吡罗昔康
毒性
替诺西康
美洛昔康
氯诺昔康
血浆浓度
化学
药理学
人血清白蛋白
吸收(声学)
白蛋白
药品
内分泌学
生物化学
医学
止痛药
物理
替代医学
有机化学
病理
声学
作者
E Albengres,Saı̈k Urien,Jean La Barre,P Nguyen,Françoise Brée,Pascale Jolliet,J.P. Tillement,R. S. Tsai,Pierre‐Alain Carrupt,Bernard Testa
出处
期刊:PubMed
日期:1993-01-01
卷期号:15 (3): 125-34
被引量:22
摘要
Six oxicams, sudoxicam, isoxicam, piroxicam, tenoxicam, meloxicam and lornoxicam, were compared in an attempt to understand why, despite close chemical structures, two of them were associated with an increased risk of toxicity in patients. Different factors have been revealed which may explain these differences. A weak association constant to human serum albumin (HSA), together with a high plasma concentration, favours a rapid increase in unbound concentration (Cu) when total plasma concentration rises (peak of absorption). Pathological states may enhance this increase when both HSA plasma concentration is decreased and free fatty acid concentrations are increased. However, the main cause of toxicity may be the existence in some subjects of HSA natural mutants whose ability to bind oxicams is markedly lower than normal.
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