Optimizing the therapeutic window of sirolimus by monitoring blood concentration for the treatment of immune thrombocytopenia.

IF 2.5 3区 医学 Q3 CELL BIOLOGY
Platelets Pub Date : 2023-12-01 Epub Date: 2023-11-20 DOI:10.1080/09537104.2023.2277831
Yun Zhang, Yao Quan, Dan Wang, Kaniel Cassady, Wenhang Zou, Jingkang Xiong, Han Yao, Xiaojuan Deng, Ping Wang, Shijie Yang, Xi Zhang, Yimei Feng
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Abstract

Previous studies have demonstrated that sirolimus (SRL) is an effective agent for the treatment of refractory/relapsed (R/R) ITP. However, the therapeutic window of sirolimus in the treatment of ITP has not been established. As the toxicity of sirolimus increases with higher blood concentrations, it is crucial to determine the optimal therapeutic concentration of SRL for the treatment of ITP. Thus, in this study, we used a retrospective cohort of ITP patients treated with sirolimus to propose the therapeutic dosage window for sirolimus. A total of 275 laboratory results of SRL blood concentration from 63 ITP patients treated with SRL were analyzed retrospectively. The ITP patients were divided into five groups based on their SRL blood concentration: 0-4 ng/ml, 4-8 ng/ml, 8-12 ng/ml, 12-16 ng/ml and ≥16 ng/ml. In addition to the SRL blood concentration, platelet counts and adverse events that occurred during the first 6 weeks of SRL treatment were analyzed. These findings were then used to establish the decision matrix tables and ROC curves, which helped identify the therapeutic window of SRL. Based on the values and trends of true-positive rate (TPR) and false-positive rate (FPR) in the ROC curve, patients who achieved a SRL blood concentration of 4-12 ng/ml displayed a higher response rate compared to those with a SRL concentration of 0-4 ng/ml or ≥16ng/ml. Additionally, the response rate was better for patients with a SRL concentration of 8-12 ng/ml compared to 4-8 ng/ml. Adverse events were related to the concentration of SRL; however, there was no significant difference in the incidence of adverse events between the concentrations of 4-8 ng/ml and 8-12 ng/ml (P > .05). Regression analysis suggested that the concentration of SRL correlated with the patient's age, PLT count at the start of SRL administration, and the dose of SRL. It is suggested that the optimal blood concentration of SRL monotherapy for managing ITP is 8-12 ng/ml. This range may achieve a favorable balance between clinical efficacy and the severity of adverse events.

通过监测血药浓度优化西罗莫司治疗免疫性血小板减少症的治疗窗口。
以往的研究表明,西罗莫司(SRL)是治疗难治性/复发性(R/R)ITP的有效药物。然而,西罗莫司治疗 ITP 的治疗窗口期尚未确定。由于西罗莫司的毒性会随着血药浓度的升高而增加,因此确定SRL治疗ITP的最佳治疗浓度至关重要。因此,在本研究中,我们利用西罗莫司治疗 ITP 患者的回顾性队列,提出了西罗莫司的治疗剂量窗。我们对63名接受西罗莫司治疗的ITP患者的275份西罗莫司血药浓度化验结果进行了回顾性分析。根据 SRL 血液浓度将 ITP 患者分为五组:0-4纳克/毫升、4-8纳克/毫升、8-12纳克/毫升、12-16纳克/毫升和≥16纳克/毫升。除 SRL 血液浓度外,还分析了血小板计数和 SRL 治疗头 6 周内发生的不良事件。然后利用这些结果建立了决策矩阵表和 ROC 曲线,有助于确定 SRL 的治疗窗口期。根据ROC曲线中真阳性率(TPR)和假阳性率(FPR)的数值和趋势,与SRL浓度为0-4ng/ml或≥16ng/ml的患者相比,SRL血药浓度达到4-12ng/ml的患者反应率更高。此外,与 SRL 浓度为 4-8 纳克/毫升的患者相比,SRL 浓度为 8-12 纳克/毫升的患者的应答率更高。不良反应与 SRL 的浓度有关;但是,4-8 ng/ml 和 8-12 ng/ml 浓度之间的不良反应发生率没有显著差异(P > .05)。回归分析表明,SRL 的浓度与患者的年龄、开始服用 SRL 时的 PLT 计数和 SRL 的剂量相关。有研究表明,SRL 单药治疗 ITP 的最佳血药浓度为 8-12 纳克/毫升。这一范围可在临床疗效和不良反应的严重程度之间取得良好的平衡。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Platelets
Platelets 医学-细胞生物学
CiteScore
6.70
自引率
3.00%
发文量
79
审稿时长
1 months
期刊介绍: Platelets is an international, peer-reviewed journal covering all aspects of platelet- and megakaryocyte-related research. Platelets provides the opportunity for contributors and readers across scientific disciplines to engage with new information about blood platelets. The journal’s Methods section aims to improve standardization between laboratories and to help researchers replicate difficult methods. Research areas include: Platelet function Biochemistry Signal transduction Pharmacology and therapeutics Interaction with other cells in the blood vessel wall The contribution of platelets and platelet-derived products to health and disease The journal publishes original articles, fast-track articles, review articles, systematic reviews, methods papers, short communications, case reports, opinion articles, commentaries, gene of the issue, and letters to the editor. Platelets operates a single-blind peer review policy. Authors can choose to publish gold open access in this journal.
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