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Human hepatocellular carcinoma tumor xenografts
Authors:Dr Arthur A Dunk MRCP  Natasha Kyprianou MSc  Peter Davies PhD  Howard C Thomas PhD  FRCP
Institution:(1) Academic Department of Medicine, Royal Free Hospital and School of Medicine, Pond Street, NW3 2QG London, UK;(2) Tenovus Institute for Cancer Research, Welsh National School of Medicine, the Heath, CF4 4XX Cardiff, UK;(3) Gastroenterology Research Unit, Royal Infirmary, Room 1/055, 1st Floor, Phase I, AB9 2ZB Foresterhill, Aberdeen, UK
Abstract:Castrated or sham-operated male athymic mice were inoculated with cells from the human hepatocellular carcinoma cell line PLC/PRF/5. There were no significant differences between the two groups with respect to the number of animals developing tumors, the time to tumor development, or the subsequent rate of increase in either tumor base area or mouse serum alpha-fetoprotein concentration. Androgen receptors were assayed in nuclei obtained from three separate liver cancer cell lines and from normal adult human liver. Similar concentrations, ranging from 235 to 550 fmol/mg DNA, of nuclear androgen receptors were detected in all tissues. Low percentages of androgen receptors were retained on DNA-cellulose. Although the presence of receptors implies the potential for metabolic effects of androgens in normal and malignant liver, our in vivostudies suggest that castration does not alter significantly the growth of liver cancer xenografts in athymic mice.
Keywords:hepatocellular carcinoma  athymic mice  androgen receptors
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