Hypoadiponectinemia in Lean Lactating Women: Prolactin Inhibits Adiponectin Secretion from Human Adipocytes

Asai‐Sato, Mikiko; Okamoto, M.; Endo, Mitsuaki; Yoshida, Hiroshi; Murase, M; Ikeda, Mario; Sakakibara, Hideya; Takahashi, Tsuneo; Hirahara, Fumiki

doi:10.1507/endocrj.k06-026

Cited by 67 publications

(56 citation statements)

References 34 publications

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“…Whereas serum adiponectin levels are unchanged in PRLR- [6] or PRL-knockout mice [25], PRL at very high doses inhibits adiponectin production in cultured human adipose tissue and in mice in vivo [6,31]. Lower circulating adiponectin levels were reported in lactating women, with inhibition of adiponectin production in cultured human adipocytes by PRL [32]. These discrepancies are likely due to differences in experimental design, doses of PRL, gender or species.…”

Section: Discussionmentioning

confidence: 99%

Prolactin upregulates its receptors and inhibits lipolysis and leptin release in male rat adipose tissue

Brandebourg

Bown

Ben‐Jonathan

2007

Biochemical and Biophysical Research Communications

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Prolactin (PRL) is recognized as a metabolic regulator during lactation, but little information exists on its actions in male adipose tissue. We examined whether PRL affects the expression of its receptors (PRLR), lipolysis and adipokine secretion in male rats. Both long and short PRLR isoforms were induced 40 to 50-fold during differentiation of epididymal preadipocytes, with a 10 fold higher expression of the long isoform. PRL upregulated both isoforms before and after differentiation. PRL suppressed lipolysis in epididymal explants and mature adipocytes in a dose-and time-dependent manner, which was reversed by a Jak2 inhibitor. PRL also inhibited leptin, but not adiponectin, release. We conclude that PRL inhibits lipolysis and leptin release by acting directly on adipocytes via interaction with either of its receptors and activation of a Jak2-dependent signaling pathway(s). This is the first demonstration of substantial effects of PRL on male adipocytes.

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Section: Discussionmentioning

confidence: 99%

Prolactin upregulates its receptors and inhibits lipolysis and leptin release in male rat adipose tissue

Brandebourg

Bown

Ben‐Jonathan

2007

Biochemical and Biophysical Research Communications

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“…39 On the other hand, other investigators found hypoadiponectinemia during the 3 rd and 4 th day postpartum in normal lactating women. 40,18 It has been suggested that this hypoadiponectinemia might be due to the suppression of adipocyte-produced adiponectin by prolactin. 40,41 Otherwise, the significant decrease of the studied cytokines during the early postpartum period in pregnancies with GDM in this study could be explained by the withdrawal of cytokines produced by the placenta during pregnancy.…”

Section: Discussionmentioning

confidence: 99%

“…40,18 It has been suggested that this hypoadiponectinemia might be due to the suppression of adipocyte-produced adiponectin by prolactin. 40,41 Otherwise, the significant decrease of the studied cytokines during the early postpartum period in pregnancies with GDM in this study could be explained by the withdrawal of cytokines produced by the placenta during pregnancy. 8,9,27 The role of the placenta in the production of adiponectin and IL-1β during pregnancy is further reinforced by the non-significant but clear downward trend of these cytokines during third day postpartum found in pregnancies without GDM.…”

Section: Discussionmentioning

confidence: 99%

Pre- and early post-partum adiponectin and Interleukin-1beta levels in women with and without gestational diabetes

Vitoratos¹,

Valsamakis²,

Mastorakos³

et al. 2008

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OBJECTIVE: To investigate maternal serum adiponectin and Ιnterleukin-1beta (IL-1β) levels during the pre-and post-partum periods in pregnant women with and without Gestational Diabetes Mellitus (GDM). DESIGN: Thirty control pregnant Caucasian women without GDM and thirty Body Mass Index (BMI) and age-matched Caucasian women with GDM examined in the outpatient clinic between the 24 th and 26 th week of their pregnancy and on the 3 rd day postpartum underwent anthropometry and had serum blood taken. Both groups, were monitored by a dietitian and had comparable weight gain during pregnancy. Birth weight was also measured. RESULTS: At the 3 rd day postpartum, compared to the 2 nd trimester of pregnancy, women with GDM had lower serum adiponectin levels, lower serum IL-1β levels and lower Homeostasis Model Assessment for Insulin Resistance (HOMA-IR) values. At the 2 nd trimester of pregnancy, women with GDM had lower serum adiponectin levels, higher IL-1β and higher HOMA-IR values compared to women without GDM. At the 3 rd day postpartum, women with GDM had lower serum adiponectin levels, higher IL-1β and higher HOMA-IR values compared to women without GDM. Second trimester serum adiponectin values of women with GDM correlated negatively with birth weight. CONCLUSIONS: Gestational diabetes is a state of insulin resistance associated with altered levels of proinflammatory cytokines, increased IL-1β and decreased adiponectin values. Both of these alterations might be attributed to placental pathology in pregnancies with GDM.

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“…One study conducted in lean pregnant women demonstrated that PRL could cause insulin resistance in adipocytes by suppressing adiponectin production and secretion (38). This mechanism is plau- sible, because low levels of adiponectin can be associated with obesity and insulin resistance.…”

Section: Discussionmentioning

confidence: 99%

The STAT5A-Mediated Induction of Pyruvate Dehydrogenase Kinase 4 Expression by Prolactin or Growth Hormone in Adipocytes

et al. 2007

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The purpose of this study was to determine whether pyruvate dehydrogenase kinase (PDK)4 was expressed in adipocytes and whether PDK4 expression was hormonally regulated in fat cells. Both Northern blot and Western blot analyses were conducted on samples isolated from 3T3-L1 adipocytes after various treatments with prolactin (PRL), growth hormone (GH), and/or insulin. Transfection of PDK4 promoter reporter constructs was performed. In addition, glucose uptake measurements were conducted. Our studies demonstrate that PRL and porcine GH can induce the expression of PDK4 in 3T3-L1 adipocytes. Our studies also show that insulin pretreatment can attenuate the ability of these hormones to induce PDK4 mRNA expression. In addition, we identified a hormone-responsive region in the murine PDK4 promoter and characterized a STAT5 binding site in this region that mediates the PRL (sheep) and GH (porcine) induction in PDK4 expression in 3T3-L1 adipocytes. PDK4 is a STAT5A target gene. PRL is a potent inducer of PDK4 protein levels, results in an inhibition of insulin-stimulated glucose transport in fat cells, and likely contributes to PRL-induced insulin resistance. Diabetes 56:1623-1629, 2007 I t is well known that growth hormone (GH) and prolactin (PRL) induce signaling via the JAK-STAT pathway. In particular, STAT5 proteins are potently activated by these hormones (rev. in 1). GH is known to have profound effects on lipid metabolism (rev. in 2). The effects of PRL have been well characterized in mammary tissues, yet there is also evidence demonstrating that this hormone can affect adipose tissue in mice and humans (3,4). Yet, few molecular targets for the STAT5-mediated actions of GH and PRL on adipocytes have been identified. Although multiple lines of recent evidence suggest that STAT5 proteins can modulate adipocyte function (5-11), very few studies have identified direct STAT5 target genes in adipocytes. We recently observed that the GH and PRL inhibition of fatty acid synthase (FAS) transcription was mediated by a STAT5A binding site in the rat FAS promoter (12). Hence, our current efforts have been to identify other genes associated with glucose or lipid metabolism that are directly modulated by STAT5 proteins in adipocytes. In this study, we present data demonstrating that pyruvate dehydrogenase kinase (PDK)4 is a STAT5A target gene.PDK is a family of kinases that negatively regulate the activity of the pyruvate dehydrogenase complex (PDC) (rev. in 13). There are four tissue-specific isoforms of PDK, PDK1-4, that have been identified in mammals, and each has different patterns of gene expression (14 -16). The specificity in distribution, expression, and activity of each PDK isoform contributes to the long-term regulation of PDC in a given tissue and thus, in part, regulates glucose metabolism. There are several conditions that result in the short-term regulation of PDC activity (17-19). The longterm regulation of PDK that occurs in starvation (18,20) and diabetes involves an increase in the amount of PDK protein, whi...

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Hypoadiponectinemia in Lean Lactating Women: Prolactin Inhibits Adiponectin Secretion from Human Adipocytes

Cited by 67 publications

References 34 publications

Prolactin upregulates its receptors and inhibits lipolysis and leptin release in male rat adipose tissue

Prolactin upregulates its receptors and inhibits lipolysis and leptin release in male rat adipose tissue

Pre- and early post-partum adiponectin and Interleukin-1beta levels in women with and without gestational diabetes

The STAT5A-Mediated Induction of Pyruvate Dehydrogenase Kinase 4 Expression by Prolactin or Growth Hormone in Adipocytes

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