A Reassessment of the Therapeutic Potential of a Dopamine Receptor 2 Agonist (D2-AG) in Endometriosis by Comparison against a Standardized Antiangiogenic Treatment

6533b7dcfe1ef96bd1272b0d

RESEARCH PRODUCT

A Reassessment of the Therapeutic Potential of a Dopamine Receptor 2 Agonist (D2-AG) in Endometriosis by Comparison against a Standardized Antiangiogenic Treatment

Juan J. Tarín Antonio Cano Ana I Santos-llamas Raúl Gómez María José Fernández-ramírez Miguel Angel Tejada

subject

endometriosis 0301 basic medicine Agonist Angiogenesis medicine.drug_class Endometriosis dopamine agonist Medicine (miscellaneous)Dopamine agonist Article General Biochemistry Genetics and Molecular Biology Lesion 03 medical and health sciences heterologous mouse model 0302 clinical medicine In vivo Cabergoline medicine lcsh:QH301-705.5 030219 obstetrics & reproductive medicine business.industry antiangiogenic medicine.disease 030104 developmental biology lcsh:Biology (General)anti-VEGF Dopamine receptor Cancer research medicine.symptom business medicine.drug

description

Dopamine receptor 2 agonists (D2-ags) have been shown to reduce the size of tumors by targeting aberrant angiogenesis in pathological tissue. Because of this, the use of a D2-ag was inferred for endometriosis treatment. When assayed in mouse models however, D2-ags have been shown to cause a shift of the immature vessels towards a more mature phenotype but not a significant reduction in the amount of vascularization and size of lesions. These has raised concerns on whether the antiangiogenic effects of these compounds confer a therapeutic value for endometriosis. In the belief that antiangiogenic effects of D2-ags in endometriosis were masked due to non-optimal timing of pharmacological interventions, herein we aimed to reassess the antiangiogenic therapeutic potential of D2-ags in vivo by administering compounds at a timeframe in which vessels in the lesions are expected to be more sensitive to antiangiogenic stimuli. To prove our point, immunodeficient (NU/NU) mice were given a D2-ag (cabergoline), anti-VEGF (CBO-P11) or vehicle (saline) compounds (n = 8 per group) starting 5 days after implantation of a fluorescently labeled human lesion. The effects on the size of the implants was estimated by monitoring the extent of fluorescence emitted by the lesion during the three-week treatment period. Subsequently mice were sacrificed and lesions excised and fixed for quantitative immunohistochemical/immunofluorescent analysis of angiogenic parameters. Lesion size, vascular density and innervation were comparable in D2-ag and anti-VEGF groups and significantly decreased when compared to control. These data suggest that D2-ags are as powerful as standard antiangiogenic compounds in interfering with angiogenesis and lesion size. Our preliminary study opens the way to further exploration of the mechanisms beneath the antiangiogenic effects of D2-ags for endometriosis treatment in humans.

year	journal	country	edition	language
2021-03-01	Biomedicines

https://doi.org/10.3390/biomedicines9030269