严重的新型冠状病毒2型感染与肺移植受者产生新的人类白细胞抗原抗体的风险增加有关:单中心研究。
Severe SARS-CoV-2 infection is associated with increased risk of De novo HLA antibody production in lung transplant recipients: Single-center study.
作者信息
Shah Sadia Z, Du Zeying, El Jack Kamal, Pham Si M, Elrefaei Mohamed
机构信息
Department of Transplantation, Mayo Clinic, Jacksonville, FL, United States of America.
Department of Laboratory Medicine and Pathology, Mayo Clinic, Jacksonville, FL, United States of America.
出版信息
Transpl Immunol. 2025 Feb;88:102161. doi: 10.1016/j.trim.2024.102161. Epub 2024 Dec 5.
THE PURPOSE
The COVID-19 pandemic has led to significant morbidity and mortality in lung transplant recipients (LTR). Respiratory viral infections may be associated with de-novo HLA donor-specific antibody (DSA) production and impact lung transplant outcomes. Since one of the immunomodulation strategies post-SARS-CoV-2 infection in LTR include decreasing or holding anti-metabolites, concerns have been raised for higher incidence of de-novo DSA production in LTR.
METHODS
We performed a retrospective chart review of 63 consecutive LTR diagnosed with COVID-19 to investigate this concern. COVID-19 disease severity was divided into 3 groups: mild, moderate, and severe. Mild disease was defined as patients with COVID-19 diagnosis who were stable enough to be treated as out-patients. Moderate disease was defined as patients who required admission to the hospital and were on less than 10 l of oxygen at rest. Severe disease was identified as patients who required hospitalization and were on more than 10 l of oxygen with or without mechanical ventilation or extra corporal membrane oxygenation (ECMO). Groups were compared using the Kruskal-Wallis test. A total of 11, 43, and 9 LTR were diagnosed with mild, moderate, and severe COVID-19 respectively.
RESULTS
We observed no significant differences in the CPRA pre-COVID-19 compared to 1 and 6 months post-COVID-19 diagnosis in 6/11 (54.5 %), 18/43 (41.8 %), and 6/9 (66.9 %) LTR with mild (p = 0.66), moderate (p = 0.74), and severe (p = 0.22) COVID-19 respectively. HLA class I and II DSA were detected pre-COVID-19 diagnosis and persisted with no significant differences in the median MFI levels at 1 and 6 months post-COVID-19 diagnosis in 2/11 (p = 0.93), 7/43 (p = 0.71), and 0/9 LTR with mild, moderate, and severe COVID-19 respectively. De-novo HLA DSA were detected within 6 months post-COVID-19 diagnosis in 0/11 (0 %), 1/43 (2.3 %), and 3/9 (33.3 %%) LTR with mild, moderate, and severe COVID-19 respectively (p = 0.001).
CONCLUSION
Severe COVID-19 may be associated with increased risk of de novo HLA DSA production resulting in allograft dysfunction.
目的
新冠疫情导致肺移植受者(LTR)出现了严重的发病情况和死亡情况。呼吸道病毒感染可能与新产生的供者特异性HLA抗体(DSA)有关,并影响肺移植的结果。由于LTR感染新冠病毒后的免疫调节策略之一包括减少或停用抗代谢药物,因此人们担心LTR中新产生DSA的发生率会更高。
方法
我们对63例连续诊断为新冠的LTR进行了回顾性病历审查,以调查这一问题。新冠疾病的严重程度分为3组:轻度、中度和重度。轻度疾病定义为确诊新冠且病情稳定可作为门诊患者治疗的患者。中度疾病定义为需要住院且静息时吸氧低于10升的患者。重度疾病定义为需要住院且静息时吸氧超过10升,无论是否使用机械通气或体外膜肺氧合(ECMO)的患者。使用Kruskal-Wallis检验对各组进行比较。分别有11例、43例和9例LTR被诊断为轻度、中度和重度新冠。
结果
我们观察到,在分别患有轻度(p = 0.66)、中度(p = 0.74)和重度(p = 0.22)新冠的11例LTR中的6例(54.5%)、43例LTR中的18例(41.8%)和9例LTR中的6例(66.9%)中,新冠诊断前的CPRA与新冠诊断后1个月和6个月相比无显著差异。在分别患有轻度、中度和重度新冠的11例LTR中的2例(p = 0.93)、43例LTR中的7例(p = 0.71)和9例LTR中的0例中,新冠诊断前检测到HLA I类和II类DSA,且在新冠诊断后1个月和6个月时,中位MFI水平无显著差异。在分别患有轻度、中度和重度新冠的11例LTR中的0例(0%)、43例LTR中的1例(2.3%)和9例LTR中的3例(33.3%)中,在新冠诊断后6个月内检测到新的HLA DSA(p = 0.001)。
结论
重度新冠可能与新产生HLA DSA导致移植物功能障碍的风险增加有关。
Zotero 插件