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临床药代动力学对精神分裂症患者抗精神病药物治疗的影响。

Impact of clinical pharmacokinetics on neuroleptic therapy in patients with schizophrenia.

作者信息

Midha K K, Hubbard J W, Marder S R, Marshall B D, Van Putten T

机构信息

College of Pharmacy, University of Saskatchewan, Saskatoon.

出版信息

J Psychiatry Neurosci. 1994 Jul;19(4):254-64.

Abstract

This review covers some recent work on: 1. The effects of route of administration on the pharmacokinetics of fluphenazine and some of its metabolites; 2. The clinical pharmacokinetics of fluphenazine in acute patients medicated with oral fluphenazine; 3. The clinical pharmacokinetics of haloperidol in acute patients medicated with oral haloperidol; 4. The clinical pharmacokinetics of fluphenazine in the maintenance of individuals with chronic schizophrenia with fluphenazine decanoate; 5. A systematic dose reduction study in maintenance treatment refractory patients with oral haloperidol. A study in which plasma levels of fluphenazine and fluphenazine sulfoxide were measured in a group of DSM-III-R patients with schizophrenia before and after switching from oral fluphenazine to depot fluphenazine, decanoate revealed much higher levels of fluphenazine sulfoxide with oral medication compared with those found with depot fluphenazine. These data illustrate the effect of "first pass" metabolism after oral fluphenazine. Thus in a group of 33 patients randomly assigned to receive 5 mg, 10 mg or 25 mg oral fluphenazine daily, steady state plasma fluphenazine levels at each dose were significantly lower that those of fluphenazine sulfoxide or 7-hydroxy-fluphenazine, although there were no significant differences between the levels of fluphenazine and fluphenazine N4-oxide. On the other hand, plasma levels of the parent drug were significantly higher than those of any metabolite in a corresponding group of patients at steady state on depot medication. These observations underscore the importance of route dependent differences in the pharmacokinetics of fluphenazine which can lead to problems when switching patients from oral to depot neuroleptics. The concept of "disabling side-effects" is an important development in understanding relationships between plasma levels of neuroleptic drugs and clinical response in patients with schizophrenia. Risk-benefit analysis shows clearly that evaluation of relationships between plasma levels and clinical response must take into account the consequences of side-effects which the patient feels have a negating effect on therapy. Emerging data on putative therapeutic plasma level ranges in maintenance therapy are potentially important and may be particularly useful in the maintenance of patients on low dose therapy. It is noteworthy that in a carefully executed dose reduction study in treatment resistant patients under medication with haloperidol, the mean lowest effective dose (8.7 ng/mL) lay within the optimal therapeutic range (5 ng/mL to 12 ng/mL) found in acutely psychotic patients. The study showed that gradual dose reduction of neuroleptic was possible in chronic treatment resistant patients with schizophrenia who were originally thought by ward staff to require high doses of neuroleptic.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

本综述涵盖了一些近期的研究工作

  1. 给药途径对氟奋乃静及其某些代谢产物药代动力学的影响;2. 口服氟奋乃静治疗急性患者时的临床药代动力学;3. 口服氟哌啶醇治疗急性患者时的临床药代动力学;4. 用氟奋乃静癸酸酯维持治疗慢性精神分裂症患者时氟奋乃静的临床药代动力学;5. 口服氟哌啶醇维持治疗难治性患者的系统剂量减少研究。一项在一组DSM-III-R精神分裂症患者中进行的研究,测量了从口服氟奋乃静转换为长效氟奋乃静癸酸酯前后血浆中氟奋乃静和氟奋乃静亚砜的水平,结果显示与长效氟奋乃静相比,口服药物时氟奋乃静亚砜的水平要高得多。这些数据说明了口服氟奋乃静后“首过”代谢的作用。因此,在一组随机分配每天接受5毫克、10毫克或25毫克口服氟奋乃静的33名患者中,各剂量下氟奋乃静的稳态血浆水平均显著低于氟奋乃静亚砜或7-羟基氟奋乃静的水平,尽管氟奋乃静和氟奋乃静N4-氧化物的水平之间没有显著差异。另一方面,在相应的一组接受长效药物治疗达到稳态的患者中,母体药物的血浆水平显著高于任何代谢产物的水平。这些观察结果强调了氟奋乃静药代动力学中途径依赖性差异的重要性,这在患者从口服抗精神病药物转换为长效抗精神病药物时可能会导致问题。“致残性副作用”的概念是理解抗精神病药物血浆水平与精神分裂症患者临床反应之间关系的一个重要进展。风险效益分析清楚地表明,评估血浆水平与临床反应之间的关系必须考虑到患者认为对治疗有负面影响的副作用的后果。维持治疗中假定的治疗性血浆水平范围的新数据可能具有潜在的重要性,在低剂量治疗患者的维持治疗中可能特别有用。值得注意的是,在一项对接受氟哌啶醇治疗的难治性患者精心实施的剂量减少研究中,平均最低有效剂量(8.7纳克/毫升)处于急性精神病患者中发现的最佳治疗范围(5纳克/毫升至12纳克/毫升)内。该研究表明对于最初被病房工作人员认为需要高剂量抗精神病药物的慢性难治性精神分裂症患者,逐渐减少抗精神病药物剂量是可行的。(摘要截选至400字)
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3d1/1188605/7fb17db08b50/jpn00056-0017-a.jpg

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