基于证据的皮下注射阿特珠单抗剂量递减理论。

IF 4.4 3区 医学 Q2 ONCOLOGY
Targeted Oncology Pub Date : 2024-09-01 Epub Date: 2024-07-31 DOI:10.1007/s11523-024-01087-4
Mart P Kicken, Maarten J Deenen, Dirk J A R Moes, Jeroen J M A Hendrikx, Ben E E M van den Borne, Daphne W Dumoulin, Anthonie J van der Wekken, Michiel M van den Heuvel, Rob Ter Heine
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引用次数: 0

摘要

研究背景阿特珠单抗是一种程序性死亡配体1(PD-L1)检查点抑制剂,用于治疗各种癌症。阿特珠单抗的皮下注射制剂最近已获得批准。然而,atezolizumab的治疗费用仍然很高,而需要使用这种药物治疗的患者人数却在不断增加:我们提出了两种皮下注射阿特珠单抗的替代给药方案,以在确保有效暴露的同时降低药物费用;其中一种方案可在临床上直接实施:我们在药代动力学建模和模拟的基础上开发了两种可供选择的剂量间隔延长策略。第一种给药方案基于患者的体重,同时通过遵守美国食品药品管理局(FDA)的硅学剂量调整指南来维持等效的全身药物暴露。第二种给药方案旨在使阿特珠单抗的最低浓度高于6微克/毫升的阈值,同时使至少95%的患者达到95%的瘤内PD-L1受体饱和度:我们发现,就基于体重的给药方案而言,对于体重小于 50 千克的患者,已批准的 3 周给药间隔可延长至 5 周,对于体重 50-65 千克的患者,可延长至 4 周。除了为患者提供更多便利外,这些可供选择的给药间隔还可使美国或欧洲人群的成本分别降低 7% 和 12%。对于第二种给药方案,我们预测 6 周的给药间隔将使 95% 的患者血药浓度高于 6 µg/mL 的阈值,同时成本降低 50%:我们开发并评估了两种可供选择的给药方案,从而降低了成本。我们基于体重的给药方案可以直接实施,并且符合美国食品药品管理局关于 PD-L1 抑制剂替代给药方案的指南。对于针对瘤内 PD-L1 受体阈值的渐进式替代给药方案,在实施前还需要进一步的疗效和安全性证据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

An Evidence-Based Rationale for Dose De-escalation of Subcutaneous Atezolizumab.

An Evidence-Based Rationale for Dose De-escalation of Subcutaneous Atezolizumab.

Background: Atezolizumab is a programmed death-ligand 1 (PD-L1) checkpoint inhibitor for the treatment of different forms of cancer. The subcutaneous formulation of atezolizumab has recently received approval. However, treatment with atezolizumab continues to be expensive, and the number of patients needing treatment with this drug continues to increase.

Objective: We propose two alternative dosing regimens for subcutaneous atezolizumab to reduce drug expenses while ensuring effective exposure; one may be directly implemented in the clinic.

Patients and methods: We developed two alternative dose interval prolongation strategies based on pharmacokinetic modeling and simulation. The first dosing regimen was based on patients' weight while maintaining equivalent systemic drug exposure by adhering to Food and Drug Administration (FDA) guidelines for in silico dose adjustments. The second dosing regimen aimed to have a minimum atezolizumab concentration above the 6 µg/mL threshold, associated with 95% intratumoral PD-L1 receptor saturation for at least 95% of all patients.

Results: We found that, for the weight-based dosing regimen, the approved 3-week dosing interval could be extended to 5 weeks for patients < 50 kg and 4 weeks for patients weighing 50-65 kg. Besides improving patient convenience, these alternative dosing intervals led to a predicted 7% and 12% cost reduction for either the USA or European population. For the second dosing regimen, we predicted that a 6-week dosing interval would result in 95% of the patients above the 6 µg/mL threshold while reducing costs by 50%.

Conclusions: We have developed and evaluated two alternative dosing regimens that resulted in a cost reduction. Our weight-based dosing regimen can be directly implemented and complies with FDA guidelines for alternative dosing regimens of PD-L1 inhibitors. For the more progressive alternative dosing regimen aimed at the intratumoral PD-L1 receptor threshold, further evidence on efficacy and safety is needed before implementation.

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来源期刊
Targeted Oncology
Targeted Oncology 医学-肿瘤学
CiteScore
8.40
自引率
3.70%
发文量
64
审稿时长
>12 weeks
期刊介绍: Targeted Oncology addresses physicians and scientists committed to oncology and cancer research by providing a programme of articles on molecularly targeted pharmacotherapy in oncology. The journal includes: Original Research Articles on all aspects of molecularly targeted agents for the treatment of cancer, including immune checkpoint inhibitors and related approaches. Comprehensive narrative Review Articles and shorter Leading Articles discussing relevant clinically established as well as emerging agents and pathways. Current Opinion articles that place interesting areas in perspective. Therapy in Practice articles that provide a guide to the optimum management of a condition and highlight practical, clinically relevant considerations and recommendations. Systematic Reviews that use explicit, systematic methods as outlined by the PRISMA statement. Adis Drug Reviews of the properties and place in therapy of both newer and established targeted drugs in oncology.
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