Prolactin potentiates insulin-stimulated leptin expression and release from differentiated brown adipocytes

Viengchareun, Say; Bouzinba-Ségard, Haniaa; Jp, Laigneau; Zennaro, Maria-Christina; Kelly, P. A.; Bado, André; Lombès, Marc; Binart, Nadine

doi:10.1677/jme.1.01563

Cited by 34 publications

(25 citation statements)

References 45 publications

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“…In mouse adipocytes, PRL alone has no effect on leptin release but it inhibits the insulin-induced production of leptin [33]. Conversely, when combined with insulin, PRL increases leptin release from brown adipocytes, which contradicts the higher concentration of leptin in brown adipose tissue in PRL receptor-deficient mice [34]. The present study showed that serum leptin levels did not differ with PRL treatment among diabetic groups.…”

Section: Discussioncontrasting

confidence: 66%

Serum prolactin concentrations determine whether they improve or impair β‐cell function and insulin sensitivity in diabetic rats

Park

Kim

Daily³

et al. 2011

Diabetes Metabolism Res

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Section: Discussioncontrasting

confidence: 66%

Serum prolactin concentrations determine whether they improve or impair β‐cell function and insulin sensitivity in diabetic rats

Park

Kim

Daily³

et al. 2011

Diabetes Metabolism Res

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“…The cross talk between prolactin and insulin signaling pathway in brown adipocytes demonstrated that prolactin potentiates insulin-stimulated secretion of leptin by brown adipose tissue (Viengchareun et al, 2004). In PCOS patients with hyperprolactinemia other causes must be investigated because hyperprolactinemia is not a clinical manifestation of PCOS (Filno et al, 2007).…”

Section: Discussionmentioning

confidence: 99%

Leptin levels in relation to marital status and neuroendocrine function in Iraqi females with polycystic ovary syndrome

Khalaf

2010

Saudi Pharmaceutical Journal

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The present study was designed to evaluate the relationship between serum leptin levels and the hormones related to fertility in Iraqi females with polycystic ovary syndrome (PCOS) and marital status. This study was conducted during the period from July to December 2007. Twenty-four women (12 married and 12 unmarried) with PCOS and not maintained on any type of therapy were included in the study. Twelve healthy and normal ovulatory women with an age range matched with that of PCOS women were included. After an overnight fasting, blood samples were drawn from all women at random days. While in those with regular menstrual cycles, blood samples were obtained during the follicular phase of the cycle, except for samples utilized for the assay of progesterone that performed in the day 21 of the cycle (luteal phase). After preparation of serum, the levels of leptin, luteinizing hormone (LH), follicle-stimulation hormone (FSH), progesterone, testosterone and prolactin were analyzed. Both groups of PCOS patients showed significantly lower levels of serum leptin, while prolactin, LH and FSH and testosterone were significantly elevated compared to controls. No significant differences were reported among PCOS patients with different marital status. In conclusion, impaired plasma leptin levels in PCOS women were associated with impaired endocrinological parameters related to fertility.

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“…169 resistin, 170 leptin 171 and adiponectin 172 are produced by fat during pregnancy in mice. Prl receptor signaling can regulate adipokine expression, 173,174,175 suggesting the possibility that while the mouse placenta is not the direct source of all metabolic hormones, unlike humans, it may still orchestrate the network. The best evidence in mice that placental hormones regulate fetal growth is that of the pleckstrin homology-like domain, family A member 2 gene which regulates the fetal growth by influencing the number of endocrine cells in the placenta.…”

Section: Review Of Placental Development and Function In The Contementioning

confidence: 99%

Placental origins of adverse pregnancy outcomes: potential molecular targets: an Executive Workshop Summary of the Eunice Kennedy Shriver National Institute of Child Health and Human Development

Ilekis

Tsilou

Fisher

et al. 2016

American Journal of Obstetrics and Gynecology

232

167

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Although much progress is being made in understanding the molecular pathways in the placenta involved in the pathophysiology of pregnancy related disorders, a significant gap exists in utilizing this information for developing new drug therapies to improve pregnancy outcome. On March 5–6, 2015, the Eunice Kennedy Shriver National Institute of Child Health and Human Development of the National Institutes of Health sponsored a two day workshop titled Placental Origins of Adverse Pregnancy Outcomes: Potential Molecular Targets to begin to address this gap. Particular emphasis was given in the identification of important molecular pathways that could serve as drug targets and the advantages and disadvantages of targeting these particular pathways. This article is a summary of the proceedings of this workshop. A broad number of topics were covered ranging from basic placental biology to clinical trials. This included research in the basic biology of placentation, such as trophoblast migration and spiral artery remodeling, and trophoblast sensing and response to infectious and non-infectious agents. Research findings in these areas will be critical for formulating developing future treatments and developing therapies for the prevention of a number of pregnancy disorders of placental origin including preeclampsia, fetal growth restriction, and uterine inflammation. Research was also presented summarizing ongoing clinical efforts in the U.S. and in Europe testing novel interventions for preeclampsia and fetal growth restriction, including agents such as oral arginine supplementation, sildenafil, pravastatin, gene therapy using virally-delivered vascular endothelial growth factor, and oxygen supplementation therapy. Strategies were also proposed to improve fetal growth by enhancing nutrient transport to the fetus by modulating their placental transporters, as well as targeting placental mitochondrial dysfunction and oxidative stress to improve placental health. The roles of microRNAs and placental-derived exosomes, as well as messenger RNAs, were also discussed in the context of their use for diagnostics and as drug targets. The workshop discussed the aspect of safety and pharmacokinetic profiles of potential existing and new therapeutics that will need to be determined especially in the context of the unique pharmacokinetic properties of pregnancy, as well as the hurdles and pitfalls of translating research findings into practice. The workshop also discussed novel methods of drug delivery and targeting during pregnancy using macromolecular carriers, such as nanoparticles and biopolymers, to minimize placental drug transfer and hence fetal drug exposure. In closing, a major theme that developed from the workshop was that the scientific community needs to change their thinking of the pregnant women and her fetus as a vulnerable patient population for which drug development should be avoided, but rather thought of as a deprived population in need of more effective therapeutic interventions.

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Prolactin potentiates insulin-stimulated leptin expression and release from differentiated brown adipocytes

Cited by 34 publications

References 45 publications

Serum prolactin concentrations determine whether they improve or impair β‐cell function and insulin sensitivity in diabetic rats

Serum prolactin concentrations determine whether they improve or impair β‐cell function and insulin sensitivity in diabetic rats

Leptin levels in relation to marital status and neuroendocrine function in Iraqi females with polycystic ovary syndrome

Placental origins of adverse pregnancy outcomes: potential molecular targets: an Executive Workshop Summary of the Eunice Kennedy Shriver National Institute of Child Health and Human Development

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