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Relative impact of HLA phenotype and CD4‐CD8 ratios on the clinical expression of hemochromatosis
Author(s) -
Porto G,
Vicente C,
Teixeira M A,
Martins O,
Cabeda J M,
Lacerda R,
Gonçalves C,
Fraga J,
Macedo G,
Silva B M,
Alves H,
Justiça B,
de Sousa M
Publication year - 1997
Publication title -
hepatology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.488
H-Index - 361
eISSN - 1527-3350
pISSN - 0270-9139
DOI - 10.1002/hep.510250223
Subject(s) - hemochromatosis , phenotype , hereditary hemochromatosis , human leukocyte antigen , context (archaeology) , disease , immunology , variable expression , biology , medicine , genetics , antigen , gene , paleontology
Hemochromatosis is a hereditary iron‐overload disease linked to HLA. The clinical expression of hemochromatosis is influenced by sex and age. However, other factors must account for the notorious heterogeneity of expression of the disease independent of sex, age, and HLA phenotype. The present study attempts to clarify some of these additional factors based on exhaustive statistical analysis of data collected from 43 selected patients with hemochromatosis. The statistical analysis focused on three groups of variables: the first group included variables reflecting the clinical expression of the disease; the second group represented the biochemical and hematological values at the time of diagnosis; and the third group consisted of the independent variables sex, age, HLA phenotype, and T‐cell subset profile, i.e., the percentages and total numbers of CD4+ and CD8+ cells and the CD4‐CD8 ratios. The results show that the relative expansion of the two main T‐cell subsets, in the context of the HLA phenotype, correlates significantly with the clinical expression of hemochromatosis and the severity of iron overload. The present findings substantiate further the postulate that T cells have a role in the regulation of iron metabolism.