TY - JOUR
T1 - Gene expression in giant cell myocarditis
T2 - Altered expression of immune response genes
AU - Kittleson, Michelle M.
AU - Minhas, Khalid M.
AU - Irizarry, Rafael A.
AU - Ye, Shui Q.
AU - Edness, Gina
AU - Breton, Elayne
AU - Conte, John V.
AU - Tomaselli, Gordon
AU - Garcia, Joe G.N.
AU - Hare, Joshua M.
PY - 2005/7/10
Y1 - 2005/7/10
N2 - Background: Giant cell myocarditis is a rapidly progressive and often fatal condition without a clear etiology or treatment. A better understanding of giant cell myocarditis pathogenesis is critical to developing treatments to prevent progression and reverse damage. We compared the gene expression of giant cell myocarditis with that of nonfailing hearts. Methods: Left ventricular samples from two giant cell myocarditis patients harvested during ventricular assist device placement and six unused donor hearts were examined using Affymetrix U133A microarrays. Differential gene expression was defined with a Bonferroni-adjusted p value ≤ 0.05 from a Student's t-test and an absolute fold change ≥ 2.0. Select gene expression was confirmed with quantitative PCR. Results: Of 115 differentially expressed genes, most were upregulated in giant cell myocarditis and involved in immune response, transcriptional regulation, and metabolism. T-cell activation genes included chemokine receptor 4; chemokine ligands 5, 9, 13, and 18; interleukin-10 receptor alpha; and beta-2 integrin. Conclusions: Gene expression analysis of giant cell myocarditis offers novel insights into its pathogenesis, namely the role of T-cell activators of the Th1 subset and immune response genes previously implicated in heart failure. This forms the basis for future work aimed at defining novel therapeutic targets for giant cell myocarditis.
AB - Background: Giant cell myocarditis is a rapidly progressive and often fatal condition without a clear etiology or treatment. A better understanding of giant cell myocarditis pathogenesis is critical to developing treatments to prevent progression and reverse damage. We compared the gene expression of giant cell myocarditis with that of nonfailing hearts. Methods: Left ventricular samples from two giant cell myocarditis patients harvested during ventricular assist device placement and six unused donor hearts were examined using Affymetrix U133A microarrays. Differential gene expression was defined with a Bonferroni-adjusted p value ≤ 0.05 from a Student's t-test and an absolute fold change ≥ 2.0. Select gene expression was confirmed with quantitative PCR. Results: Of 115 differentially expressed genes, most were upregulated in giant cell myocarditis and involved in immune response, transcriptional regulation, and metabolism. T-cell activation genes included chemokine receptor 4; chemokine ligands 5, 9, 13, and 18; interleukin-10 receptor alpha; and beta-2 integrin. Conclusions: Gene expression analysis of giant cell myocarditis offers novel insights into its pathogenesis, namely the role of T-cell activators of the Th1 subset and immune response genes previously implicated in heart failure. This forms the basis for future work aimed at defining novel therapeutic targets for giant cell myocarditis.
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U2 - 10.1016/j.ijcard.2005.03.075
DO - 10.1016/j.ijcard.2005.03.075
M3 - Article
C2 - 15982506
AN - SCOPUS:20744435933
SN - 0167-5273
VL - 102
SP - 333
EP - 340
JO - International Journal of Cardiology
JF - International Journal of Cardiology
IS - 2
ER -