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Search for Circulating Immune Complexes and Activation of the Complement System in Relation to Estrogen Treatment
Author(s) -
Bukh Anne,
Jensen Hakon Kaalund,
Andersen Hans Jakob,
Eriksen Peter Bonne,
Peter Niels,
Möller Hundahl
Publication year - 1987
Publication title -
acta obstetricia et gynecologica scandinavica
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.401
H-Index - 102
eISSN - 1600-0412
pISSN - 0001-6349
DOI - 10.3109/00016348709004147
Subject(s) - estrogen , complement system , immune system , medicine , hormone , endocrinology , luteal phase , immunology
By employing an ammonium sulphate precipitation technique, previous studies have shown circulating immune complexes (cIC) in an increased proportion of women using oral contraceptives, as compared with non‐users. The pathogenicity of cIC is well established, as deposition in organs may lead to activation of the complement system and thereby inflammation and tissue destruction. The purpose of the present study was to determine whether estrogen treatment could induce the formation of cIC, as measured by more specific immune complex assays. To test for complement activation, plasma samples were analysed for the complement split product C3d. Thirty‐one women treated with estrogen for menopausal hormone deficiency symptoms and 38 untreated controls were analysed for cIC. Using a solid‐phase Clq‐anti‐lgG binding assay, the mean level of clC in the estrogen‐treated group did not differ significantly from that of the untreated control group (p>0.05). In a solid‐phase Clq‐protein A binding assay a very small average increase in the clC values for the estrogen–treated group in comparison with the untreated group was found, expressing a significant difference (p = 0.04). Moreover, the C3d levels for the estrogen–treated group did not differ from the untreated control group. Finally, no differences could be demonstrated in cIC and C3d levels between patients treated with synthetic estrogens and patients treated with natural estrogens.

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