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[Effect of 7,12-dimethylbenz(a)athrancene on immune function in metallothionein gene-knocked-out mice]. | LitMetric

[Effect of 7,12-dimethylbenz(a)athrancene on immune function in metallothionein gene-knocked-out mice].

Zhonghua Yu Fang Yi Xue Za Zhi

Department of Toxicology, School of Public Health, Peking University, Beijing 100083, China.

Published: November 2002

AI Article Synopsis

  • This study examines the immunotoxic effects of DMBA on mice lacking metallothionein (MT), comparing them to normal mice with MT.
  • Female mice were treated with different doses of DMBA and immune functions were assessed through various tests like spleen weight and antibody response.
  • Results showed significant suppression of humoral immune function in MT(-/-) mice, indicating that the presence of metallothionein helps protect against DMBA-induced immune damage.

Article Abstract

Objective: To study the immunotoxicity induced by 9,10-dimethyl-1,2-benzathrancene (DMBA) in metallothionein gene-knocked-out mice [MT(-/-)] as compared with that in wild-type mice [(MT(+/+)].

Methods: Female mice were treated with 25 mg/kg and 50 mg/kg of DMBA i.p., respectively and immunized with sheep red blood cells (SRBC) i.v. on the following day and rechallenged by injection of SRBC via footpad s.c. on the fourth day post-immunization. Humoral and cell-mediated immune function was assessed by the number of spleen IgM antibody plaque formation cells (PFC) to SRBC and cell-mediated delayed-type hypersensitivity (DTH) measured by footpad swelling thickness.

Results: After treatment with 25 mg/kg DMBA, a decrease in weight of their spleen and thymus and PFC/spleen were observed in MT(-/-) mice, while only decrease in thymus weight of MT(+/+) mice. The humoral function was suppressed by 72% in MT(-/-) mice. No obvious change in cell-mediated immune function was observed both in MT(-/-) and MT(+/+) mice. Both humoral and cell-mediated immune function were suppressed more severe (91%) in MT(-/-) mice treated with 50 mg/kg DMBA than those treated with 25 mg/kg DMBA (72%). DTH was not altered by DMBA in MT(+/+) mice. The weight of their spleen and thymus decreased and humoral immune function suppressed in MT(+/+) mice, but these changes were significantly less severe. No obvious suppression of cell-mediated immune function was observed in MT(+/+) mice.

Conclusion: Their humoral and cell-mediated immune function was more susceptible to being suppressed by DMBA in MT(-/-) mice, indicating that MT could protect their immune function from damage caused by DMBA.

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