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Response to hydrocodone, codeine and oxycodone in a CYP2D6 poor metabolizer.

机译:CYP2D6弱代谢者对氢可酮,可待因和羟考酮的反应。

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摘要

Codeine is metabolized by the cytochrome P450 2D6 (CYP2D6) to morphine. Codeine is a much weaker agonist at mu opioid receptors than morphine. Therefore, codeine analgesia is highly dependent on CYP2D6 activity. Large prospective studies in the clinical environment do not exist, but it appears reasonable to avoid codeine use in CYP2D6 poor metabolizers (PMs). CYP2D6 metabolizes other opioid analgesics, including tramadol, dihydrocodeine, oxycodone and hydrocodone, although they have been less systematically studied. It is unclear whether these other pro-drugs may be as completely dependent on CYP2D6 for their analgesia as codeine. We describe a patient identified as a CYP2D6 PM with a history of problems with opioid analgesics. The patient was an 85-year-old female Caucasian who had hip surgery. The patient had a long-standing intolerance to codeine. In her first admission, she couldn't tolerate the regimen of oxycodone combined with tramadol prns (as needed). She was genotyped as a CYP2D6 PM and afterthe information was provided to the treating physician in her second admission, she seemed to have a better response to hydrocodone. Large case-control naturalistic studies followed by randomized trials in patients taking opioid analgesics may be needed to definitively establish that CYP2D6 genotyping has clinical relevance in the use of several opioid analgesics.
机译:可待因被细胞色素P450 2D6(CYP2D6)代谢为吗啡。可待因对μ阿片受体的激动剂比吗啡弱得多。因此,可待因镇痛高度依赖于CYP2D6活性。在临床环境中尚无大型前瞻性研究,但在可CYP2D6弱代谢者(PMs)中避免使用可待因似乎是合理的。 CYP2D6代谢其他阿片类镇痛药,包括曲马多,二氢可待因,羟考酮和氢可酮,尽管它们的系统研究较少。尚不清楚这些其他前药是否像可待因一样完全依赖CYP2D6的镇痛作用。我们描述了一个被确定为CYP2D6 PM的患者,该患者具有阿片类镇痛药问题的历史。该患者是一名85岁的女性高加索人,她接受了髋关节手术。该患者长期对可待因不耐受。在她的第一次入院时,她无法忍受羟考酮与曲马多的联合用药方案(根据需要)。她的基因型为CYP2D6 PM,在第二次入院后将信息提供给治疗医师后,她似乎对氢可酮的反应更好。为了确定CYP2D6基因型在使用几种类阿片镇痛剂中具有临床意义,可能需要进行大型病例对照自然研究,然后在接受阿片类镇痛剂的患者中进行随机试验。

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