Genetic variation in complement component 2 of the classical complement pathway is associated with increased mortality and infection: a study of 627 patients with trauma

John A Morris Jr; Cedric Francois; Paul K Olson; Bryan A Cotton; Marshall Summar; Judith M Jenkins; Patrick R Norris; Jason H Moore; Anna E Williams; Brent S McNew; Jeffrey A Canter

doi:10.1097/TA.0b013e31819ea61a

Genetic variation in complement component 2 of the classical complement pathway is associated with increased mortality and infection: a study of 627 patients with trauma

J Trauma. 2009 May;66(5):1265-70; discussion 1270-2. doi: 10.1097/TA.0b013e31819ea61a.

Authors

John A Morris Jr¹, Cedric Francois, Paul K Olson, Bryan A Cotton, Marshall Summar, Judith M Jenkins, Patrick R Norris, Jason H Moore, Anna E Williams, Brent S McNew, Jeffrey A Canter

Affiliation

¹ Division of Trauma and Surgical Critical Care, Vanderbilt University Medical Center, Nashville, Tennessee, USA. john.morris@vanderbilt.edu

Abstract

Background: Trauma is a disease of inflammation. Complement Component 2 (C2) is a protease involved in activation of complement through the classical pathway and has been implicated in a variety of chronic inflammatory diseases. We hypothesized that genetic variation in C2 (E318D) identifies a high-risk subgroup of patients with trauma reflecting increased mortality and infection (ventilator-associated pneumonia [VAP]). Consequently, genetic variation in C2 may stratify patient risk and illuminate underlying mechanisms for therapeutic intervention.

Methods: DNA samples from 702 patients with trauma were genotyped for C2 E318D and linked with covariates (age: mean 42.8 years, gender: 74% male, ethnicity: 80% white, mechanism: 84% blunt, injury severity score: mean 25.0, admission lactate: mean 3.13 mEq/L) and outcomes: mortality 9.9% and VAP: 18.5%. VAP was defined by quantitative bronchoalveolar lavage (> 10). Multivariate regression analysis determined the relationship of genotype and covariates to risk of death and VAP. However, patients with injury severity score > or = 45 were excluded from the multivariate analysis, as magnitude of injury overwhelms genetics and covariates in determining outcome.

Results: Fifty-two patients (8.3%) had the high-risk heterozygous genotype, associated with a significant increase in mortality and VAP.

Conclusion: In 702 patients with trauma, 8.3% had a high-risk genetic variation in C2 associated with increased mortality (odds ratio = 2.65) and infection (odds ratio = 2.00). This variation: (1) identifies a previously unknown high-risk group for infection and mortality; (2) can be determined at admission; (3) may provide opportunity for early therapeutic intervention; and (4) requires validation in a distinct cohort of patients.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Age Distribution
Analysis of Variance
Cause of Death*
Cohort Studies
Complement C2 / analysis
Complement C2 / genetics*
Complement Pathway, Classical / genetics*
Cross Infection / diagnosis
Cross Infection / genetics
Cross Infection / mortality
Female
Genetic Predisposition to Disease / epidemiology
Genetic Variation*
Hospital Mortality / trends*
Hospitals, University
Humans
Incidence
Injury Severity Score
Logistic Models
Male
Middle Aged
Multivariate Analysis
Odds Ratio
Pneumonia, Ventilator-Associated / genetics*
Pneumonia, Ventilator-Associated / mortality
Prognosis
Risk Assessment
Sensitivity and Specificity
Sex Distribution
Trauma Centers
Wounds and Injuries / diagnosis
Wounds and Injuries / genetics*
Wounds and Injuries / mortality
Young Adult

Substances

Complement C2

Abstract

Publication types

MeSH terms

Substances

Grants and funding