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唾液是否可以替代血浆用于癌症患者体内羟考酮及其代谢物的药代动力学研究?

Is saliva a valid substitute for plasma in pharmacokinetic studies of oxycodone and its metabolites in patients with cancer?

机构信息

Department of Palliative and Supportive Care, Mater Health Services, Raymond Terrace, South Brisbane QLD 4101, Australia.

出版信息

Support Care Cancer. 2012 Apr;20(4):767-72. doi: 10.1007/s00520-011-1147-3. Epub 2011 Apr 15.

Abstract

PURPOSE

Little is known about the pharmacokinetics (PKs) of oxycodone in patients with advanced cancer. There is considerable reluctance to subject these patients to non-essential tests including repeated venipuncture that has been necessary in PK studies to date. We investigated the possibility of using saliva sampling as a simple non-invasive test to investigate opioid PKs.

METHODS

Patients with malignant disease receiving oral sustained release (SR) oxycodone at any dose were asked to provide saliva samples at the same time as blood samples. Samples were not taken within 6 h of a dose of immediate release oxycodone. Plasma and saliva oxycodone and metabolite concentrations were measured using HPLC coupled with tandem mass spectrometric detection.

RESULTS

One hundred and thirty-nine paired plasma/saliva samples were collected from 43 cancer patients who had been taking SR oxycodone for more than 5 days at doses ranging from 10 to 600 mg/day (median 40 mg/day). Plasma concentrations of oxycodone and noroxycodone ranged from 1.0 to 256.0 and 0.9-269.4 μg/L, respectively. Salivary concentrations of oxycodone (range 0.93-3,620, mean 336 μg/L) were much higher than plasma concentrations (mean 38.2 μg/L). There was a poor correlation between concentrations of both oxycodone and noroxycodone in plasma and saliva over a range of times following dosing (r (2) = 0.4641 and 0.3891, respectively). No correlation was shown between salivary pH and oxycodone or noroxycodone concentrations. The majority of patients questioned chose saliva sampling over plasma sampling as the preferred method.

CONCLUSION

High levels of both oxycodone and its major metabolite are present in saliva, but this does not provide a valid substitute for plasma when monitoring oxycodone levels for PK studies or therapeutic monitoring.

摘要

目的

关于晚期癌症患者体内羟考酮的药代动力学(PKs)知之甚少。由于迄今为止的 PK 研究需要重复静脉穿刺等非必要的检查,因此患者对此类检查存在较大的抵触情绪。我们研究了使用唾液取样作为简单无创性测试来研究阿片类 PKs 的可能性。

方法

要求接受任何剂量口服控释(SR)羟考酮的恶性肿瘤患者同时提供血液和唾液样本。在服用即时释放羟考酮 6 小时内不采集样本。使用 HPLC 串联质谱检测法测量血浆和唾液中羟考酮和代谢物浓度。

结果

从 43 名接受 SR 羟考酮治疗 5 天以上、剂量范围为 10 至 600mg/天(中位数 40mg/天)的癌症患者中收集了 139 对血浆/唾液样本。羟考酮和去甲羟考酮的血浆浓度范围分别为 1.0 至 256.0 和 0.9 至 269.4μg/L。羟考酮(范围 0.93-3620,平均 336μg/L)的唾液浓度明显高于血浆浓度(平均 38.2μg/L)。在给药后不同时间范围内,血浆和唾液中羟考酮和去甲羟考酮的浓度相关性均较差(r (2)分别为 0.4641 和 0.3891)。唾液 pH 值与羟考酮或去甲羟考酮浓度之间无相关性。大多数被调查的患者选择唾液采样而不是血浆采样作为首选方法。

结论

唾液中同时存在高水平的羟考酮及其主要代谢物,但在监测羟考酮水平用于 PK 研究或治疗监测时,这并不能替代血浆。

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