早期评估硫嘌呤代谢物可识别炎症性肠病中硫嘌呤诱导白细胞减少症的风险患者。
Early Assessment of Thiopurine Metabolites Identifies Patients at Risk of Thiopurine-induced Leukopenia in Inflammatory Bowel Disease.
机构信息
Department of Clinical Pharmacy, Pharmacology and Toxicology, Zuyderland Medical Center, Sittard-Geleen, The Netherlands
Department of Human Genetics, Radboud University Medical Center, Nijmegen, The Netherlands.
出版信息
J Crohns Colitis. 2017 Feb;11(2):175-184. doi: 10.1093/ecco-jcc/jjw130. Epub 2016 Jul 9.
BACKGROUND AND AIMS
Only a quarter of thiopurine-induced myelotoxicity in inflammatory bowel disease [IBD] patients is related to thiopurine S-methyltransferase deficiency. We determined the predictive value of 6-thioguanine nucleotide [6-TGN] and 6-methylmercaptopurine ribonucleotide [6-MMPR] concentrations 1 week after initiation [T1] for development of leukopenia during the first 8 weeks of thiopurine treatment.
METHODS
The study was performed in IBD patients starting thiopurine therapy as part of the Dutch randomized controlled TOPIC trial [ClinicalTrials.gov NCT00521950]. Blood samples for metabolite measurement were collected at T1. Leukopenia was defined by leukocyte counts of <3.0 × 10/L. For comparison, patients without leukopenia who completed the 8 weeks on the stable dose were selected from the first 272 patients of the TOPIC trial.
RESULTS
Thirty-two patients with, and 162 patients without leukopenia were analysed. T1 threshold 6-TGN concentrations of 213 pmol/8 × 10 erythrocytes and 3525 pmol/8 × 10 erythrocytes for 6-MMPR were defined: patients exceeding these values were at increased leukopenia risk (odds ratio [OR] 6.2 [95% CI: 2.8-13.8] and 5.9 [95% CI: 2.7-13.3], respectively). Leukopenia rates were higher in patients treated with mercaptopurine, compared with azathioprine (OR 7.3 [95% CI: 3.1-17.0]), and concurrent anti-TNF therapy (OR 5.1 [95% CI: 1.6-16.4]). Logistic regression analysis of thiopurine type, threshold concentrations, and concurrent anti-tumour necrosis factor [TNF] therapy revealed that elevations of both T1 6-TGN and 6-MMPR resulted in the highest risk for leukopenia, followed by exceeding only the T1 6-MMPR or 6-TGN threshold concentration (area under the curve 0.84 [95% CI: 0.76-0.92]).
CONCLUSIONS
In ~80% of patients, leukopenia could be explained by T1 6-TGN and/or 6-MMPR elevations. Validation of the predictive model is needed before implementing in clinical practice.
背景与目的
在炎症性肠病(IBD)患者中,仅有四分之一的巯嘌呤诱导的骨髓毒性与巯嘌呤 S-甲基转移酶缺乏有关。我们测定了在开始使用巯嘌呤治疗后 1 周(T1)时 6-硫鸟嘌呤核苷酸(6-TGN)和 6-甲基巯基嘌呤核糖核苷酸(6-MMPR)浓度对前 8 周巯嘌呤治疗期间白细胞减少症发生的预测价值。
方法
本研究在开始巯嘌呤治疗的 IBD 患者中进行,该研究是荷兰随机对照 TOPIC 试验(ClinicalTrials.gov NCT00521950)的一部分。在 T1 时采集用于代谢物测量的血样。白细胞减少症定义为白细胞计数<3.0×10/L。为了进行比较,从 TOPIC 试验的前 272 例患者中选择了未发生白细胞减少症且完成 8 周稳定剂量治疗的患者。
结果
对 32 例发生白细胞减少症的患者和 162 例未发生白细胞减少症的患者进行了分析。T1 时 6-TGN 浓度超过 213 pmol/8×10 个红细胞和 3525 pmol/8×10 个红细胞,6-MMPR 浓度超过这两个值的患者发生白细胞减少症的风险增加(比值比 [OR] 6.2[95%CI:2.8-13.8]和 5.9[95%CI:2.7-13.3])。与硫唑嘌呤相比,使用巯嘌呤治疗的患者白细胞减少症发生率更高(OR 7.3[95%CI:3.1-17.0]),并且与同时使用抗 TNF 治疗相比(OR 5.1[95%CI:1.6-16.4])。对巯嘌呤类型、阈值浓度和同时使用抗肿瘤坏死因子 [TNF] 治疗进行逻辑回归分析表明,T1 时 6-TGN 和/或 6-MMPR 升高均导致白细胞减少症风险最高,其次是仅超过 T1 时 6-MMPR 或 6-TGN 阈值浓度(曲线下面积 0.84[95%CI:0.76-0.92])。
结论
在约 80%的患者中,白细胞减少症可以用 T1 时 6-TGN 和/或 6-MMPR 升高来解释。在将预测模型付诸临床实践之前,需要对其进行验证。
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