Interleukin 4 content in chronic lymphocytic leukaemia (CLL) B cells and blood CD8(+) T cells from B-CLL patients: impact on clonal B-cell apoptosis

B-chronic lymphocytic leukaemia (CLL) clonal B cells are characterized by r esistance to apoptosis. We evaluated clonal B cells and blood T cells for i nterleukin 4 (IL-4) content as IL-4 is able to increase CLL cell resistance to apoptosis, The content of IL-4 in CD8(+) T cells of CLL patients (n = 9 ) ranged from 37% to 63% of the total CD8(+) T cells (mean level of 49% +/- 3.4) compared with a range of 5-10% for control CD8(+) T cells. Clonal B c ells positive for cytoplasmic IL-4 ranged from 1% to 97% (mean value 57.8 /- 6.9%). CD8(+) T cells and clonal B cells secreted detectable levels of I L-4, but only clonal CLL B cells (n = 4) secreted IL-4 in association with increasing cell numbers. Fludarabine (F-ara-AMP, 0.1-100 mu mol/ml) was abl e to downregulate the IL-4 content of CD8(+) T cells, but not clonal B-cell IL-4. Culture supernatant from CLL CD8(+) T cells decreased the spontaneou s apoptotic rate of clonal B cells that was reversed with anti-IL-4 and sol uble IL-4 receptor. These findings show that IL-4 is present in the microen vironment of B-CLL. in addition, use of agents that can interfere with IL-4 presentation to clonal B cells can be effective in increasing clonal B-cel l apoptosis.