硫唑嘌呤代谢物水平与风湿病孕妇的妊娠结局

IF 3.7 2区 医学 Q1 RHEUMATOLOGY Lupus Science & Medicine Pub Date : 2024-01-01 DOI:10.1136/lupus-2023-001036
Stephen Balevic, Catherine A Sims, Amanda Eudy, Valerie Smith, Megan Clowse
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The therapeutic target for 6-TGN was ≥159 pmol/8×108 RBC. Repeated correlation measures were used to evaluate the relationship between metabolite concentrations and pregnancy duration, and the relationship between 6-TGN concentration and SLE Physician Global Assessment (PGA). The relationship between pregnancy average 6-TGN and neonatal gestational age at birth was analysed using linear regression. Results Thirty-seven pregnancies in 35 women with 108 serum samples were included. There was no significant difference in dose-adjusted 6-TGN concentrations across pregnancy and peripartum, whereas 6-MMPN concentrations appeared higher during pregnancy. No elevated transaminases or cholestasis were observed concurrently with 6-MMPN above 5700 pmol/8×108 RBC. Metabolite concentrations were related to total AZA dosage, weight-based dosage and TPMT phenotype. 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引用次数: 0

摘要

尽管硫唑嘌呤(AZA)在妊娠期间被广泛使用,但还没有研究评估了妊娠对风湿病患者 AZA 代谢物 6-硫鸟嘌呤核苷酸(6-TGN)和 6-甲基巯基嘌呤核苷酸(6-MMPN)处置的影响。本研究描述了患有风湿病的妇女在整个孕期中 AZA 代谢物浓度的变化,并探讨了代谢物浓度、母体疾病活动和新生儿预后之间的关系。方法 纳入来自一个中心的风湿病患者,这些患者在怀孕前服用了 AZA,并且在怀孕期间(2016 年 5 月 5 日至 2022 年 4 月 4 日)采集了≥1 份血液样本。商业实验室对 AZA 代谢物浓度进行量化。6-MMPN 的安全上限为 >5700 pmol/8×108 RBC。6-TGN的治疗目标是≥159 pmol/8×108 RBC。重复相关测量用于评估代谢物浓度与妊娠持续时间之间的关系,以及6-TGN浓度与系统性红斑狼疮医生总体评估(PGA)之间的关系。使用线性回归分析了孕期平均 6-TGN 与新生儿出生时胎龄之间的关系。结果 共纳入了 35 名妇女的 37 例妊娠和 108 份血清样本。经剂量调整的 6-TGN 浓度在妊娠期和围产期没有明显差异,而 6-MMPN 浓度在妊娠期更高。在 6-MMPN 超过 5700 pmol/8×108 RBC 的同时,没有观察到转氨酶或胆汁淤积的升高。代谢物浓度与 AZA 总用量、体重用量和 TPMT 表型有关。在平均 6-TGN 达到治疗范围的系统性红斑狼疮孕妇中,我们观察到 PGA 无明显下降,新生儿出生时的胎龄增加。结论 在这项探索性研究中,我们没有观察到 6-TGN 浓度在整个孕期和围产期的系统性变化,而 6-MMPN 浓度在孕期较高。监测妊娠期 AZA 代谢物浓度是一种潜在的工具,可用于识别不遵医嘱用药以及 6-MMPN 偏高的患者,对这些患者进行剂量调整或密切的实验室监测可优化用药安全性。如有合理要求,可提供相关数据。在通讯作者的合理要求下,可提供有限的数据集。
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Azathioprine metabolite levels and outcomes during pregnancies with rheumatic disease
Objective Despite widespread use of azathioprine (AZA) during pregnancy, no studies evaluated the impact of pregnancy on AZA metabolites 6-thioguanine nucleotide (6-TGN) and 6-methylmercaptopurine nucleotide (6-MMPN) disposition in rheumatic diseases. This study characterises changes in AZA metabolite concentrations throughout pregnancy in women with rheumatic disease and explores relationships between metabolite concentrations, maternal disease activity, and neonatal outcomes. Methods Patients with rheumatic disease from a single centre prescribed AZA prior to pregnancy and ≥1 blood sample during pregnancy (5/2016 to 4/2022) were included. Commercial laboratories quantified AZA metabolite concentrations. The upper safety limit for 6-MMPN was >5700 pmol/8×108 RBC. The therapeutic target for 6-TGN was ≥159 pmol/8×108 RBC. Repeated correlation measures were used to evaluate the relationship between metabolite concentrations and pregnancy duration, and the relationship between 6-TGN concentration and SLE Physician Global Assessment (PGA). The relationship between pregnancy average 6-TGN and neonatal gestational age at birth was analysed using linear regression. Results Thirty-seven pregnancies in 35 women with 108 serum samples were included. There was no significant difference in dose-adjusted 6-TGN concentrations across pregnancy and peripartum, whereas 6-MMPN concentrations appeared higher during pregnancy. No elevated transaminases or cholestasis were observed concurrently with 6-MMPN above 5700 pmol/8×108 RBC. Metabolite concentrations were related to total AZA dosage, weight-based dosage and TPMT phenotype. In pregnant women with SLE achieving average 6-TGN in the therapeutic range, we observed a non-significant reduction in PGA and increase in neonatal gestational age at birth. Conclusions In this exploratory study, we did not observe systematic changes in 6-TGN concentrations throughout pregnancy and peripartum, whereas 6-MMPN concentrations were higher during pregnancy. Monitoring AZA metabolite concentrations in pregnancy is a potential tool to identify medication non-adherence as well as patients with high 6-MMPN in whom dosage adjustment or close laboratory monitoring may optimise safety. Data are available upon reasonable request. A limited dataset may be made available upon reasonable request of the corresponding author.
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来源期刊
Lupus Science & Medicine
Lupus Science & Medicine RHEUMATOLOGY-
CiteScore
5.30
自引率
7.70%
发文量
88
审稿时长
15 weeks
期刊介绍: Lupus Science & Medicine is a global, peer reviewed, open access online journal that provides a central point for publication of basic, clinical, translational, and epidemiological studies of all aspects of lupus and related diseases. It is the first lupus-specific open access journal in the world and was developed in response to the need for a barrier-free forum for publication of groundbreaking studies in lupus. The journal publishes research on lupus from fields including, but not limited to: rheumatology, dermatology, nephrology, immunology, pediatrics, cardiology, hepatology, pulmonology, obstetrics and gynecology, and psychiatry.
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