Zobrazeno 1 - 10
of 15
pro vyhledávání: '"D. J. Judah"'
Autor:
G. E. Neal, M. J. Nagler, Laurentius Hoogenboom, P. Carthew, L. Weir, A. Verma, R. D. Coker, I. Latour, D. J. Judah
Publikováno v:
Food Additives and Contaminants, 18(2), 137-149
Food Additives and Contaminants 18 (2001) 2
Food Additives and Contaminants 18 (2001) 2
A sample of peanut meal, highly contaminated with aflatoxins, has been subjected to decontamination by two commercial ammonia-based processes. The original contaminated and the two decontaminated meals were fed to rats for 90 days. No lesions associa
Publikováno v:
Journal of Biological Chemistry. 269:20707-20717
Fetal rat liver possesses substantial levels of glutathione S-transferase (GST) activity toward aflatoxin B1-8,9-epoxide. The enzyme responsible for this activity is an Alpha-class GST heterodimer comprising Yc1 and Yc2 subunits. The cDNAs encoding t
Autor:
V P, Kelly, E M, Ellis, M M, Manson, S A, Chanas, G J, Moffat, R, McLeod, D J, Judah, G E, Neal, J D, Hayes
Publikováno v:
Cancer research. 60(4)
Structurally diverse compounds can confer resistance to aflatoxin B1 (AFB1) hepatocarcinogenesis in the rat. Treatment with either phytochemicals [benzyl isothiocyanate, coumarin (CMRN), or indole-3-carbinol] or synthetic antioxidants and other drugs
Publikováno v:
Toxicology and applied pharmacology. 151(1)
Aflatoxin M 1 (AFM 1 ) is the principal hydroxylated aflatoxin metabolite present in the milk of dairy cows fed a diet contaminated with aflatoxin B 1 , (AFB 1 ) and the metabolite is also present in the milk of human nursing mothers consuming foodst
Publikováno v:
Cancer research. 57(19)
Fischer 344 rats fed on a diet that is deficient in selenium are more resistant to the hepatocarcinogen aflatoxin B1 (AFB1) than those fed on a selenium-sufficient diet. Hepatic cytosol from either selenium-deficient Fischer 344 rats or Hooded Lister
Autor:
J D, Hayes, R, McLeod, E M, Ellis, D J, Pulford, L S, Ireland, L I, McLellan, D J, Judah, M M, Manson, G E, Neal
Publikováno v:
IARC scientific publications. (139)
A number of xenobiotics, including the synthetic antioxidant ethoxyquin, inhibit aflatoxin B1 (AFB1)-induced hepatocarcinogenesis in the rat. Two detoxification enzymes that mediate ethoxyquin-induced chemoprotection against AFB1 have been identified
Publikováno v:
The Journal of biological chemistry. 269(32)
Fetal rat liver possesses substantial levels of glutathione S-transferase (GST) activity toward aflatoxin B1-8,9-epoxide. The enzyme responsible for this activity is an Alpha-class GST heterodimer comprising Yc1 and Yc2 subunits. The cDNAs encoding t
Publikováno v:
Cancer research. 53(17)
Fischer 344 rats readily develop liver cancer when exposed to aflatoxin B1 (AFB1) but dietary administration of the antioxidant ethoxyquin (EQ) provides protection against hepatocarcinogenesis. Chemoprotection by EQ is accompanied by the overexpressi
Publikováno v:
Hepatology (Baltimore, Md.). 18(1)
A need exists for an appropriate animal model for the involvement of both hepatitis B virus infection and ingestion of aflatoxins in the etiology of liver cancer. Duck hepatitis B virus-infected ducks, on the basis of hepatoma development in the wild
Publikováno v:
Carcinogenesis. 2:457-461