Anker Stefan D, Friede Tim, Butler Javed, Talha Khawaja M, Diek Monika, Nosko Anna, Placzek Marius, Hasenfuß Gerd, Ponikowski Piotr, Karakas Mahir
Department of Cardiology (CVK) of German Heart Center Charité, Institute of Health Center for Regenerative Therapies (BCRT), Berlin, Germany.
German Centre for Cardiovascular Research (DZHK) partner site Berlin, Charité Universitätsmedizin, Berlin, Germany.
Eur J Heart Fail. 2025 Apr;27(4):681-689. doi: 10.1002/ejhf.3574. Epub 2025 Jan 28.
While it is widely accepted that intravenous (IV) iron improves functional capacity, symptoms, and cardiovascular outcomes in patients with heart failure (HF) with reduced ejection fraction (HFrEF) diagnosed with iron deficiency (ID), three recently published cardiovascular outcome trials (AFFIRM-AHF, IRONMAN and HEART-FID) of IV iron supplementation in HF failed to demonstrate a significant benefit on their respective primary endpoints. Dosing of IV iron after the initial correction of baseline ID - by design or as a result of trial circumstances - was relatively low (i.e. <500 mg/year). The primary objective of the FAIR-HF2 trial is to evaluate the treatment effect of ferric carboxymaltose (FCM) compared with placebo in ambulatory patients with HFrEF using a higher dose of IV iron during follow-up (i.e. >1000 mg/year). The second objective of the study is to create prospective evidence for patients fulfilling the new definition of ID for patients with HF, i.e. for those with a transferrin saturation <20%.
FAIR-HF2 is an investigator-initiated, multicentre, randomized, double-blind, placebo-controlled trial that has recruited 1105 patients with chronic HF with a left ventricular ejection fraction of ≤45% and concomitant ID, defined as serum ferritin <100 ng/ml or serum ferritin 100-299 ng/ml with a transferrin saturation <20%. Patients were consented and randomized to receive either IV FCM (treatment) or saline (placebo). During an estimated median follow-up of over 2 years, patients underwent a placebo-controlled repletion and maintenance phase, with an initial iron supplementation of up to 2000 mg, followed by 500 mg every 4 months unless stop criteria of haemoglobin >16 mg/dl or serum ferritin >800 ng/ml are met on repeat visits. The trial will evaluate three primary hypotheses: (i) time to first event of cardiovascular death or hospitalization for HF, (ii) the rate of total (first and recurrent) HF hospitalizations (both analysed in the full study population), and (iii) the time to first event of cardiovascular death or hospitalization for HF in patients with a transferrin saturation <20% at baseline. The familywise type I error rate across the three primary endpoint hypotheses will be controlled using the Hochberg procedure (alpha 0.05).
The FAIR-HF2 will evaluate the efficacy of FCM in patients with HFrEF in improving cardiovascular outcomes by utilizing a more aggressive approach towards iron supplementation ensuring prevention of transitional ID after initial repletion targets have been met.
虽然静脉注射铁剂可改善射血分数降低的心力衰竭(HFrEF)且诊断为缺铁(ID)患者的功能能力、症状及心血管结局,这一点已被广泛接受,但最近发表的三项关于HFrEF患者静脉补充铁剂的心血管结局试验(AFFIRM - AHF、IRONMAN和HEART - FID)均未在各自的主要终点上显示出显著益处。因设计或试验情况,在基线ID初步纠正后静脉注射铁剂的剂量相对较低(即<500mg/年)。FAIR - HF2试验的主要目的是评估在随访期间使用更高剂量静脉铁剂(即>1000mg/年)的情况下,与安慰剂相比,羧基麦芽糖铁(FCM)对门诊HFrEF患者的治疗效果。该研究的第二个目的是为符合HFrEF患者ID新定义的患者,即转铁蛋白饱和度<20%的患者,提供前瞻性证据。
FAIR - HF2是一项由研究者发起的多中心、随机、双盲、安慰剂对照试验,招募了1105例左心室射血分数≤45%且伴有ID的慢性心力衰竭患者,ID定义为血清铁蛋白<100ng/ml或血清铁蛋白100 - 299ng/ml且转铁蛋白饱和度<20%。患者签署知情同意书后被随机分组,分别接受静脉注射FCM(治疗组)或生理盐水(安慰剂组)。在估计超过2年的中位随访期间,患者经历了安慰剂对照的补充和维持阶段,初始铁补充量高达2000mg,随后每4个月补充500mg,除非在复诊时满足血红蛋白>16mg/dl或血清铁蛋白>800ng/ml的停药标准。该试验将评估三个主要假设:(i)首次发生心血管死亡或因心力衰竭住院的时间;(ii)总的(首次和复发)心力衰竭住院率(在整个研究人群中分析);(iii)基线时转铁蛋白饱和度<20%的患者首次发生心血管死亡或因心力衰竭住院的时间。将使用霍奇伯格程序(α = 0.05)控制三个主要终点假设的家族性I型错误率。
FAIR - HF2将通过采用更积极的铁补充方法来评估FCM对HFrEF患者改善心血管结局的疗效,确保在达到初始补充目标后预防短暂性ID。
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