口服曲前列尼尔药物基因组学与肺动脉高压患者治疗持续性的初步研究。
A pilot study of oral treprostinil pharmacogenomics and treatment persistence in patients with pulmonary arterial hypertension.
机构信息
University of Pittsburgh School of Pharmacy, Clinical Pharmacist, Cardiology, UPMC Presbyterian Hospital, Salk Hall, Room 727, 3501 Terrace Street, Pittsburgh, PA 15261, USA.
Department of Pharmaceutical Sciences, Center for Clinical Pharmaceutical Sciences, University of Pittsburgh School of Pharmacy, Pittsburgh, PA, USA.
出版信息
Ther Adv Respir Dis. 2021 Jan-Dec;15:17534666211013688. doi: 10.1177/17534666211013688.
BACKGROUND AND AIMS
Treprostinil is a prostacyclin analog used to treat pulmonary arterial hypertension. Dosing is empiric and based on tolerability. Adverse effects are common and can affect treatment persistence. Pharmacogenomic variants that may affect treprostinil metabolism and transport have not been well-characterized. We aimed to investigate the pharmacogenomic sources of variability in treatment persistence and dosing.
METHODS
Patients were prospectively recruited from an IRB approved biobank registry at a single pulmonary hypertension center. A cohort of patients who received oral treprostinil were screened for participation. Pharmacogenomic analysis was for variants in , , and . A retrospective review was conducted for demographics, clinical status, dosing, and response. Fisher's exact test was used for categorical data and Kruskal-Wallis test or Wilcoxon rank sum were used for continuous data.
RESULTS
A total of 15 patients received oral treprostinil and were consented. Their median age was 53 years, 73% were female, and 93% were White. The median total daily dose was 22.5 mg (13.5, 41) at last clinical observation. 40% of patients discontinued treatment with a majority due to adverse effects. Approximately 27% of patients had a loss-of-function variant in (*1/*3 or *1/*4), whereas 47% of patients had a loss-of-function variant in (*1/*2, *1/*3, or *2/*2). Minor allele frequencies for (rs1751034 and rs3742106) were 0.17 and 0.43, respectively. Survival analysis showed that increased CYP2C9 activity score was associated with decreased risk for treatment discontinuation [hazard ratio (HR): 0.13; 95% confidence interval (CI): 0.02, 0.91; = 0.04]. Genetic variants were not significantly associated with dosing.
CONCLUSION
Genetic variants responsible for the metabolism and transport of oral treprostinil were common. Increased CYP2C9 activity score was associated with decreased risk for treatment discontinuation. However, dosing was not associated with genetic variants in metabolizing enzymes for treprostinil. Our findings suggest significant variability in treatment persistence to oral treprostinil, with pharmacogenomics being a potentially important contributor.
背景与目的
曲前列尼尔是一种前列环素类似物,用于治疗肺动脉高压。剂量是经验性的,基于耐受性。不良反应很常见,可能会影响治疗的持续性。尚未充分描述可能影响曲前列尼尔代谢和转运的药物基因组学变异。我们旨在研究治疗持续性和剂量的药物基因组学来源的可变性。
方法
前瞻性地从单一肺动脉高压中心的经机构审查委员会批准的生物银行登记处招募患者。筛选接受口服曲前列尼尔的患者以参与研究。药物基因组学分析针对 、 和 中的变体进行。对人口统计学、临床状况、剂量和反应进行回顾性审查。使用 Fisher 确切检验进行分类数据的分析,使用 Kruskal-Wallis 检验或 Wilcoxon 秩和检验进行连续数据的分析。
结果
共 15 名患者接受口服曲前列尼尔治疗并同意参与研究。他们的中位年龄为 53 岁,73%为女性,93%为白人。在最后一次临床观察时,他们的中位总日剂量为 22.5mg(13.5,41)。40%的患者停止治疗,大多数是由于不良反应。大约 27%的患者在 (*1/*3 或 *1/*4)中存在功能丧失变异,而 47%的患者在 (*1/*2、*1/*3 或 *2/*2)中存在功能丧失变异。 (rs1751034 和 rs3742106)的次要等位基因频率分别为 0.17 和 0.43。生存分析表明,CYP2C9 活性评分增加与治疗停药风险降低相关[风险比(HR):0.13;95%置信区间(CI):0.02,0.91; = 0.04]。遗传变异与剂量无显著相关性。
结论
负责口服曲前列尼尔代谢和转运的遗传变异很常见。CYP2C9 活性评分增加与治疗停药风险降低相关。然而,剂量与曲前列尼尔代谢酶的遗传变异无关。我们的研究结果表明,口服曲前列尼尔的治疗持续性存在显著差异,药物基因组学可能是一个重要的影响因素。
Zotero 插件