Evidence of thymic dysfunction in ataxia telagiectasia - 25/08/11
Abstract |
Rationale |
There is evidence of low thymic output in patients with ataxia telangiectasia (A-T). Thymulin, a peptide hormone only secreted by thymic epithelial cells, is essential for T-lymphocyte formation and is a reproducible indicator of functional thymic tissue. We analyzed thymic output and function, using thymulin, in three children with A-T.
Methods |
Thymic output and function were performed in three patients with A-T by the following measurements: 1) thymulin using sheep cell rosette assay; 2) the presence of TREC in PBMCs using real-time PCR; 3) peripheral blood naïve T-lymphocyte (CD3+CD4+CD45RA+CD62L+ cells) phenotyping by flow cytometry; and 4) lymphocyte proliferation assays performed with phytomitogens and antigens.
Results |
Mean age was 13 years (range 12-15 years). Thymulin levels were undetectable in two patients and 1:8 in one pt (normal 1:16-1:128). Mean TREC was 309 copies/106 cells (normal 40,000-600,000); mean CD4+ percentage was 29% (36-47%); mean absolute CD4+ cell count was 274 cells/: L (900-2,860 cells/: L); mean naïve CD4+ percentage was 1% (53%); and mean absolute naïve CD4+ cell count was 8 cells/: L (364 ± 200 cells/: L). Lymphocyte proliferation to mitogens was normal in all patients and lymphocyte proliferation to antigens was normal in 2 out of 3 patients.
Conclusions |
We present the first report of diminished levels of thymulin, in addition to low thymic output, in patients with A-T. These results indicate abnormal T-lymphocyte genesis and maturation, while normal proliferation studies reveal normal T-lymphocyte function. The mechanism of the low output may be a defect in thymic.
Le texte complet de cet article est disponible en PDF. Funding: University Monies |
Vol 113 - N° 2S
P. S46 - février 2004 Retour au numéroBienvenue sur EM-consulte, la référence des professionnels de santé.
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