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硫嘌呤甲基转移酶酶活性的生物学变异:何时发生了显著变化?

Biological variation of thiopurine methyltransferase enzyme activity: when has a significant change taken place?

机构信息

Department of Clinical Pharmacology, Christchurch Hospital, New Zealand.

出版信息

Ann Clin Biochem. 2013 Sep;50(Pt 5):473-8. doi: 10.1177/0004563212473441. Epub 2013 Jun 17.

DOI:10.1177/0004563212473441
PMID:23774052
Abstract

BACKGROUND

Thiopurine methyltransferase (TPMT) enzyme activity is measured before initiating thiopurine therapy to reduce the risk of severe drug-associated myelotoxicity in patients with low enzyme activity. TPMT activity may vary over time in relation to drug treatment and patient clinical condition. What constitutes a significant change in TPMT activity can be derived from biological variation and analytical imprecision.

METHODS

A large national laboratory database was used to identify patients with three or more TPMT activity measurements. Variance of TPMT activity was analysed by determining the total coefficient of variation (CVTOT) of repeated measurements and by correlation with parameters including gender and follow-up time. Between-run analytical imprecision (CVa) was determined by replicate analysis (n = 314).

RESULTS

Of 7383 patients with TPMT measurements, 136 were identified as having three or more measurements over time (range 3-14). Median CVTOT for individual patient results was 14.5% (range 2.5-36.7%). Analytical imprecision (CVa) was 10.3%. A reference change value (or critical difference) with 95% probability was calculated as 42%. Therefore, a change in measured TPMT activity above 42% should lead to considering sources of variation other than biological variation and analytical imprecision.

CONCLUSIONS

TPMT enzyme activity needs to change by at least 42% to determine that a true change has taken place beyond biological variation and analytical imprecision. A single measurement of TPMT activity is sufficient for most clinical purposes.

摘要

背景

在开始使用硫嘌呤甲基转移酶(TPMT)酶治疗之前,需要测量该酶的活性,以降低低酶活性患者发生严重药物相关骨髓毒性的风险。TPMT 活性可能会随着药物治疗和患者临床状况的变化而发生变化。什么构成 TPMT 活性的显著变化,可以从生物学变异性和分析不精密度中得出。

方法

使用大型国家实验室数据库来确定有三个或更多 TPMT 活性测量值的患者。通过确定重复测量的总变异系数(CVTOT)以及与性别和随访时间等参数的相关性,分析 TPMT 活性的变异性。通过重复分析(n = 314)确定批间分析不精密度(CVa)。

结果

在 7383 名接受 TPMT 测量的患者中,有 136 名患者被确定为在一段时间内进行了三次或更多次测量(范围为 3-14 次)。单个患者结果的中位 CVTOT 为 14.5%(范围为 2.5-36.7%)。分析不精密度(CVa)为 10.3%。计算出 95%概率的参考变化值(或临界差值)为 42%。因此,测量的 TPMT 活性变化超过 42%,应该导致考虑除生物学变异性和分析不精密度之外的其他变异源。

结论

TPMT 酶活性需要至少变化 42%,才能确定发生了真正的变化,而不仅仅是生物学变异性和分析不精密度。大多数临床目的只需要单次 TPMT 活性测量即可。

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