Abstract:The course of disease in patients suffering from chronic lymphocytic leukemia (CLL) is determined by a profound dysregulation of the immune system. The resulting immune suppression is the main cause of death in those patients. In the present study we addressed the question of whether leukemic B cells (B-CLL) are able to suppress regular T cell/B cell interaction. Activated CD4+ T cell clones induce expression of the early activation antigen CD23 on B lymphocytes in vitro. Under conditions used, this B cell act… Show more
“…As such, CLL cells can compete with normal B cells for cognate interactions with T cells, thereby reducing the probability for chance encounter of T cells with antigen-reactive normal B cells. CLL cells also can inhibit the generation of effective cognate-interactions between activated T cells and normal B cells in vitro (31). Moreover, CLL cells can down-modulate the expression of CD154 on activated T cells (32), and elaborate factors, such as TGF-beta (33) or receptors for IL-2 that can mitigate the activity of helper T cells to stimulate antigen-reactive cells (34).…”
Section: Disruption Of Healthy Niches By Cll Cellsmentioning
“…As such, CLL cells can compete with normal B cells for cognate interactions with T cells, thereby reducing the probability for chance encounter of T cells with antigen-reactive normal B cells. CLL cells also can inhibit the generation of effective cognate-interactions between activated T cells and normal B cells in vitro (31). Moreover, CLL cells can down-modulate the expression of CD154 on activated T cells (32), and elaborate factors, such as TGF-beta (33) or receptors for IL-2 that can mitigate the activity of helper T cells to stimulate antigen-reactive cells (34).…”
Section: Disruption Of Healthy Niches By Cll Cellsmentioning
Synovial B cells from patients with RA and patients with PsA express different antigen-presenting cell phenotypes, suggesting that this cell type plays a dissimilar role in the pathogenesis of each disease.
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