Ekman Bertil, Fitts David, Marelli Claudio, Murray Robert D, Quinkler Marcus, Zelissen Pierre M J
ViroPharma Incorporated, Exton, Pennsylvania, USA.
BMC Endocr Disord. 2014 May 9;14:40. doi: 10.1186/1472-6823-14-40.
Increased morbidity and mortality associated with conventional glucocorticoid replacement therapy for primary adrenal insufficiency (primary AI; estimated prevalence 93-140/million), secondary AI (estimated prevalence, 150-280/million, respectively) or congenital adrenal hyperplasia (estimated prevalence, approximately 65/million) may be due to the inability of typical glucocorticoid treatment regimens to reproduce the normal circadian profile of plasma cortisol. A once-daily modified-release formulation of hydrocortisone has been developed to provide a plasma cortisol profile that better mimics the daytime endogenous profile of cortisol. Here, we describe the protocol for the European Adrenal Insufficiency Registry (EU-AIR), an observational study to assess the long-term safety of modified-release hydrocortisone compared with conventional glucocorticoid replacement therapies in routine clinical practice (ClinicalTrials.gov identifier: NCT01661387).
Patients enrolled in EU-AIR have primary or secondary AI and are receiving either modified-release or conventional glucocorticoid replacement therapy. The primary endpoints of EU-AIR are the incidence of intercurrent illness, adrenal crisis and serious adverse events (SAEs), as well as the duration of SAEs and dose changes related to SAEs. Data relating to morbidity, mortality, adverse drug reactions, dosing and concomitant therapies will be collected. Patient diaries will record illness-related dose changes between visits. All decisions concerning medical care are made by the registry physician and patient. Enrolment is targeted at achieving 3600 patient-years of treatment (1800 patient-years per group) for the primary analysis, which is focused on determining the non-inferiority of once-daily modified-release replacement therapy compared with conventional glucocorticoid therapy.
Recruitment began in August 2012 and, as of March 2014, 801 patients have been enrolled. Fifteen centres are participating in Germany, the UK and Sweden, with recruitment soon to be initiated in the Netherlands.
EU-AIR will provide a unique opportunity not only to collect long-term safety data on a modified-release preparation of glucocorticoid but also to evaluate baseline data on conventional glucocorticoid replacement. Such data should help to improve the treatment of AI.
原发性肾上腺皮质功能减退(原发性 AI;估计患病率为 93 - 140/百万)、继发性 AI(估计患病率分别为 150 - 280/百万)或先天性肾上腺皮质增生(估计患病率约为 65/百万)患者采用传统糖皮质激素替代疗法时,发病率和死亡率增加,可能是因为典型的糖皮质激素治疗方案无法重现血浆皮质醇正常的昼夜节律。已研发出一种氢化可的松每日一次的缓释制剂,以提供更能模拟皮质醇日间内源性水平的血浆皮质醇水平。在此,我们描述欧洲肾上腺皮质功能减退注册研究(EU - AIR)的方案,这是一项观察性研究,旨在评估在常规临床实践中,与传统糖皮质激素替代疗法相比,缓释氢化可的松的长期安全性(ClinicalTrials.gov 标识符:NCT01661387)。
纳入 EU - AIR 的患者患有原发性或继发性 AI,且正在接受缓释或传统糖皮质激素替代疗法。EU - AIR 的主要终点是并发疾病、肾上腺危象和严重不良事件(SAE)的发生率,以及 SAE 的持续时间和与 SAE 相关的剂量变化。将收集有关发病率、死亡率、药物不良反应、给药及伴随治疗的数据。患者日记将记录就诊期间与疾病相关的剂量变化。所有关于医疗护理的决定均由注册研究医生和患者做出。入组目标是为主要分析实现 3600 患者年的治疗(每组 1800 患者年),主要分析重点是确定每日一次的缓释替代疗法与传统糖皮质激素疗法相比的非劣效性。
招募工作于 2012 年 8 月开始,截至 2014 年 3 月,已纳入 801 例患者。德国、英国和瑞典的 15 个中心参与其中,荷兰的招募工作即将启动。
EU - AIR 将提供一个独特的机会,不仅可收集糖皮质激素缓释制剂的长期安全性数据,还能评估传统糖皮质激素替代疗法的基线数据。此类数据应有助于改善 AI 的治疗。
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