Association of genetic polymorphisms and risk of late post-transplantation infection in pediatric heart recipients

Erin L Ohmann; Maria M Brooks; Steven A Webber; Diana M Girnita; Robert E Ferrell; Gilbert J Burckart; Richard Chinnock; Charles Canter; Linda Addonizio; Daniel Bernstein; James K Kirklin; David C Naftel; Adriana Zeevi

doi:10.1016/j.healun.2010.07.013

Association of genetic polymorphisms and risk of late post-transplantation infection in pediatric heart recipients

J Heart Lung Transplant. 2010 Dec;29(12):1342-51. doi: 10.1016/j.healun.2010.07.013.

Authors

Erin L Ohmann¹, Maria M Brooks, Steven A Webber, Diana M Girnita, Robert E Ferrell, Gilbert J Burckart, Richard Chinnock, Charles Canter, Linda Addonizio, Daniel Bernstein, James K Kirklin, David C Naftel, Adriana Zeevi

Affiliation

¹ Department of Pediatrics, Division Cardiology, University of Pittsburgh, Pittsburgh, Pennsylvania, USA.

PMID: 20869265
DOI: 10.1016/j.healun.2010.07.013

Abstract

Background: Late infections are common causes of morbidity and mortality after pediatric heart transplantation. In this multicenter study from 6 centers, we investigated the association between genetic polymorphisms (GPs) in immune response genes and late post-transplantation infections in 524 patients.

Methods: Late infection was defined as a clinical infectious process occurring >60 days after transplantation and requiring hospitalization, intravenous antimicrobial therapy, or a life-threatening infection requiring oral therapy. All patients provided a blood sample for GP analyses of 18 GPs in cytokine, growth factor, and effector molecule genes by single specific primer-polymerase chain reaction and/or sequencing. Significant associations in univariable analyses were tested in multivariable Cox regression models.

Results: Late infection was common, with 48.7% of patients experiencing ≥ 1 late infection, 25.2% had ≥ 1 late bacterial infection, and 30.5% had ≥ 1 late viral infection. Older age at transplantation was a protective factor for late infection, both bacterial and viral (hazard ratio [HR] 0.89-0.92 per 1-year age increase, p < 0.001). Adjusting for age, race, and transplant etiology, late bacterial infection was associated with HMOX1 A+326G AG and GG genotypes (HR, 2.41, 95% confidence interval [CI] 1.35-4.30; p = 0.003) and GZMB A-295G AA genotype (HR, 1.47; 95% CI; 1.03-2.1; p = 0.036). Late viral infection was associated with FAS A-670G GG genotype (HR, 1.42; 95% CI, 1.00-2.00; p = 0.050) in the adjusted model and with CTLA4 A+49G AA and AG genotypes (HR, 1.49; 95% CI, 1.02-2.19; p = 0.041) in univariable analysis.

Conclusion: We found an association between late bacterial infection and GP of HMOX1, which may control macrophage activation. A weaker association was also found between late viral infection and GP of CTLA4, a regulator of T-cell activation. This represents progress toward understanding the clinical and genetic risk factors of outcomes after transplantation.

Publication types

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

MeSH terms

Adolescent
Antigens, CD / genetics
Bacterial Infections / genetics*
CTLA-4 Antigen
Child
Child, Preschool
Cohort Studies
Female
Genes, MHC Class II / genetics*
Genetic Predisposition to Disease*
Genotype
Heart Transplantation / immunology*
Heme Oxygenase-1 / genetics
Humans
Infant
Male
Polymorphism, Genetic / immunology*
Risk Factors
Virus Diseases / genetics*

Substances

Antigens, CD
CTLA-4 Antigen
CTLA4 protein, human
HMOX1 protein, human
Heme Oxygenase-1

Grants and funding

5P50 HL 074 732-05/HL/NHLBI NIH HHS/United States