4.6 Article

Bazedoxifene does not share estrogens effects on IgG sialylation

Journal

PLOS ONE
Volume 18, Issue 5, Pages -

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PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0285755

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The incidence of rheumatoid arthritis (RA) increases during menopause when estrogen levels decrease. Estrogen treatment can reduce the pathogenicity of IgG by increasing sialylation, inhibiting binding to the Fc gamma receptor. However, estrogen treatment has negative side effects, so selective estrogen receptor modulators (SERMs) with minimal side effects have been developed. In this study, the impact of the SERM bazedoxifene on IgG and serum protein sialylation was investigated.
The incidence of rheumatoid arthritis (RA) increases at the same time as menopause when estrogen level decreases. Estrogen treatment is known to reduce the IgG pathogenicity by increasing the sialylation grade on the terminal glycan chain of the Fc domain, inhibiting the binding ability to the Fc gamma receptor. Therefore, treatment with estrogen may be beneficial in pre-RA patients who have autoantibodies and are prone to get an autoimmune disease. However, estrogen treatment is associated with negative side effects, therefore selective estrogen receptor modulators (SERMs) have been developed that have estrogenic protective effects with minimal side effects. In the present study, we investigated the impact of the SERM bazedoxifene on IgG sialylation as well as on total serum protein sialylation. C57BL6 mice were ovariectomized to simulate postmenopausal status, followed by ovalbumin immunization, and then treated with estrogen (estradiol), bazedoxifene, or vehicle. We found that estrogen treatment enhanced IgG levels and had a limited effect on IgG sialylation. Treatment with bazedoxifene increased the sialic acids in plasma cells in a similar manner to E2 but did not reach statistical significance. However, we did not detect any alteration in IgG-sialylation with bazedoxifene treatment. Neither estrogen nor bazedoxifene showed any significant alteration in serum protein sialylation but had a minor effect on mRNA expression of glycosyltransferase in the bone marrow, gonadal fat, and liver.

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