The Clearance and Metabolism of Estradiol and Estradiol-17-Esters in the Rat*

Larner, Janice M.; Hochberg, Richard B.

doi:10.1210/endo-117-3-1209

Cited by 54 publications

(17 citation statements)

References 12 publications

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“…4) and led to normal spontaneous meal patterns, food intake, and body weight (15). Note that because of the rapid rates of esterification of estradiol benzoate in the plasma and clearance of estradiol from the plasma in rats (417,724), the durations of the estradiol increases in these studies are due mainly to the slow entry of subcutaneously injected estradiol into the circulation. Doses more than 20 g estradiol consistently elicit signs of aversion in female rats, such as abnormal latency and duration of the eating-inhibitory effect, abnormal orofacial expressions, and the formation of conditioned taste aversions (253,254,333).…”

Section: Physiological Sex Differences In Disordered Eating)mentioning

confidence: 84%

Sex differences in the physiology of eating

Asarian

Geary²

2013

American Journal of Physiology-Regulatory, Integrative and Comp

414

349

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(HPG) axis function fundamentally affects the physiology of eating. We review sex differences in the physiological and pathophysiological controls of amounts eaten in rats, mice, monkeys, and humans. These controls result from interactions among genetic effects, organizational effects of reproductive hormones (i.e., permanent early developmental effects), and activational effects of these hormones (i.e., effects dependent on hormone levels). Male-female sex differences in the physiology of eating involve both organizational and activational effects of androgens and estrogens. An activational effect of estrogens decreases eating 1) during the periovulatory period of the ovarian cycle in rats, mice, monkeys, and women and 2) tonically between puberty and reproductive senescence or ovariectomy in rats and monkeys, sometimes in mice, and possibly in women. Estrogens acting on estrogen receptor-␣ (ER␣) in the caudal medial nucleus of the solitary tract appear to mediate these effects in rats. Androgens, prolactin, and other reproductive hormones also affect eating in rats. Sex differences in eating are mediated by alterations in orosensory capacity and hedonics, gastric mechanoreception, ghrelin, CCK, glucagon-like peptide-1 (GLP-1), glucagon, insulin, amylin, apolipoprotein A-IV, fatty-acid oxidation, and leptin. The control of eating by central neurochemical signaling via serotonin, MSH, neuropeptide Y, Agouti-related peptide (AgRP), melanin-concentrating hormone, and dopamine is modulated by HPG function. Finally, sex differences in the physiology of eating may contribute to human obesity, anorexia nervosa, and binge eating. The variety and physiological importance of what has been learned so far warrant intensifying basic, translational, and clinical research on sex differences in eating.neuroendocrinology; estrogens; testosterone; eating disorders; obesity SEX DIFFERENCES ARE PERVASIVE in physiology and medicine (51,64,73,109,110,466,797,826). The controls of eating and energy homeostasis are no exceptions. It was observed approximately 100 years ago that removal of the ovaries leads to marked accretion of adipose tissue in rats (697), that daily food intake expressed as kilocalories per gram body weight differs between male and female rats (778), and that food intake varies regularly through the ovarian cycle in intact female rats (674, 779). Sex differences in eating have been the subject of physiological research ever since. The clinical relevance of this work is increasingly evident. In the United States, women are approximately threefold more vulnerable than men to psychiatric eating disorders (346,351) and approximately twofold more vulnerable to severe and morbid obesity (BMI Ն 35 and 40 kg/m 2 , respectively, mass/height 2 ) (226). Women also appear to suffer more from these disorders in terms of physical and psychological functioning and quality of life (24,84,273,292,465,531,762). The increased obesity burden suffered by women is reflected in the fact that Ͼ80% of bariatric surgery patients in the U...

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Section: Physiological Sex Differences In Disordered Eating)mentioning

confidence: 84%

Sex differences in the physiology of eating

Asarian

Geary²

2013

American Journal of Physiology-Regulatory, Integrative and Comp

414

349

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“…However, DHEA-FAE associated with lipoproteins had a surprisingly short half-life in plasma (ϳ40 min) when injected into guinea pigs (6). This is in contrast to E 2 -FAE that exhibited a much longer half-time (6 h) in the rat (27). Further studies on the metabolic fate of lipoprotein-associated DHEA-FAE are needed to understand the physiological role of these differences.…”

Section: Discussionmentioning

confidence: 96%

Role of lysosomal acid lipase in the intracellular metabolism of LDL-transported dehydroepiandrosterone-fatty acyl esters

Wang

Wang²,

Wähälä³

et al. 2008

American Journal of Physiology-Endocrinology and Metabolism

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H]DHEA-FAE entered cells via LDL receptor or LDL receptorrelated receptor-mediated uptake, followed by intracellular hydrolysis and further metabolism into 5␣-adione and 4-adione that were excreted from cells. Although LAL contributed to the deesterification of DHEA-FAE, it was not solely responsible for the hydrolysis. ribonucleic acid interference; chromatography; dehydroepiandrosterone STEROID FATTY ACYL ESTERS (FAE) such as 17␤-estradiol-FAE (E 2 -FAE) and dehydroepiandrosterone-FAE (DHEA-FAE) belong to a unique family of naturally occurring hydrophobic hormone derivatives (15, 16). These steroids are esterified in a reaction catalyzed by plasma lecithin-cholesterol acyltransferase associated with high-density lipoprotein (HDL) particles and transported to other lipoprotein particles (14,18,30,35,42). The physiological role of steroid-FAE remains unclear. E 2 -FAE have been considered as the storage form of active estrogen in lipoproteins and adipose tissues that may be released as an active unconjugated hormone (3). It has also been suggested that E 2 -FAE may act as an antioxidant, protecting lipoproteins against oxidation (17, 41). Our previous studies (4) in a cell culture model demonstrated that lipoprotein-associated E 2 -FAE can be transferred into target cells and hydrolyzed to free E 2 .Compared with E 2 -FAE that is present in picomolar concentration in the circulation, nanomolar concentrations of circulating DHEA-FAE have been reported (7,26). Moreover, its hydrolysis product, DHEA, is one of the relatively abundant adrenal steroids secreted in humans and the precursor of estrogens and androgens (24). In blood, Ͼ90% of DHEA-FAE is associated with lipoproteins (38, 39). We are interested in the intracellular hydrolysis and metabolic fate of lipoproteinbound DHEA-FAE in target tissues.In postmenopausal women, only trace amounts of E 2 are present in serum, the overwhelming majority of estradiol residing in adipose tissue, mostly in the form of FAE (3). This finding opens up the possibility that adipose tissue could constitute a reservoir of many other steroid-FAEs from which active steroid hormones could, in principle, be liberated by hydrolysis of the FAE bond. Therefore, we aimed at exploring possible hydrolytic mechanisms involved in generating free DHEA and identifying potential bioactive metabolites of DHEA generated in cells. Lysosomal acid lipase (LAL) is the enzyme responsible for the intracellular hydrolysis of LDLassociated cholesteryl esters (cholesteryl-FAE) that are taken up by LDL-receptor-mediated endocytosis (12). Because of the similar ring structure of DHEA and cholesterol, we investigated the possibility that DHEA-FAE is also hydrolyzed by LAL. We chose HeLa cells as a model to study the hydrolysis and metabolism of LDL-associated DHEA-FAE because these cells, derived from the reproductive tract, have previously been useful in the study cholesterol metabolism (19,22,37). Moreover, HeLa cells express LAL mRNA (1) and RNA silencing works very reproducibly in these cells. Thus we inv...

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“…Actually, Hpt was found to inhibit ApoA-I-dependent LCAT activity in vitro (23) and to associate with low reverse cholesterol transport in human ovarian follicular fluid (24). In addition, estradiol esterification in the follicle and ester delivery through HDL-mediated circulation to storage tissue (25,26) for long acting hormonal and antioxidant function (27,28) might be influenced by defective reverse cholesterol transport and reduced LCAT activity (24).…”

mentioning

confidence: 99%

Assignment of the Binding Site for Haptoglobin on Apolipoprotein A-I

Spagnuolo

Cigliano

D’Andrea

et al. 2005

Journal of Biological Chemistry

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Haptoglobin (Hpt) was previously found to bind the high density lipoprotein (HDL) apolipoprotein A-I (ApoA-I) and able to inhibit the ApoA-I-dependent activity of the enzyme lecithin:cholesterol acyltransferase (LCAT), which plays a major role in the reverse cholesterol transport. The ApoA-I structure was analyzed to detect the site bound by Hpt. ApoA-I was treated by cyanogen bromide or hydroxylamine; the resulting frag

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The Clearance and Metabolism of Estradiol and Estradiol-17-Esters in the Rat*

Cited by 54 publications

References 12 publications

Sex differences in the physiology of eating

Sex differences in the physiology of eating

Role of lysosomal acid lipase in the intracellular metabolism of LDL-transported dehydroepiandrosterone-fatty acyl esters

Assignment of the Binding Site for Haptoglobin on Apolipoprotein A-I

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