Ikuya Shimizu scite author profile

Aims-To examine the eVects of oestradiol and testosterone on the early carcinogenic changes expressed in rat liver from the diethylnitrosamine (DEN), 2-acetylaminofluorene (AAF), partial hepatectomy (PH) model of hepatocarcinogenesis. Methods-Preneoplastic liver lesions were evaluated using immunohistochemical analysis of glutathione-S-transferase placental form (GST-P) expression; oestrogen and androgen receptor levels were measured by radioimmunoassay. Results-Oestradiol administration to non-castrated DEN-AAF-PH treated males resulted in a decrease in the area of GST-P positive foci, while testosterone increased the serum oestradiol level and reduced the area. In males, castration alone and castration with oestradiol replacement significantly reduced the GST-P positive area, and increased the hepatic oestrogen receptor level. In DEN-AAF-PH treated females, castration with testosterone replacement was associated with a significant increase in the GST-P positive area and the hepatic androgen receptor level. Conclusion-These findings suggest that exogenous and endogenous oestradiol can suppress chemical hepatocarcinogenesis. It appears that oestrogen receptors may be involved in the inhibition of malignant transformation of preneoplastic liver cells, while androgens and androgen receptors are involved in hepatocarcinogenesis.

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Relationship Between [³H]Mazindol Binding to Dopamine Uptake Sites and [³H]Dopamine Uptake in Rat Striatum During Aging

Shimizu

Prasad

1991

Journal of Neurochemistry

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Certain drugs exhibit a remarkable correlation between their ability to inhibit synaptosomal uptake of dopamine and the binding of [3H]mazindol to striatal membranes. To investigate the role of mazindol binding sites in the dopamine uptake process and the fate of these sites (labeling dopaminergic neurons) during aging, we have examined the properties of mazindol binding and dopamine uptake in individual young and old rats. There was a 48% decrease (p = 0.0001) in the Bmax of mazindol binding and a 23% decrease (p = 0.0166) in the Vmax of dopamine uptake with no apparent change in their affinities with age. Regression analysis of the relationship between Bmax and Vmax exhibited a significant correlation in old (p = 0.0156) but not young rats (p = 0.1398). These data suggest that the number of mazindol binding sites decreases with age and that the number of sites on the dopamine transporter complex far exceeds the number required to elicit maximal dopamine uptake.

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Ikuya Shimizu

Uterine Artery Doppler Velocimetry in Relation to Trophoblast Migration into the Myometrium of the Placental Bed

Growth inhibition by danazol in a human endometrial cancer cell line with estrogen-independent progesterone receptors

Suppressive effect of oestradiol on chemical hepatocarcinogenesis in rats

Relationship Between [³H]Mazindol Binding to Dopamine Uptake Sites and [³H]Dopamine Uptake in Rat Striatum During Aging

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Ikuya Shimizu

Uterine Artery Doppler Velocimetry in Relation to Trophoblast Migration into the Myometrium of the Placental Bed

Growth inhibition by danazol in a human endometrial cancer cell line with estrogen-independent progesterone receptors

Suppressive effect of oestradiol on chemical hepatocarcinogenesis in rats

Relationship Between [3H]Mazindol Binding to Dopamine Uptake Sites and [3H]Dopamine Uptake in Rat Striatum During Aging

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Product

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Relationship Between [³H]Mazindol Binding to Dopamine Uptake Sites and [³H]Dopamine Uptake in Rat Striatum During Aging