Comparison of the Effect of Several Gonadotropin Releasing Hormone Antagonists on Luteinizing Hormone Secretion, Receptor Binding and Ovulation
Open Access
- 1 September 1983
- journal article
- research article
- Published by Oxford University Press (OUP) in Biology of Reproduction
- Vol. 29 (2) , 374-378
- https://doi.org/10.1095/biolreprod29.2.374
Abstract
The biological activity of three gonadotropin releasing hormone (GnRH) antagonists was evaluated in the following assays: suppression of GnRH-mediated luteinizing hormone (LH) secretion by cultured pituitary cells, suppression of the spontaneous LH release by ovariectomized rats, blockade of ovulation in regularly cycling females and inhibition of binding of a potent radiolabeled agonist to rat pituitary membrane homogenates. The peptides were:2 [Ac-Δ3Pro1,4FDPhe2, DTrp3,6]-GnRH (Antagonist 1); [Ac-Δ3Pro1,4FDPhe2,DNAL(2)3,6]-GnRH (Antagonist 2); and [Ac-DNAL(2)2,4FDPhe2,DTrp3,DArg6]-GnRH (Antagonist 3). All three antagonists exhibited similarly high potency in suppressing LH secretion in vitro, while Antagonist 1 was the most active peptide in the radioreceptor assay. When administered by gavage, Antagonist 3 exhibited the highest potency to inhibit LH secretion in gonadectomized rats and to block ovulation. Comparison of the oral versus the subcutaneous mode of administration of these analogs indicates that less than 1% is absorbed after gavage. However, these data demonstrate that the intragastric administration of GnRH antagonists can lower gonadotropin secretion and interfere with reproductive functions.This publication has 14 references indexed in Scilit:
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