Abstract
BackgroundOestrogen-deficiency induced by menopause is associated with reduced bone density and primary osteoporosis, resulting in an increased risk of fracture. While the exact etiology of menopause-induced primary osteoporotic bone loss is not fully known, members of the tumour necrosis factor super family (TNFSF) are known to play a role. Recent studies have revealed that the TNFSF members death receptor 3 (DR3) and one of its ligands, TNF-like protein 1A (TL1A) have a key role in secondary osteoporosis; enhancing CD14+ peripheral blood mononuclear cell (PBMC) osteoclast formation and bone resorption. Whether DR3 and TL1A contribute towards bone loss in menopause-induced primary osteoporosis however, remains unknown.MethodsTo investigate this we performed flow cytometry analysis of DR3 expression on CD14+ PBMCs isolated from pre- and early post-menopausal females and late post-menopausal osteoporotic patients. Serum levels of TL1A, CCL3 and total MMP-9 were measured by ELISA. In vitro osteoclast differentiation assays were performed to determine CD14+ monocyte osteoclastogenic potential. In addition, splenic CD4+ T cell DR3 expression was investigated 1 week and 8 weeks post-surgery, using the murine ovariectomy model.ResultsIn contrast to pre-menopausal females, CD14+ monocytes isolated from post-menopausal females were unable to induce DR3 expression. Serum TL1A levels were decreased approx. 2-fold in early post-menopausal females compared to pre-menopausal controls and post-menopausal osteoporotic females; no difference was observed between pre-menopausal and late post-menopausal osteoporotic females. Analysis of in vitro CD14+ monocyte osteoclastogenic potential revealed no significant difference between the post-menopausal and post-menopausal osteoporotic cohorts. Interestingly, in the murine ovariectomy model splenic CD4+ T cell DR3 expression was significantly increased at 1 week but not 8 weeks post-surgery when compared to the sham control.ConclusionOur results reveals for the first time that loss of oestrogen has a significant effect on DR3; decreasing expression on CD14+ monocytes and increasing expression on CD4+ T cells. These data suggest that while oestrogen-deficiency induced changes in DR3 expression do not affect late post-menopausal bone loss they could potentially have an indirect role in early menopausal bone loss through the modulation of T cell activity.
Highlights
Oestrogen-deficiency induced by menopause is associated with reduced bone density and primary osteoporosis, resulting in an increased risk of fracture
This study focused on the tumour necrosis factor super family (TNFSF) members tumour necrosis factor (TNF)-like protein 1A (TL1A, TNFSF15) and its only confirmed trans-membrane receptor, death receptor 3 (DR3; TNFRSF25) [12]
In the present study we investigated serum levels of TL1A and the expression of DR3 on peripheral blood CD14+ cells isolated from pre-menopausal, postmenopausal and late post-menopausal osteoporotic females to determine whether changes in oestrogen status result in significant modulation of these TNFSF members
Summary
Oestrogen-deficiency induced by menopause is associated with reduced bone density and primary osteoporosis, resulting in an increased risk of fracture. Several mechanisms are known to contribute to the pathology of menopause-induced primary osteoporosis such as increased expression of tumour necrosis factor (TNF) superfamily members TNFα (TNFSF2) and receptor activator of nuclear factor kappa-B ligand (RANKL; TNFSF11) [6,7,8,9,10,11]. It is currently unknown what role other members of the TNFSF play in this pathological bone loss. This study focused on the TNFSF members TNF-like protein 1A (TL1A, TNFSF15) and its only confirmed trans-membrane receptor, death receptor 3 (DR3; TNFRSF25) [12]
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