4.7 Article

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

Journal

BLOOD
Volume 137, Issue 12, Pages 1679-1689

Publisher

AMER SOC HEMATOLOGY
DOI: 10.1182/blood.2020009246

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Funding

  1. National Marrow Donor Program Amy Strelzer Manasevit Grant
  2. National Institutes of Health, Eunice Kennedy Shriver National Institute of Child Health and Human Development [K12HD000850]
  3. National Institutes of Health, National Heart, Lung, and Blood Institute [K23HL146936, R01HL134828, R35HL140026]
  4. American Thoracic Society Foundation
  5. Chan Zuckerberg Biohub

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This study analyzed biospecimens from 181 pediatric HCT candidates to investigate the association between pre-HCT pulmonary metatranscriptomes and post-HCT lung injury. The results showed that certain gene expression patterns and microbiome compositions in the lungs prior to transplantation were linked to an increased risk of developing lung injury after the procedure. Data from this study suggest that assessment of pre-HCT BAL fluid could potentially help identify high-risk pediatric HCT candidates who may benefit from targeted interventions.
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 metatran-scriptome 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.

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