Thymic
atrophy and humoral immunosuppression by certain
polychlorinated biphenyls is associated with the
aromatic hydrocarbon (
Ah) receptor in mice. We examined the relationship between these two toxic effects.
3,3',4,4'-Tetrachlorobiphenyl (TCB), which causes immunosuppression and thymic
atrophy, and
2,3,3',4,4',5-hexachlorobiphenyl, which causes immunosuppression without thymic
atrophy, were administered i.p. to C57BL/6 mice at 0, 35 and 350 mumol/kg b.wt. 2 days before i.v. immunization with 10 micrograms of Escherichia coli
lipopolysaccharide. Both congeners caused significant suppression of the day 4 anti-
lipopolysaccharide plaque-forming cell response/spleen (less than or equal to 46% of control). TCB (350 mumol/kg) was also administered 2 days before either a primary or secondary i.p. immunization with sheep erythrocytes. TCB treatment before primary immunization had no effects on the day 5 secondary response, whereas treatment before the secondary immunization significantly inhibited both day 5
immunoglobulin M and
immunoglobulin G plaque-forming cells (less than 10 and less than 2% of control, respectively) and decreased serum antibody. TCB administered either 8 or 2 days before or 2 or 4 days after immunization with sheep erythrocytes demonstrated that significant suppression of both plaque-forming cells and serum antibody could occur without thymic
atrophy. Immunity was most impaired when TCB was given 2 days before immunization. These results demonstrate that thymic
atrophy does not always accompany the severe immunosuppression caused by
Ah receptor ligands and suggests that it may not be a sensitive measure of
Ah receptor-mediated immunosuppression. The data also suggests that differentiation of B lymphocytes into antibody producing cells is impaired during
Ah receptor-mediated gene activation.