Ba. Pietra et al., TCR V-BETA FAMILY REPERTOIRE AND T-CELL ACTIVATION MARKERS IN KAWASAKI-DISEASE, The Journal of immunology, 153(4), 1994, pp. 1881-1888
Kawasaki disease (KD) is the leading cause of acquired heart disease i
n children in the United States. The etiology is unknown. Data regardi
ng the presence of T cell activation and its potential role in the pat
hogenesis of the disease have been conflicting. Expansion of T cells b
earing V beta 2 and V beta 8 has recently been reported in the acute p
hase of KD, which suggests that a superantigen may mediate the disease
process. To further assess the potential role of T cells in KD, T cel
l phenotypes were evaluated by using flow cytometry in a large series
of patients, acutely and during convalescence. Included in this analys
is were assessments of changes in the percentage of T cells bearing TC
R V beta 2, V beta 5.1, V beta 6.7, V beta 8, V beta 12.1, and V beta
19 over time; the percentage of each V beta family bearing the activat
ion markers HLA-DR and IL-2R; and the percentage of each V beta family
bearing the memory marker, CD45 RO. No expansion of any V beta family
was present acutely, nor were increases in HLA-DR and IL-2R observed.
However, a significant increase was observed during convalescence in
the percentage of cells bearing CD45RO in the CD8(+), but not the CD4(
+), population. CD45RO expression was also increased on V beta 2, V be
ta 8, and V beta 19 CD8(+) T cells in a subset of patients. These data
suggest that one or more conventional Ags drive the T cell immune res
ponse in KD, and argue against a role for superantigens in the disease
process.