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在儿科造血干细胞移植前的肺部宏转录组可识别移植后肺部损伤。

The pulmonary metatranscriptome prior to pediatric HCT identifies post-HCT lung injury.

机构信息

Division of Critical Care Medicine and.

Division of Allergy, Immunology, and Bone Marrow Transplantation, Department of Pediatrics, School of Medicine, University of California, San Francisco, CA.

出版信息

Blood. 2021 Mar 25;137(12):1679-1689. doi: 10.1182/blood.2020009246.

Abstract

Lung injury after pediatric allogeneic hematopoietic cell transplantation (HCT) is a common and disastrous complication that threatens long-term survival. To develop strategies to prevent lung injury, novel tools are needed to comprehensively assess lung health in HCT candidates. Therefore, this study analyzed biospecimens from 181 pediatric HCT candidates who underwent routine pre-HCT bronchoalveolar lavage (BAL) at the University Medical Center Utrecht between 2005 and 2016. BAL fluid underwent metatranscriptomic sequencing of microbial and human RNA, and unsupervised clustering and generalized linear models were used to associate microbiome gene expression data with the development of post-HCT lung injury. Microbe-gene correlations were validated using a geographically distinct cohort of 18 pediatric HCT candidates. The cumulative incidence of post-HCT lung injury varied significantly according to 4 pre-HCT pulmonary metatranscriptome clusters, with the highest incidence observed in children with pre-HCT viral enrichment and innate immune activation, as well as in children with profound microbial depletion and concomitant natural killer/T-cell activation (P < .001). In contrast, children with pre-HCT pulmonary metatranscriptomes containing diverse oropharyngeal taxa and lacking inflammation rarely developed post-HCT lung injury. In addition, activation of epithelial-epidermal differentiation, mucus production, and cellular adhesion were associated with fatal post-HCT lung injury. In a separate validation cohort, associations among pulmonary respiratory viral load, oropharyngeal taxa, and pulmonary gene expression were recapitulated; the association with post-HCT lung injury needs to be validated in an independent cohort. This analysis suggests that assessment of the pre-HCT BAL fluid may identify high-risk pediatric HCT candidates who may benefit from pathobiology-targeted interventions.

摘要

儿童异基因造血细胞移植(HCT)后肺损伤是一种常见且灾难性的并发症,威胁着长期生存。为了制定预防肺损伤的策略,需要新的工具来全面评估 HCT 候选者的肺部健康。因此,本研究分析了 2005 年至 2016 年期间在乌得勒支大学医学中心接受常规移植前支气管肺泡灌洗(BAL)的 181 名儿童 HCT 候选者的生物标本。BAL 液进行了微生物和人类 RNA 的宏转录组测序,使用无监督聚类和广义线性模型将微生物组基因表达数据与移植后肺损伤的发展相关联。使用来自 18 名儿科 HCT 候选者的地理位置不同的队列验证了微生物-基因相关性。根据 4 个移植前肺部宏转录组聚类,移植后肺损伤的累积发生率有显著差异,具有移植前病毒富集和先天免疫激活、以及严重微生物耗竭和同时自然杀伤/T 细胞激活的儿童发生率最高(P<0.001)。相比之下,具有包含多样化口咽类群且缺乏炎症的移植前肺部宏转录组的儿童很少发生移植后肺损伤。此外,上皮-表皮分化、粘液产生和细胞黏附的激活与致命的移植后肺损伤相关。在一个单独的验证队列中,肺部呼吸道病毒载量、口咽类群和肺部基因表达之间的关联得到了重现;与移植后肺损伤的关联需要在独立队列中得到验证。该分析表明,评估移植前 BAL 液可以识别高风险的儿科 HCT 候选者,他们可能受益于针对病理生物学的干预措施。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/77b5/7995292/458f9d29fcd8/bloodBLD2020009246absf1.jpg

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