Abstract
Immunotherapy with anti-CD20-specific antibodies (rituximab), has become the standard of care for B cell lymphoproliferative disorders and many autoimmune diseases. In rheumatological patients the effect of rituximab on bone mass yielded conflicting results, while in lymphoma patients it has not yet been described. Here, we used cross-sectional X-ray imaging (CT/PET-CT) to serially assess bone density in patients with follicular lymphoma receiving rituximab maintenance therapy. Remarkably, this treatment prevented the decline in bone mass observed in the control group of patients who did not receive active maintenance therapy. In accordance with these data, anti-CD20-mediated B cell depletion in normal C57BL/6J female mice led to a significant increase in bone mass, as reflected by a 7.7% increase in bone mineral density (whole femur), and a ~5% increase in cortical as well as trabecular tissue mineral density. Administration of anti-CD20 antibodies resulted in a significant decrease in osteoclastogenic signals, including RANKL, which correlated with a reduction in osteoclastogenic potential of bone marrow cells derived from B-cell-depleted animals. Taken together, our data suggest that in addition to its anti-tumor activity, anti-CD20 treatment has a favorable effect on bone mass. Our murine studies indicate that B cell depletion has a direct effect on bone remodeling.
Highlights
Immunotherapy with anti-CD20-specific antibodies has become the standard of care for many hematological and autoimmune diseases [1]
We retrospectively evaluated the skeletal effects of rituximab in patients with low-grade lymphoma (FL), who were treated with rituximab in the setting of maintenance therapy, that is, a period when rituximab was administered periodically, as monotherapy
This study describes the effect of anti-CD20 antibody treatment on bone mass in hematological patients as well as in mice
Summary
Immunotherapy with anti-CD20-specific antibodies has become the standard of care for many hematological and autoimmune diseases [1]. Despite a significant amount of published research linking B cells to bone homeostasis [2,3,4,5], only a few studies have addressed the effect of anti-CD20 on bone mass in human patients, and no studies have yet addressed this issue in hematological patients. One study on rituximab treatment in patients with rheumatoid arthritis (RA), described an increase in lumbar spine BMD (bone mineral density) irrespective of clinical response, whereas in the femur, rituximab merely prevented bone loss, and only in responders [6]. Another study suggested that treatment with rituximab reduced osteoclast activity as assessed by serum markers of bone resorption [7], and a recent study, in RA patients [8], demonstrated a significant reduction in the femoral BMD with no effect in the spine. A similar effect was found in patients with systemic lupus erythematosus (female patients only), especially in those who attained a good clinical response to the treatment [9]
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