Early embryonic blood cells collect antigens and induce immunotolerance in the hatched chicken

Earlier experimental data in our laboratory showed that introduction of an exogenous protein into early chicken embryonic blood leads to immunotolerance of hatched chicken to that protein. However, the underlying mechanism is yet unknown. In the present study, we show that the blood cells collecting...

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Bibliographic Details
Published in:Poultry science 2010-03, Vol.89 (3), p.457-463
Main Authors: Wu, G.J, Yuan, F, Du, M.H, Han, H.T, Lu, L.Q, Yan, L, Zhang, W.X, Wang, X.P, Sun, P, Li, Z.D
Format: Article
Language:English
Subjects:
Animals
antibodies
Antibodies - immunology
antigens
Antigens - blood
B-lymphocytes
B-Lymphocytes - physiology
blood cells
bovine serum albumin
Chick Embryo
chickens
Chickens - blood
Chickens - immunology
chicks
embryo (animal)
embryogenesis
Fluorescein-5-isothiocyanate - analogs & derivatives
Fluorescein-5-isothiocyanate - metabolism
immune response
Immune Tolerance - immunology
immunity
immunotolerance
lymphocytes
self-tolerance
Serum Albumin, Bovine - metabolism
T-lymphocytes
T-Lymphocytes - physiology
trinitrophenol
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Summary:Earlier experimental data in our laboratory showed that introduction of an exogenous protein into early chicken embryonic blood leads to immunotolerance of hatched chicken to that protein. However, the underlying mechanism is yet unknown. In the present study, we show that the blood cells collecting circulating antigen might contribute to the establishment of immunotolerance. In this experiment, most of the chicken embryo blood cells took up injected fluorescein isothiocyanate-BSA at approximately embryonic d 3. At the same stage, 1 μL of embryo blood was taken out and incubated with BSA. After being loaded with BSA in vitro and washed, these cells were injected back into the original embryo. The BSA-specific lymphocytes were depleted in chickens whose early embryo cells had been loaded with BSA, as evidenced by a significant decrease in anti-BSA antibody after challenge with BSA when the chickens were 3 wk old. In addition, by direct injection of BSA to embryonic d 3 embryo blood, the hatched chickens had decreased amounts of anti-trinitrophenol antibody after the chickens were challenged with trinitrophenol-BSA, indicating that the helper function of BSA-specific T cells was impaired. In conclusion, these observations suggest that some early embryo blood cells possibly collect and store antigen for the establishment of self-tolerance before the maturation of B and T cells.
ISSN:0032-5791
1525-3171
DOI:10.3382/ps.2009-00437