Airway rejection after lung transplantation is recognized histologically as lymphocytic bronchiolitis (LB). We hypothesized that inhaled steroids could control LB and that changes in exhaled nitric oxide (eNO) would correlate with the development of LB and also have a role in monitoring response to treatment. A cohort of 120 lung transplant (LT) recipients attending for review and biopsy had eNO measurements, FEV1, lavage microbiology, and biopsy histology performed prospectively. Wilcoxon signed-rank test was used to assess the significance of changes in eNO and FEV1. The coefficient of reproducibility of eNO measurement in stable recipients was 2.36 ppb. Fourteen developed graft dysfunction owing to isolated LB and were treated with inhaled budesonide 800 microg twice daily. They showed significant increases in eNO at diagnosis, median (range) 10.9 ppb (4.6 to 48) ppb compared with baseline, 4.33 (1.0 to 10.76), p = 0.008, and a decrease in FEV1. After inhaled treatment, both eNO and FEV1 returned to baseline values. Seven developed acute vascular rejection (with or without LB) and were treated with oral corticosteroids; no changes in eNO occurred at diagnosis or after treatment. Serial eNO measurements provide a useful noninvasive method of identifying airway inflammation in LT recipients. Inhaled budesonide may be a useful addition to systemic immunosuppressants in controlling airway inflammation posttransplant.

译文

肺移植后:气道排斥在组织学上被认为是淋巴细胞性细支气管炎(LB)。我们假设吸入的类固醇可以控制LB,而呼出的一氧化氮(eNO)的变化将与LB的发生有关,并且在监测对治疗的反应中也具有作用。参加检查和活检的120名肺移植(LT)接受者队列前瞻性地进行了eNO测量,FEV1,灌洗微生物学和活检组织学检查。 Wilcoxon符号秩检验用于评估eNO和FEV1变化的重要性。在稳定的受者中,eNO测量的可重复性系数为2.36 ppb。由于分离出的LB,有十四个移植物功能障碍,每天两次吸入布地奈德800μg吸入治疗。他们显示出诊断时的eNO显着增加,中位数(范围)与基线相比为10.9 ppb(4.6至48)ppb,4.33(1.0至10.76),p = 0.008,FEV1降低。吸入治疗后,eNO和FEV1均恢复到基线值。 7例出现急性血管排斥反应(有或没有LB),并接受口服皮质类固醇激素治疗;诊断或治疗后eNO均无变化。连续的eNO测量为鉴定LT受体的气道炎症提供了一种有用的非侵入性方法。在控制移植后气道炎症中,吸入布地奈德可能是对全身免疫抑制剂的有用补充。

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