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Title: [A change in antigen presentation ability of spleen macrophage from Balb/c mouse during late pregnancy].
Author: Tan Z, Li S, Cao Z, Zhao Z, Ma Q, Huang Z, Li L.
Journal: Sichuan Da Xue Xue Bao Yi Xue Ban; 2003 Oct; 34(4):674-7. PubMed ID: 14619578.
Abstract:
OBJECTIVE: To study the antigen presentation ability of spleen macrophage from Balb/c mouse during late gestation. METHODS: The spleen of Balb/c mouse during late gestation was collected aseptically and macrophage was separated; the mice in estrus were used as control. The ability of macrophage to prime original T cells to human gamma globulin antigen (HGG-Ag) or placenta antigen (Pla-Ag) was evaluated by a delayed-type hyper sensitivity (DTH) response induced by the same antigen, and the ability of macrophage to induce the proliferation of primed normal T cells to HGG-Ag or Pla-Ag was assessed by an antigen special lymphocyte transformation in vitro. RESULTS: After being sensitized previously by spleen macrophage from Balb/c mice during late gestation that has been pulsed by HGG-Ag or Pla-Ag, the DTH intensity of mice response to the same antigen was significantly weaker than that being sensitized by macrophage from mice in estrus (P < 0.05). When spleen macrophage from Balb/c mice during late gestation was used as antigen presentation cell (APC), the proliferability of primed T cell induced by HGG-Ag or Pla-ag was significantly lower than that when macrophage from estrous Balb/c mouse was used in vitro (P < 0.05). CONCLUSION: The antigen presentation ability of spleen macrophage from Balb/c mouse is inhibited during late pregnancy. This may be the important mechanism by which maternal immune system tolerates embryo antigen and may be responsible for the down-regulation of maternal cell mediated immunity during pregnancy.

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