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高剂量对乙酰氨基酚未导致肝损伤的代谢基础:一项病例研究。

Metabolic basis for high paracetamol dosage without hepatic injury: a case study.

作者信息

Tredger J M, Thuluvath P, Williams R, Murray-Lyon I M

机构信息

Institute of Liver Studies, King's College Hospital, Denmark Hill, London, UK.

出版信息

Hum Exp Toxicol. 1995 Jan;14(1):8-12. doi: 10.1177/096032719501400102.

Abstract
  1. Studies of paracetamol metabolism were performed in a 58-year-old female with rheumatoid arthritis who had consumed 15-20 g paracetamol daily for 5 years without developing liver damage and data were compared with results in seven normal volunteers. 2. After a test dose of 2 g paracetamol, the formation of paracetamol sulphate and glucuronide conjugates detected in plasma from the patient was delayed by around 2 h relative to values in normal volunteers and the proportion of sulphate conjugates excreted in urine was 1.5 to 2 times those in normal volunteers (52% vs 26-35% of dose, respectively). The fractional metabolite clearance of paracetamol to glutathione-derived conjugates (0.28 ml min-1 kg-1) in our patient was > 30% lower than in normal females. 3. A combination of slow paracetamol absorption, enhanced detoxication of paracetamol (by sulphation) and reduced metabolism to potentially cytotoxic metabolites may have reduced the risk of liver damage in this patient. The latter may have reflected pharmacogenetic deficiencies in cytochrome P450 isoenzymes persisting despite chronic alcohol consumption (40-60 g per day) or resulted from inhibition of paracetamol activation by concomitant ingestion of aminophylline.
摘要
  1. 对一名58岁患类风湿关节炎的女性进行了扑热息痛代谢研究。该女性连续5年每日服用15 - 20克扑热息痛而未出现肝损伤,并将数据与7名正常志愿者的结果进行了比较。2. 给予2克扑热息痛测试剂量后,患者血浆中扑热息痛硫酸盐和葡萄糖醛酸结合物的形成相对于正常志愿者延迟了约2小时,尿中排泄的硫酸盐结合物比例是正常志愿者的1.5至2倍(分别为剂量的52%和26% - 35%)。我们的患者中扑热息痛向谷胱甘肽衍生结合物的代谢物清除分数(0.28毫升·分钟⁻¹·千克⁻¹)比正常女性低30%以上。3. 扑热息痛吸收缓慢、扑热息痛解毒增强(通过硫酸化)以及向潜在细胞毒性代谢物的代谢减少,这些因素共同作用可能降低了该患者肝损伤的风险。后者可能反映了尽管长期饮酒(每天40 - 60克),细胞色素P450同工酶仍存在药物遗传学缺陷,或者是由于同时摄入氨茶碱抑制了扑热息痛的活化所致。

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