The role of B lymphocytes in osteoclast (OC) formation is controversial, because both stimulatory and Inhibitory effects of B-lineage cells on osteoclastogenesis and life span have been reported. In this study, we have Investigated the effects of mature B cells on human osteoclastogenesis using cultures of peripheral blood stem cells (PBSC), a system that generates functional OCs in the absence of stromal cells. We report that B cells inhibit the formation or OCs and shorten the life span of mature OCs by secreting transforming growth factor beta (TGF beta), a factor that induces apoptosis in these cells. The antiosteoclastogenic effects of B cells are abolished by addition of anti-TGF beta antibody to osteoclast cultures and mimicked by treatment of B cell-deprived PBSC cultures with recombinant TGF beta, thus confirming TGF beta as the B cell produced antiosteoclastogenic activity. Thus, the ability of B cells to downregulate osteoclastogenesis by secretion of the apoptotic cytokine TCF beta provides new insights into the ability of immune cells to regulate OC formation under basal and inflammatory conditions. (C) 2000 Wiley-Liss. Inc.
B lymphocytes inhibit human osteoclastogenesis by secretion of TGF beta / Weitzmann, Mn; Cenci, S; Haug, J; Brown, C; Dipersio, J; Pacifici, R. - In: JOURNAL OF CELLULAR BIOCHEMISTRY. - ISSN 0730-2312. - 78:2(2000), pp. 318-324. [10.1002/(SICI)1097-4644(20000801)78:2<318::AID-JCB13>3.0.CO;2-N]
B lymphocytes inhibit human osteoclastogenesis by secretion of TGF beta
Cenci SCo-primo
Investigation
;
2000-01-01
Abstract
The role of B lymphocytes in osteoclast (OC) formation is controversial, because both stimulatory and Inhibitory effects of B-lineage cells on osteoclastogenesis and life span have been reported. In this study, we have Investigated the effects of mature B cells on human osteoclastogenesis using cultures of peripheral blood stem cells (PBSC), a system that generates functional OCs in the absence of stromal cells. We report that B cells inhibit the formation or OCs and shorten the life span of mature OCs by secreting transforming growth factor beta (TGF beta), a factor that induces apoptosis in these cells. The antiosteoclastogenic effects of B cells are abolished by addition of anti-TGF beta antibody to osteoclast cultures and mimicked by treatment of B cell-deprived PBSC cultures with recombinant TGF beta, thus confirming TGF beta as the B cell produced antiosteoclastogenic activity. Thus, the ability of B cells to downregulate osteoclastogenesis by secretion of the apoptotic cytokine TCF beta provides new insights into the ability of immune cells to regulate OC formation under basal and inflammatory conditions. (C) 2000 Wiley-Liss. Inc.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.