Autor: |
Rao GN; National Institute of Environmental Health Sciences, Farnell DR; Southern Research Institute, Giles HD; Southern Research Institute, Kelley CA; Southern Research Institute, Lindamood C III; Southern Research Institute, Rogers TS; Southern Research Institute, Grimes LK; Environmental Health Research and Testing, Inc., Sexton TA; Environmental Health Research and Testing, Inc., Thomas M; Environmental Health Research and Testing, Inc., Brine D; Research Triangle Institute, Handy RW; Research Triangle Institute, Keller CD; Research Triangle Institute, Morris R; Analytical Sciences, Inc. |
Abstrakt: |
Male and female B6C3F 1 mice were dosed orally with AZT alone (100, 200, or 400 mg/kg), rifampicin alone (100, 200, or 400 mg/kg), or combinations of AZT and rifampicin for up to 94 days. Mice were evaluated for clinical findings, mean body weight, hematology and clinical chemistry parameters, and sperm function and vaginal cytology. All core study animals and the clinical pathology study animals that died early were necropsied and subjected to histopathological evaluations. A summary of the most significant toxicological parameters is presented in Table 1. AZT alone or rifampicin alone did not cause significant changes in body weights. Combination therapy with AZT and rifampicin caused marked and treatment-related decreases in body weights. The primary toxicity of AZT was bone marrow suppression manifested by macrocytic anemia, thrombocytosis, and reticulocytopenia followed by reticulocytosis. Bone marrow atrophy was observed microscopically and was considered the major drug-related effect. Administration of rifampicin alone resulted in both hematological toxicity and hepatotoxicity. Males and females developed a mild microcytic anemia and reticulocytopenia. Hepatotoxicity was manifested by increased liver enzymes in the serum, increased liver weights, and cytoplasmic vacuolization of hepatocytes. Administration of AZT and rifampicin in combination resulted in hematological toxicity of far greater magnitude than that observed subsequent to the administration of either drug alone. Marked anemia and bone marrow atrophy contributed to significant mortality in groups treated with the higher concentration combinations. Females were more sensitive to the hematological toxicity of combination therapies than the males, and the female mice died earlier than the males. Combination therapy with AZT and rifampicin did not exacerbate the hepatotoxicity induced by rifampicin alone. Serum enzyme levels, liver weights, and cytoplasmic vacuolization of hepatocytes were similar to those observed in mice treated with rifampicin alone. Treatment-related decreases occurred in absolute thymus weights of mice treated with the higher concentration combinations of AZT and rifampicin, and the decreased thymus weights corresponded with thymic atrophy. Testicular degeneration was observed in groups treated with AZT and rifampicin at 400mg/kg and 400mg of AZT + 200 mg of rifampicin. However, testicular degeneration was generally associated with anemia, lower testis weights, and decreased sperm motility. |