Juan M. Dellacha scite author profile

The somatotropic and lactotropic receptors were studied in liver microsomal preparations from transgenic mice carrying the human growth hormone (hGH) or bovine growth hormone (bGH) gene fused to mouse metallothionein-I (MT) or phosphoenolpyruvate carboxykinase promoter/regulator (PEPCK). Specificity studies indicated that, similarly to normal mice, liver microsomes from the transgenic animals possess a mixed population of somatotropic and lactotropic binding sites. In transgenic animals of both sexes, the binding capacity of somatotropic receptors was significantly increased without corresponding changes in affinity. Expression of the MT-hGH hybrid gene was associated with the induction of somatotropic receptors which was approximately twice as great as that measured in animals expressing the MT-bGH hybrid gene. The binding capacity of lactotropic receptors in liver microsomes (quantitated by the use of labelled ovine prolactin) was increased 2-3 fold in transgenic females and approximately 10-fold in transgenic males as compared to the respective normal controls. We conclude that lifelong excess of GH up-regulates hepatic GH and prolactin receptors, and that lactogenic activity of GH is not essential for induction of prolactin receptors in the liver of transgenic mice.

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Specific Binding of Iodinated Growth Hormone to Rat Liver in Vivo*

Turyn¹,

Dellacha²

1978

Endocrinology

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The specific uptake by rat liver of human (hGH) and bovine (bGH) GHs labeled with 125I was studied by an in vivo procedure. A significant reduction of the uptake was observed when labeled hormones were injected together with different amounts of the corresponding native GH. This reduction was dose dependent, and the concentration of native hormone that prevents 50% of the liver uptake of the labeled hormone was close to 12 microgram/100 g BW. In normal rats, only native hGH or bGH significantly decreased the liver uptake of [125I]iodo-bGH, while bovine PRL (oPRL) or heat-denatured bGH were inactive. The highest inhibition of the uptake of [125I]iodo-hGH by rat liver was obtained when this labeled hormone was injected either together with hGH or with bGH plus oPRL while partial displacement was observed with bGH or oPRL. These data suggest that hGH binds to both somatotropic and lactogenic sites in the liver of normal rats. In hypophysectomized animals, only the somatogenic binding sites could be detected.

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Juan M. Dellacha

CHEMICAL AND BIOLOGICAL CHARACTERIZATION OF CLINICALLY ACTIVE TRYPTIC DIGESTS OF BOVINE GROWTH HORMONE^*

Somatotropic and lactotropic receptors in transgenic mice expressing human or bovine growth hormone genes

Specific Binding of Iodinated Growth Hormone to Rat Liver in Vivo*

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Juan M. Dellacha

CHEMICAL AND BIOLOGICAL CHARACTERIZATION OF CLINICALLY ACTIVE TRYPTIC DIGESTS OF BOVINE GROWTH HORMONE*

Somatotropic and lactotropic receptors in transgenic mice expressing human or bovine growth hormone genes

Specific Binding of Iodinated Growth Hormone to Rat Liver in Vivo*

Contact Info

Product

Resources

About

CHEMICAL AND BIOLOGICAL CHARACTERIZATION OF CLINICALLY ACTIVE TRYPTIC DIGESTS OF BOVINE GROWTH HORMONE^*