T-cell receptor diversity is selectively skewed in T-cell populations of patients with Wiskott-Aldrich syndrome.

[wiskott-aldrich syndrome]

Wiskott-Aldrich syndrome (WAS ) is a severe disorder characterized by thrombocytopenia , eczema , immunodeficiency , and increased risk of autoimmune disease and lymphoid malignancies . The immunodeficiency caused by a lack of WAS protein expression has been mainly attributed to defective T -cell functions . Whether WAS mutations differentially influence the T -cell receptor (TCR ) diversity of different T -cell subsets is unknown .We aimed to identify the degree and pattern of skewing in the variable region of the TCR β-chain (Vβ ) in different T -cell subsets from patients with WAS .T he TCR repertoire diversity in total peripheral T cells , sorted CD 4 (+) and CD 8 (+) T cells , and CD 4 5 RA (+) (CD 4 5 RA (+)CD 4 5 RO (-) cells ) and CD 4 5 RO (+) (CD 4 5 RA (-)CD 4 5 RO (+) cells ) CD 4 (+) and CD 8 (+) T cells from patients with WAS and age-matched healthy control subjects was analyzed and compared by using spectratyping of complementarity-determining region 3 . The complementarity-determining region 3 of TCRβ transcripts in CD 4 5 RA (+)CD 4 (+) and CD 4 5 RA (+)CD 8 (+) T cells , CD 4 5 RO (+)CD 4 (+) T cells , CD 8 (+) terminally differentiated effector memory T (Temra ) cells , and naive CD 8 (+) T cells (CD 8 (+)CD 4 5 RO (-)CCR 7 (+) cells ) from patients and control subjects were analyzed and compared by using high -throughput sequencing .The TCR repertoire diversity in CD 4 5 RO (+)CD 4 (+) T cells and CD 8 (+) Temra cells of patients with WAS was significantly skewed in comparison with that seen in age-matched control subjects .Our results indicate that WAS gene mutations selectively influence TCR repertoire development or expansion in CD 4 5 RO (+) (memory ) CD 4 (+) T cells .