Hormonal control of postnatal development of corticosteroid-binding globulin

Abstract

The hormonal regulation of the ontogenic rise in serum corticosteroid-binding globulin (CBG) was studied in the rat. Pups received daily injections of estrogens (either estradiol, estrone, or diethylstilbesterol, each at 0.05 .mu.g/g body wt) or thyroxine [T4] (0.1 .mu.g/g body wt) on postnatal days 2-7. When CBG binding capacity was determined on day 8, only the T4-injected pups had elevated CBG. This effect of T4 on CBG binding capacity was further studied by daily administration of the hormone (0.1 .mu.g .cntdot. g body wt-1 .cntdot. day-1) between postnatal days 5-12. This caused a precocious rise in serum CBG, with CBG values 6- to 38-fold higher than euthyroid controls on days 8, 10, and 12. Conversely, in pups made hypothyroid by administration of propylthiouracil, the normal ontogenic increase in CBG was suppressed. T4 replacement resulted in the reappearance of the CBG rise. The developmental rise in the binding capacity of CBG is apparently independent of estradiol and estrone and instead is elicited by the rising concentrations of circulating T4 that normally occur in the early postnatal period.