Interleukin Regulation of Asymmetric Antibody Synthesized by Isolated Placental B Cells

CANELLADA, ANDREA; FARBER, ANGELA; ZENCLUSSEN, ANA; GENTILE, TERESA; DOKMETJIAN, JOSE; KEIL, ANJA; BLOIS, SANDRA; MIRANDA, SILVIA; BEROD, LUCIANA; GUTIÉRREZ, GABRIELA; MARKERT, UDO; MARGNI, RICARDO

AMERICAN JOURNAL OF REPRODUCTIVE IMMUNOLOGY

Blackwell Munksgaard

Año: 2002 vol. 48 p. 275 - 282

8755-8920

PROBLEM: Protecting antibodies against trophoblast surface molecules were previously described. Here we analysed the synthesis of asymmetric IgG by placental B-lymphocytes. METHOD OF STUDY: B cells were isolated from human term placenta and cord blood, stimulated with anti-CD40 IgG and cocultured with transfected Fcgamma R-expressing mice Ltk-fibroblast. Interleukin-4, IL-6, IL-10, IL-11 and IL-13 were added to cultures for 14 days. Asymmetric IgG were assessed in culture supernatants by concanavalin A (Con A) fixation and enzyme-linked immunosorbent assay. RESULTS: When IL-6 was added to the cultures, the percentages of asymmetric IgG synthesized by placental B cells were: IL-6: 29 +/- 10; IL-6 + IL-10: 24 +/- 7; IL-4 + IL-10 + IL-6: 38 +/- 9. The last combination induced the highest increase in the asymmetric IgG synthesis as compared with control (19 +/- 10%, P < 0.05). Additionally, placental B cells synthesized more asymmetric IgG than umbilical cord blood B-lymphocytes (P = 0.0015). CONCLUSIONS: Isolated placental B-lymphocytes synthesized asymmetric IgG in response to Th2 interleukins, more notably IL-6 in combination with IL-4 and IL-10. The in vitro increase of protective asymmetric IgG synthesis in response to Th2-cytokines support the hypothesis that a local Th2-switch is beneficial for pregnancy outcome.