目标剂量:HEAL试验中缺氧缺血性脑病新生儿的促红细胞生成素暴露情况
On target dosing: erythropoietin exposure in neonates with hypoxic-ischemic encephalopathy in the HEAL trial.
作者信息
Frymoyer Adam, Vasconcelos Ana Gabriela, Juul Sandra E, Comstock Bryan A, Heagerty Patrick J, Wu Yvonne W
机构信息
Department of Pediatrics, Stanford University, Palo Alto, CA, USA.
Department of Biostatistics, University of Washington, Seattle, WA, USA.
出版信息
Pediatr Res. 2024 Nov 10. doi: 10.1038/s41390-024-03709-z.
BACKGROUND
The High-Dose Erythropoietin for Asphyxia and Encephalopathy (HEAL) trial for neonates with hypoxic-ischemic encephalopathy (HIE) treated with therapeutic hypothermia demonstrated no neurodevelopmental benefit but was associated with a higher rate of serious adverse events (SAEs). Understanding if targeted Epo plasma exposures were achieved in the HEAL trial and if SAEs were associated with higher exposures would help future therapeutic programs of Epo as a candidate neuroprotective treatment.
METHODS
Ancillary study of a subset of HEAL neonates who received Epo (1000 U/kg IV on days 1, 2, 3, 4, and 7) and had plasma drug concentrations measured. Within a Bayesian pharmacokinetic framework, the area under the curve during the first 48 h (AUC) and 7 days (AUC) of treatment was estimated. The % of neonates who achieved animal model neuroprotective targets of AUC >140,000 mUh/ml and AUC >420,000 mUh/ml was calculated. The relationship between AUC and SAEs after study drug was evaluated using logistic regression.
RESULTS
Among n = 89 neonates, variation in Epo exposure was low, and over 95% of neonates achieved the target AUC and AUC. No meaningful relationship was seen between AUC and risk of SAE.
CONCLUSIONS
The Epo dosing strategy in the HEAL trial consistently achieved target plasma exposures. Higher exposures were not associated with SAEs.
IMPACT
In the HEAL randomized, placebo-controlled trial of high-dose erythropoietin (Epo) for neonates with hypoxic-ischemic encephalopathy (HIE) receiving therapeutic hypothermia, the Epo dosing strategy achieved animal model neuroprotective plasma exposure targets in >95% of neonates. This understanding further strengthens the HEAL trial's primary conclusion that Epo provides no additional benefit in neonates with HIE also receiving therapeutic hypothermia. While Epo treatment was associated with a higher rate of serious adverse events (SAEs) compared to placebo in the primary HEAL trial, higher plasma exposures of Epo were not associated with the risk of SAEs.
背景
针对接受治疗性低温治疗的缺氧缺血性脑病(HIE)新生儿的大剂量促红细胞生成素治疗窒息和脑病(HEAL)试验显示,该治疗对神经发育无益处,但与较高的严重不良事件(SAE)发生率相关。了解HEAL试验中是否达到了促红细胞生成素(Epo)的目标血浆暴露水平,以及SAE是否与更高的暴露水平相关,将有助于未来将Epo作为候选神经保护治疗的治疗方案。
方法
对HEAL试验中接受Epo治疗(在第1、2、3、4和7天静脉注射1000 U/kg)并测量血浆药物浓度的一部分新生儿进行辅助研究。在贝叶斯药代动力学框架内,估计治疗前48小时(AUC)和7天(AUC)的曲线下面积。计算达到动物模型神经保护目标AUC>140,000 mUh/ml和AUC>420,000 mUh/ml的新生儿百分比。使用逻辑回归评估研究药物后AUC与SAE之间的关系。
结果
在n = 89例新生儿中,Epo暴露的变异性较低,超过95%的新生儿达到了目标AUC和AUC。未发现AUC与SAE风险之间存在有意义的关系。
结论
HEAL试验中的Epo给药策略始终达到了目标血浆暴露水平。较高的暴露水平与SAE无关。
影响
在针对接受治疗性低温治疗的缺氧缺血性脑病(HIE)新生儿的HEAL随机、安慰剂对照高剂量促红细胞生成素(Epo)试验中,Epo给药策略在超过95%的新生儿中达到了动物模型神经保护血浆暴露目标。这一认识进一步强化了HEAL试验的主要结论,即Epo对同时接受治疗性低温治疗的HIE新生儿没有额外益处。虽然在主要的HEAL试验中,与安慰剂相比,Epo治疗与更高的严重不良事件(SAE)发生率相关,但更高的Epo血浆暴露水平与SAE风险无关。
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