Abstract

We tested the hypothesis that tumor necrosis factor-α (TNF-α) would be teratogenic in mice due in part to its effects on zinc metabolism. In Experiment 1, nonpregnant mice were injected with a single dose of TNF-α (40,000 U) or PBS and then received a 65Zn-labeled meal. Mice killed 10 h after TNF-α treatment had high liver 65Zn and low plasma 65Zn, compared with controls. In Experiment 2, gestation day 8 (GD 8) mice were injected with PBS or TNF-α and then received a 65Zn-labeled meal. Dams killed 10 h after TNF-α treatment had higher liver and kidney 65Zn and lower plasma and embryonic 65Zn accumulation than controls. In Experiment 3, TNF-α dosing from GD 7–12 was associated with high maternal liver Zn and metallothionein concentrations on GD 13 and a high frequency of exencephaly on GD 18. In Experiment 4, dams fed diets containing 4.5, 12.5 or 50.0 µg Zn/g were given PBS or TNF-α on GD 7–12. Gross fetal defects were not observed in the PBS-treated litters evaluated on GD 18. In contrast, TNF-α-treated litters were characterized by multiple defects, with the incidence and severity being highest in the low Zn diet group. In Experiment 5, embryos cultured in serum from TNF-α-treated animals exhibited a high frequency of defects; the developmental toxicity of this serum was ameliorated when it was supplemented with Zn. Thus, the developmental toxicity of TNF-α is due in part to its influence on Zn metabolism.

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