concluded that cholestyramine efficiently sequesters intestinally secreted tenoxicam and can thereby accelerate drug elimination from the body.

摘要

对两种常用吸附剂——活性炭和考来烯胺进行了体外评估,以测定它们吸附非甾体抗炎药替诺昔康的能力,并进行了体内评估,以研究它们对该药物消除动力学的影响。在pH 7.5的缓冲溶液中测定的朗缪尔吸附等温线表明,对于pKa为5.3的酸性药物,考来烯胺(每克树脂吸附1.63克药物)的吸附能力比活性炭(每克吸附剂吸附0.18克/克)大得多。给犬单次静脉注射替诺昔康后多次口服考来烯胺,药物的消除速率急剧加快。由于总体清除率增加(0.65对0.13升/小时),消除半衰期从中位数基线值31小时降至5.4小时,药物在体内的平均驻留时间从41小时降至7.9小时。与考来烯胺相反,活性炭几乎没有使替诺昔康的消除速率超过在相同动物中测定的基线值。鉴于在所有三只研究动物中这些结果均相似,且由于研究设计排除了治疗顺序的影响,因此得出结论,考来烯胺可有效螯合肠道分泌的替诺昔康,从而加速药物从体内的消除。

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