Lung transplant outcomes for recipients with alpha-1 antitrypsin deficiency, by use of alpha-1 antitrypsin augmentation therapy

JHLT Open Pub Date : 2025-02-01 DOI:10.1016/j.jhlto.2024.100201

Atharv V. Oak MEng , Jessica M. Ruck MD, PhD , Alfred J. Casillan MD, PhD , Armaan F. Akbar BS , Ramon A. Riojas MD, PhD , Pali D. Shah MD , Jinny S. Ha MD, MHS , Sara Strout PharmD , Allan B. Massie PhD , Dorry L. Segev MD, PhD , Christian A. Merlo MD, MPH , Errol L. Bush MD

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Abstract

Background

For patients with alpha-1 antitrypsin (AAT) deficiency, AAT augmentation therapy can be an important part of care. However, for those who require a lung transplant (LT), there is currently only limited information to guide the use of AAT augmentation therapy post-LT.

Methods

We identified all LT recipients from 2011-2021 in the Scientific Registry of Transplant Recipients with an AAT deficiency diagnosis. We categorized recipients by use of AAT augmentation therapy post-LT and compared their baseline characteristics using Fisher’s exact test and Wilcoxon rank-sum tests. We used Kaplan-Meier analyses and estimated the average treatment effect (ATE) of post-LT AAT augmentation therapy on mortality and all-cause graft failure (ACGF). The ATE measures the observed effect we would see if everyone in the population received the intervention as opposed to just a subset.

Results

Among the 447 recipients with AAT deficiency, 109 used AAT augmentation therapy pre-LT, of which 32 (29.4%) continued post-LT. Recipients who used augmentation therapy post-LT were younger (56.5 [53-59.75] vs 57 [53.75-63], p = 0.04) and had shorter ischemia time (mean 311 vs 363 minutes, p = 0.03) than those who did not. The age-adjusted ATE estimate of post-LT augmentation therapy use on time to death and ACGF was +1.69 and +1.48 years, respectively. Post-LT augmentation therapy use was associated with a mortality reduction in the top quartile bilirubin subgroup (p = 0.02, log-rank test).

Conclusions

In our study, the use of augmentation therapy post-LT was associated with improved survival. Confirmatory prospective studies should be considered to inform post-LT AAT therapy guidelines.

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α -1抗胰蛋白酶增强治疗对α -1抗胰蛋白酶缺乏症患者肺移植结果的影响

背景：对于α -1抗胰蛋白酶（AAT）缺乏的患者，AAT增强治疗可能是护理的重要组成部分。然而，对于那些需要肺移植（LT）的患者，目前只有有限的信息来指导移植后AAT增强治疗的使用。方法：我们在2011-2021年移植受者科学登记中确定所有AAT缺陷诊断的肝移植受者。我们通过肝移植后AAT增强治疗对受者进行分类，并使用Fisher精确检验和Wilcoxon秩和检验比较他们的基线特征。我们使用Kaplan-Meier分析并估计了lt后AAT增强治疗对死亡率和全因移植物衰竭（ACGF）的平均治疗效果（ATE）。ATE衡量的是观察到的效果如果人群中的每个人都接受了干预而不是一小部分人。结果447例AAT缺乏患者中，109例在肝移植前使用了AAT增强治疗，其中32例（29.4%）在肝移植后继续使用AAT增强治疗。肝移植后接受增强治疗的患者更年轻（56.5 [53-59.75]vs 57 [53.75-63], p = 0.04），缺血时间更短（平均311分钟vs 363分钟，p = 0.03）。经年龄调整的肝移植后增强治疗至死亡时间和ACGF的ATE估计值分别为+1.69和+1.48年。在前四分位数胆红素亚组中，lt增强治疗的使用与死亡率降低相关（p = 0.02， log-rank检验）。结论：在我们的研究中，肝移植后增强治疗的使用与生存率的提高有关。应考虑验证性前瞻性研究，为lt后AAT治疗指南提供信息。

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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JHLT Open

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