Dissecting inflammatory complications in critically injured patients by within-patient gene expression changes: a longitudinal clinical genomics study.

Keyur H Desai; Chuen Seng Tan; Jeffrey T Leek; Ronald V Maier; Ronald G Tompkins; John D Storey; Inflammation and the Host Response to Injury Large-Scale Collaborative Research Program

doi:10.1371/journal.pmed.1001093

PLoS Medicine (Sep 2011)

Dissecting inflammatory complications in critically injured patients by within-patient gene expression changes: a longitudinal clinical genomics study.

Keyur H Desai,
Chuen Seng Tan,
Jeffrey T Leek,
Ronald V Maier,
Ronald G Tompkins,
John D Storey,
Inflammation and the Host Response to Injury Large-Scale Collaborative Research Program

Affiliations

Keyur H Desai
Chuen Seng Tan
Jeffrey T Leek
Ronald V Maier
Ronald G Tompkins
John D Storey
Inflammation and the Host Response to Injury Large-Scale Collaborative Research Program

DOI: https://doi.org/10.1371/journal.pmed.1001093
Journal volume & issue: Vol. 8, no. 9
p. e1001093

Abstract

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Trauma is the number one killer of individuals 1-44 y of age in the United States. The prognosis and treatment of inflammatory complications in critically injured patients continue to be challenging, with a history of failed clinical trials and poorly understood biology. New approaches are therefore needed to improve our ability to diagnose and treat this clinical condition.We conducted a large-scale study on 168 blunt-force trauma patients over 28 d, measuring ∼400 clinical variables and longitudinally profiling leukocyte gene expression with ∼800 microarrays. Marshall MOF (multiple organ failure) clinical score trajectories were first utilized to organize the patients into five categories of increasingly poor outcomes. We then developed an analysis framework modeling early within-patient expression changes to produce a robust characterization of the genomic response to trauma. A quarter of the genome shows early expression changes associated with longer-term post-injury complications, captured by at least five dynamic co-expression modules of functionally related genes. In particular, early down-regulation of MHC-class II genes and up-regulation of p38 MAPK signaling pathway were found to strongly associate with longer-term post-injury complications, providing discrimination among patient outcomes from expression changes during the 40-80 h window post-injury.The genomic characterization provided here substantially expands the scope by which the molecular response to trauma may be characterized and understood. These results may be instrumental in furthering our understanding of the disease process and identifying potential targets for therapeutic intervention. Additionally, the quantitative approach we have introduced is potentially applicable to future genomics studies of rapidly progressing clinical conditions.ClinicalTrials.gov NCT00257231

Published in PLoS Medicine

ISSN: 1549-1277 (Print); 1549-1676 (Online)
Publisher: Public Library of Science (PLoS)
Country of publisher: United States
LCC subjects: Medicine
Website: https://journals.plos.org/plosmedicine/

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