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Regulation of prolactin in mice with altered hypothalamic melanocortin activity
Authors:Roxanne Dutia  Andrea J Kim  Eugene Mosharov  Eriika Savontaus  Streamson C Chua  Sharon L Wardlaw
Institution:Department of Medicine, Columbia University College of Physicians & Surgeons, New York, NY, United States.
Abstract:This study used two mouse models with genetic manipulation of the melanocortin system to investigate prolactin regulation. Mice with overexpression of the melanocortin receptor (MC-R) agonist, α-melanocyte-stimulating hormone (Tg-MSH) or deletion of the MC-R antagonist agouti-related protein (AgRP KO) were studied. Male Tg-MSH mice had lower blood prolactin levels at baseline (2.9±0.3 vs. 4.7±0.7ng/ml) and after restraint stress (68±6.5 vs. 117±22ng/ml) vs. WT (p<0.05); however, pituitary prolactin content was not different. Blood prolactin was also decreased in male AgRP KO mice at baseline (4.2±0.5 vs. 7.6±1.3ng/ml) and after stress (60±4.5 vs. 86.1±5.7ng/ml) vs. WT (p<0.001). Pituitary prolactin content was lower in male AgRP KO mice (4.3±0.3 vs. 6.7±0.5μg/pituitary, p<0.001) vs. WT. No differences in blood or pituitary prolactin levels were observed in female AgRP KO mice vs. WT. Hypothalamic dopamine activity was assessed as the potential mechanism responsible for changes in prolactin levels. Hypothalamic tyrosine hydroxylase mRNA was measured in both genetic models vs. WT mice and hypothalamic dopamine and 3,4-dihydroxyphenylacetic acid (DOPAC) content were measured in male AgRP KO and WT mice but neither were significantly different. However, these results do not preclude changes in dopamine activity as dopamine turnover was not directly investigated. This is the first study to show that baseline and stress-induced prolactin release and pituitary prolactin content are reduced in mice with genetic alterations of the melanocortin system and suggests that changes in hypothalamic melanocortin activity may be reflected in measurements of serum prolactin levels.
Keywords:ACTH  adrenocorticotropin  AgRP  agouti-related protein  β-EP  β-endorphin  CMV  cytomegalovirus  D2R  dopamine type-2 receptor  DHBA  3  4-dihydroxybenzylamine  DOPA  3  4-dihydroxyphenylalanine  DOPAC  3  4-dihydroxyphenylacetic acid  MBH  mediobasal hypothalamus  MC-R  melanocortin receptor  α-MSH  α-melanocyte-stimulating hormone  PCA  perchloric acid  POMC  proopiomelanocortin  Tg-MSH  MSH-overexpressing mice  TIDA  tuberoinfundibular dopaminergic
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