A Refined Population Pharmacokinetic Model-Based Guideline for Individualized PEGasparaginase Dosing in Pediatric Acute Lymphoblastic Leukemia.

IF 2.8 4区医学 Q2 MEDICAL LABORATORY TECHNOLOGY

Therapeutic Drug Monitoring Pub Date : 2024-08-13 DOI:10.1097/FTD.0000000000001252

Leiah J Brigitha, Karen Zaky, Rob Pieters, Inge M van der Sluis

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Abstract

Background: In the Dutch Childhood Oncology Group ALL11 protocol, PEGasparaginase dosing was individualized for standard-risk and medium-risk patients with acute lymphoblastic leukemia. After using our pragmatic old guideline, we aimed to improve individualized PEGasparaginase dosing by developing a population pharmacokinetic model-based dosing guideline.

Method: After the 3 doses of 1500 IU/m2 administered in induction, standard-risk patients received 1 individualized dose and medium-risk patients 14, targeting trough activity levels between 100 and 250 IU/L. The effectiveness, adherence, and toxicity of our new dosing guideline was assessed and compared with the old guideline.

Results: In total, 92 patients (714 samples) were included in the new dosing group and 509 patients (4539 samples) were included in the old dosing group. Comparing the effectiveness, we found that 32% (22/67) of patients in the new and 13% (47/354) of patients in the old dosing group were within the target range after the first individualized dose (P < 0.001). Among medium-risk patients, a median of 3 dose reductions was needed to reach and maintain levels within the target range in the new dosing group compared with 5 in the old dosing group (P < 0.001). With a continuous PEGasparaginase dosing schedule, target trough activity levels were reached after 2 dose reductions in the new group versus 4 in the old dosing group. The adherence to the new guideline was >99%, with 6/714 recommended doses deviating from the guideline. With exception of a lower proportion of patients with increased (≥grade 3) serum alanine transaminase (34% new vs 64% old, P < 0.05) in the new dosing group, toxicity was comparable between guidelines.

Conclusions: With the new dosing guideline, fewer dose-reduction steps are necessary to reach and remain within the target. The high adherence rate emphasized its simplicity and practicality, confirming that it can be easily integrated into clinical practice.

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基于人群药代动力学模型的儿科急性淋巴细胞白血病患者PEG天冬酰胺酶个体化用药指南。

背景：在荷兰儿童肿瘤学组 ALL11 方案中，PEGasparaginase 剂量是针对标准风险和中度风险急性淋巴细胞白血病患者的个体化剂量。在使用我们实用的旧指南后，我们旨在通过制定基于群体药代动力学模型的剂量指南来改进 PEG 天冬酰胺酶的个体化剂量：在诱导期给予 3 次 1500 IU/m2 剂量后，标准风险患者接受 1 次个体化剂量，中度风险患者接受 14 次个体化剂量，目标活性谷值在 100 到 250 IU/L 之间。我们对新剂量指南的有效性、依从性和毒性进行了评估，并与旧指南进行了比较：共有 92 名患者（714 个样本）被纳入新剂量组，509 名患者（4539 个样本）被纳入旧剂量组。通过比较疗效，我们发现新剂量组中 32% 的患者（22/67）和旧剂量组中 13% 的患者（47/354）在首次个体化剂量后处于目标范围内（P < 0.001）。在中危患者中，新剂量组需要减少 3 次剂量才能达到并维持在目标范围内，而旧剂量组需要减少 5 次剂量才能达到并维持在目标范围内（P < 0.001）。在 PEGasparaginase 持续给药计划中，新给药组患者在减少 2 次剂量后即可达到目标谷值活性水平，而旧给药组患者则需要减少 4 次剂量。新指南的依从性大于 99%，6/714 例患者的推荐剂量偏离了指南。除了新剂量组血清丙氨酸转氨酶升高（≥3级）的患者比例较低（新剂量组为34%，旧剂量组为64%，P＜0.05）外，两种指南的毒性具有可比性：结论：采用新的给药指南后，为达到并保持在目标值内所需的剂量减少步骤更少。较高的遵守率强调了其简便性和实用性，证明它可以很容易地融入临床实践中。

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

Therapeutic Drug Monitoring 医学-毒理学

CiteScore

5.00

自引率

8.00%

发文量

213

审稿时长

4-8 weeks

期刊介绍： Therapeutic Drug Monitoring is a peer-reviewed, multidisciplinary journal directed to an audience of pharmacologists, clinical chemists, laboratorians, pharmacists, drug researchers and toxicologists. It fosters the exchange of knowledge among the various disciplines–clinical pharmacology, pathology, toxicology, analytical chemistry–that share a common interest in Therapeutic Drug Monitoring. The journal presents studies detailing the various factors that affect the rate and extent drugs are absorbed, metabolized, and excreted. Regular features include review articles on specific classes of drugs, original articles, case reports, technical notes, and continuing education articles.

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