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基于药物遗传学的格列美脲治疗 2 型糖尿病:成本效益研究。

Pharmacogenetic-guided glimepiride therapy in type-2 diabetes mellitus: a cost-effectiveness study.

机构信息

Groupement Hospitalier Nord, Service de Pharmacie, Hospices Civils de Lyon, Lyon, France.

Pôle de santé publique, Service d'évaluation économique en santé, Hospices Civils de Lyon, Lyon, France.

出版信息

Pharmacogenomics J. 2021 Oct;21(5):559-565. doi: 10.1038/s41397-021-00232-w. Epub 2021 Mar 17.

Abstract

The demonstration of the link between certain genetic variations and drug response has allowed the emergence of pharmacogenetics, which offers many opportunities to improve patient care. Type-2 diabetes mellitus is a disease for which several gene polymorphisms have been reported to be associated with drug response. Sulfonylureas are commonly used for the management of this disease. Genetic polymorphisms of CYP2C9, the main enzyme involved in the metabolism of sulfonylureas, have been associated with the risk of severe hypoglycaemia, particularly in poor metabolizers carrying CYP2C9 *3/*3 genotype, and especially in the case of patients treated with glimepiride. The objectives of the present study were to evaluate the potential clinical and economic outcomes of using CYP2C9 genotype data to guide the management of SU regimen in patients initiating glimepiride therapy, and to identify factors affecting the cost-effectiveness of this treatment scheme. The analysis was conducted using a decision tree, considering a 1-year time horizon, and taking as perspective that of the French national health insurance system. With pharmacogenetic-guided therapy, the cost to avoid an episode of severe hypoglycaemia event per 100 000 patients treated was €421 834. Genotyping cost was the most influential factor on the incremental cost-effectiveness ratio. In conclusion, the potential cost of CYP2C9 genotype-guided dosing for glimepiride therapy is relatively high, and associated with modest improvements with respect to the number of hypoglycaemia avoided, as compared with standard dosing. Additional economic studies are required to better specify the usefulness of CYP2C9 genotyping prior to glimepiride regimen initiation.

摘要

某些基因变异与药物反应之间的联系的证明催生了药物遗传学,这为改善患者治疗带来了许多机会。2 型糖尿病是一种与药物反应相关的基因多态性已被报道的疾病。磺酰脲类药物通常用于治疗这种疾病。磺酰脲类药物代谢中主要酶 CYP2C9 的遗传多态性与严重低血糖的风险相关,特别是在携带 CYP2C9 *3/*3 基因型的代谢不良者中,尤其是在使用格列美脲治疗的患者中。本研究的目的是评估使用 CYP2C9 基因型数据指导格列美脲治疗起始时 SU 方案管理的潜在临床和经济结局,并确定影响该治疗方案成本效益的因素。使用决策树进行了分析,考虑了 1 年的时间范围,并从法国国家健康保险系统的角度考虑。采用药物遗传学指导治疗,每 100000 名接受治疗的患者避免严重低血糖事件的成本为 421834 欧元。基因分型成本是对增量成本效益比影响最大的因素。总之,与标准剂量相比,CYP2C9 基因型指导格列美脲治疗剂量的潜在成本相对较高,并且与避免低血糖的数量适度改善相关。在开始格列美脲方案之前,需要进行更多的经济研究以更好地确定 CYP2C9 基因分型的有用性。

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