Lomitapide: A Medication Use Evaluation and a Formulary Perspective

Laila Carolina Abu Esba, Hani Alharbi
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Abstract

Lomitapide is approved for lowering low-density lipoprotein cholesterol (LDL-C) in homozygous familial hypercholesterolemia, which is a rare genetic disorder. The evidence regarding its safety and efficacy from a small clinical trial requires further validation for effectiveness and safety in the real world. This study aimed to use institutional data on the effectiveness and safety of lomitapide to assist in formulating a perspective on adding it to the formulary. This was a retrospective review of patients who were actively prescribed lomitapide at King Abdulaziz Medical City, Riyadh, Saudi Arabia, from 2019 to 2022. Data collection included demographics, confirmed gene mutation results, duration of lomitapide therapy, baseline, on-treatment, last LDL-C levels, percent reduction in LDL-C after 1-3 months of therapy (whichever was first available), other LDL-C lowering therapies used, liver function tests, adverse effects, and compliance. Eight adult patients were included in the review, with a mean age of 25.5 years. Approximately 75% were female, and the duration of treatment with lomitapide ranged from 9 months to 3 years. None of the patients were on continuous LDL apheresis. The mean baseline LDL-C at presentation to our facility was 17.2 mmol/L (range, 11.78–21.97 mmol/L), the mean percent drop in LDL-C with lomitapide was 34.1% (range, 0%–87%), gastrointestinal disturbances were documented in 50% of the patients, and no cases of severe liver toxicities or increase in liver enzymes were seen. In our cohort of adult patients, lomitapide showed an overall modest reduction in LDL-C, with no cases of increase in liver enzymes and documented intolerance, indicating that most patients were likely noncompliant. This review revealed important considerations when reimbursing expensive medications for rare diseases. Real-world evidence in real-time can support healthcare systems in price negotiations and reaching mutual agreements that can eventually improve patient access to care.
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洛米他匹:用药评估和处方集视角
洛米他匹获准用于降低同卵家族性高胆固醇血症(一种罕见的遗传性疾病)患者的低密度脂蛋白胆固醇(LDL-C)。从一项小型临床试验中获得的有关其安全性和有效性的证据需要在现实世界中进一步验证其有效性和安全性。本研究旨在利用有关洛米他匹的有效性和安全性的机构数据,协助制定将其纳入处方集的观点。 本研究对沙特阿拉伯利雅得阿卜杜勒阿齐兹国王医疗城在2019年至2022年期间积极处方洛米他肽的患者进行了回顾性审查。收集的数据包括人口统计学特征、确诊基因突变结果、洛米他匹治疗持续时间、基线、治疗中、最后LDL-C水平、治疗1-3个月后LDL-C降低百分比(以最先获得的数据为准)、使用的其他降低LDL-C疗法、肝功能检测、不良反应和依从性。 本次研究共纳入了 8 名成年患者,平均年龄为 25.5 岁。约75%的患者为女性,使用洛米他匹治疗的时间从9个月到3年不等。所有患者均未持续进行低密度脂蛋白清除治疗。来我院就诊时的平均基线 LDL-C 为 17.2 mmol/L(范围为 11.78-21.97 mmol/L),使用洛美他肽后 LDL-C 的平均降幅为 34.1%(范围为 0%-87%),50% 的患者出现胃肠道紊乱,未发现严重肝毒性或肝酶升高的病例。 在我们的成年患者队列中,洛米他匹总体上显示出低密度脂蛋白胆固醇的适度降低,没有肝酶升高的病例,也没有不耐受的记录,这表明大多数患者可能没有遵从医嘱。本综述揭示了罕见病昂贵药物报销时的重要注意事项。真实世界的实时证据可以支持医疗系统进行价格谈判并达成相互协议,从而最终改善患者获得护理的机会。
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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