Low-dose dopamine agonist administration blocks vascular endothelial growth factor (VEGF)-mediated vascular hyperpermeability without altering VEGF receptor 2-dependent luteal angiogenesis in a rat ovarian hyperstimulation model.

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RESEARCH PRODUCT

Low-dose dopamine agonist administration blocks vascular endothelial growth factor (VEGF)-mediated vascular hyperpermeability without altering VEGF receptor 2-dependent luteal angiogenesis in a rat ovarian hyperstimulation model.

Ralf C. Zimmermann Miguel Gonzalez-izquierdo Antonio Pellicer Isabel Alonso-muriel José E. Sánchez-criado José Remohí Carlos Simón Raúl Gómez Edurne Novella-maestre

subject

Agonist Vascular Endothelial Growth Factor A medicine.medical_specialty Cabergoline medicine.drug_class Angiogenesis Ovarian hyperstimulation syndrome Neovascularization Physiologic Biology Dopamine agonist Capillary Permeability chemistry.chemical_compound Ovarian Hyperstimulation Syndrome Endocrinology Corpus Luteum Internal medicine Cabergoline medicine Animals RNA Messenger Ergolines Phosphorylation Rats Wistar Receptors Dopamine D2 Kinase insert domain receptor Receptor antagonist medicine.disease Vascular Endothelial Growth Factor Receptor-2 Rats Vascular endothelial growth factor Disease Models Animal Endocrinology chemistry Dopamine Agonists Female medicine.drug

description

No specific treatment is available for ovarian hyperstimulation syndrome (OHSS), the most important complication in infertile women treated with gonadotropins. OHSS is caused by increased vascular permeability (VP) through ovarian hypersecretion of vascular endothelial growth factor (VEGF)activating VEGF receptor 2 (VEGFR-2). We previously demonstrated in an OHSS rodent model that increased VP was prevented by inactivating VEGFR-2 with a receptor antagonist(SU5416).However,duetoitstoxicity(thromboembolism) and disruption of VEGFR-2-dependent angiogenic processes critical for pregnancy, this kind of compound cannot be used clinically to prevent OHSS. Dopamine receptor 2 (Dp-r2) agonists, used in the treatment of human hyperprolactinemia including pregnancy, inhibit VEGFR-2-dependent VP and angiogenesis when administered at high doses in animal cancer models. To test whether VEGFR-2-dependent VP and angiogenesis could be segregated in a dose-dependent fashion with the Dp-r2 agonist cabergoline, a well-established OHSS rat model supplemented with prolactin was used. A 100 g/kg low-dose Dp-r2 agonist cabergoline reversed VEGFR-2-dependent VP without affecting luteal angiogenesis through partial inhibition of ovarian VEGFR-2 phosphorylation levels. No luteolytic effects (serum progesterone levels and luteal apoptosis unaffected) were observed. Cabergoline administration also did not affect VEGF/VEGFR-2 ovarian mRNA levels. Results in the animal model and the safe clinical profile of Dp-r2 agonists encouraged us to administer cabergoline to oocyte donorsathighriskfordevelopingthesyndrome.Prophylactic administration of cabergoline (5–10 g/kgd) decreased the occurrence of OHSS from 65% (controls) to 25% (treatment). Therefore, a specific, safe treatment for OHSS is now available. (Endocrinology 147: 5400–5411, 2006)

year	journal	country	edition	language
2006-08-12	Endocrinology

10.1210/en.2006-0657 https://pubmed.ncbi.nlm.nih.gov/16901966