Downregulation of Tumor Suppressor Gene LKB1 During Severe Primary Graft Dysfunction After Human Lung Transplantation: Implication for the Development of Chronic Lung Allograft Dysfunction.

IF 5.3 2区 医学 Q1 IMMUNOLOGY
Mohammad Rahman, Davide Scozzi, Natsuki Eguchi, Rachel Klein, Narendra V Sankpal, Angara Sureshbabu, Timothy Fleming, Ramsey Hachem, Michael Smith, Ross Bremner, Thalachallour Mohanakumar
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引用次数: 0

Abstract

Background: Severe primary graft dysfunction (PGD) after lung transplantation (LTx) is a significant risk factor for the development of bronchiolitis obliterans syndrome (BOS). Recent data from our group demonstrated that small extracellular vesicles (sEVs) isolated from the plasma of LTx recipients with BOS have reduced levels of tumor suppressor gene liver kinase B1 (LKB1) and promote epithelial-to-mesenchymal transition (EMT) and fibrosis. Here, we hypothesized that early inflammatory responses associated with severe PGD (PGD2/3) can downregulate LKB1 levels in sEVs, predisposing to the development of chronic lung allograft dysfunction (CLAD).

Methods: sEVs were isolated from the plasma of human participants by Exosome Isolation Kit followed by 0.20-µm filtration and characterized by NanoSight and immunoblotting analysis. Lung self-antigens (K alpha 1 tubulin, Collagen V), LKB1, nuclear factor kappa B, and EMT markers in sEVs were compared by densitometry analysis between PGD2/3 and no-PGD participants. Neutrophil-derived factors and hypoxia/reperfusion effects on LKB1 levels and EMT were analyzed in vitro using quantitative real-time polymerase chain reaction and Western blotting.

Results: LKB1 was significantly downregulated in PGD2/3 sEVs compared with no-PGD sEVs. Within PGD2/3 participants, lower post-LTx LKB1 was associated with CLAD development. Hypoxia/reperfusion downregulates LKB1 and is associated with markers of EMT in vitro. Finally, lower LKB1 levels in PGD2/3 are associated with increased markers of EMT.

Conclusions: Our results suggest that in post-LTx recipients with PGD2/3, downregulation of LKB1 protein levels in sEVs is associated with increased EMT markers and may result in the development of CLAD. Our results also suggest that ischemia/reperfusion injury during LTx may promote CLAD through the early downregulation of LKB1.

人体肺移植后严重的原发性移植物功能障碍过程中肿瘤抑制基因 LKB1 的下调:对慢性肺移植功能障碍发展的影响。
背景:肺移植(LTx)后出现严重的原发性移植物功能障碍(PGD)是发生支气管炎闭塞综合征(BOS)的重要风险因素。我们研究小组的最新数据表明,从肺移植受者血浆中分离出的细胞外小泡(sEVs)会降低肿瘤抑制基因肝激酶 B1(LKB1)的水平,并促进上皮细胞向间质转化(EMT)和纤维化。方法:使用外泌体分离试剂盒从人类参与者的血浆中分离出外泌体,然后进行0.20微米过滤,并通过NanoSight和免疫印迹分析进行表征。通过密度分析比较了 PGD2/3 和无 PGD 参与者 sEV 中的肺自身抗原(K α 1 小管蛋白、胶原 V)、LKB1、核因子卡巴 B 和 EMT 标记。使用定量实时聚合酶链反应和 Western 印迹法在体外分析了中性粒细胞衍生因子和缺氧/再灌注对 LKB1 水平和 EMT 的影响:结果:与无 PGD sEV 相比,LKB1 在 PGD2/3 sEV 中明显下调。在 PGD2/3 参与者中,LTx 后 LKB1 的降低与 CLAD 的发生有关。缺氧/再灌注会使 LKB1 下调,并与体外 EMT 标记相关。最后,PGD2/3中较低的LKB1水平与EMT标记物的增加有关:我们的研究结果表明,在 LTx 术后的 PGD2/3 受体中,sEV 中 LKB1 蛋白水平的下调与 EMT 标志物的增加有关,并可能导致 CLAD 的发生。我们的结果还表明,LTx 过程中的缺血/再灌注损伤可能会通过 LKB1 的早期下调促进 CLAD 的发生。
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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来源期刊
Transplantation
Transplantation 医学-免疫学
CiteScore
8.50
自引率
11.30%
发文量
1906
审稿时长
1 months
期刊介绍: The official journal of The Transplantation Society, and the International Liver Transplantation Society, Transplantation is published monthly and is the most cited and influential journal in the field, with more than 25,000 citations per year. Transplantation has been the trusted source for extensive and timely coverage of the most important advances in transplantation for over 50 years. The Editors and Editorial Board are an international group of research and clinical leaders that includes many pioneers of the field, representing a diverse range of areas of expertise. This capable editorial team provides thoughtful and thorough peer review, and delivers rapid, careful and insightful editorial evaluation of all manuscripts submitted to the journal. Transplantation is committed to rapid review and publication. The journal remains competitive with a time to first decision of fewer than 21 days. Transplantation was the first in the field to offer CME credit to its peer reviewers for reviews completed. The journal publishes original research articles in original clinical science and original basic science. Short reports bring attention to research at the forefront of the field. Other areas covered include cell therapy and islet transplantation, immunobiology and genomics, and xenotransplantation. ​
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