Possible oncostatic action of cysteamine on the pituitary glands of oestrogen-primed hyperprolactinaemic rats.

TitlePossible oncostatic action of cysteamine on the pituitary glands of oestrogen-primed hyperprolactinaemic rats.
Publication TypeJournal Article
Year of Publication1990
AuthorsJeitner TM, Oliver JR
JournalJ Endocrinol
Volume127
Issue1
Pagination119-27
Date Published1990 Oct
ISSN0022-0795
KeywordsAnimals, Antineoplastic Agents, Body Weight, Cysteamine, Dose-Response Relationship, Drug, Estradiol, Growth Hormone, Hyperprolactinemia, Liposomes, Male, Organ Size, Pituitary Gland, Prolactin, Prolactinoma, Radioimmunoassay, Rats
Abstract

Cysteamine was investigated for its potential to reduce the size and secretion of oestrogen-primed hyperprolactinaemic rat pituitary glands. Subcutaneous administration of 80 and 120 mg cysteamine/kg significantly reduced plasma prolactin concentrations by 58 and 91% respectively, after 4h. Administration of cysteamine (60 mg s.c./kg body weight per day) for 10 days, to rats which had received an injection of 2 mg oestradiol benzoate on day 1, resulted in a significant reduction in pituitary mass (19%) and GH concentration (21%). Oral administration of 60 mg cysteamine/kg body weight to hyperprolactinaemic rats also produced a significant reduction in plasma prolactin of 94% after 2h. Oral administration of 60 mg cysteamine/kg body weight per day to rats for a 20-day period, during which they had received two injections of 2 mg oestradiol benzoate on day 1 and day 14 of treatment, resulted in a significant reduction in pituitary mass (29%) and the concentration of trunk blood prolactin concentration (35%). However, when oral cysteamine (60 mg cysteamine/kg body weight per day) was given for 20 days to rats which had been treated with 2 mg oestradiol benzoate once every 14 days over a 90-day period, it caused no change in pituitary weight, prolactin or GH concentration, or the concentration of prolactin in trunk blood.(ABSTRACT TRUNCATED AT 250 WORDS)

DOI10.1677/joe.0.1270119
Alternate JournalJ Endocrinol
PubMed ID2103572
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