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Mohiti-Ardekani J, Tarof N, Aflatonian A. Relationships between free leptin and insulin resistance in women with polycystic ovary syndrome. IJRM 2009; 7 (2) :53-58
URL: http://ijrm.ir/article-1-140-en.html
URL: http://ijrm.ir/article-1-140-en.html
1- Department of Biochemistry and Molecular Biology, Shahid Sadoughi University of Medical Sciences, Yazd, Iran , mohiti_99@yahoo.com
2- Department of Biochemistry and Molecular Biology, Shahid Sadoughi University of Medical Sciences, Yazd, Iran
3- Research and Clinical Center for Infertility, Shahid Sadoughi University of Medical Sciences, Yazd, Iran
2- Department of Biochemistry and Molecular Biology, Shahid Sadoughi University of Medical Sciences, Yazd, Iran
3- Research and Clinical Center for Infertility, Shahid Sadoughi University of Medical Sciences, Yazd, Iran
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Introduction
Leptin, the gene product of the ob gene, is thought to provide the central nervous system with feed-back information about fat storage of the body (1). Thus, leptin is thought to be a part of the regulation of appetite, food intake and the lipid metabolism (2).
Obese humans present with hyperleptinemia as an indicator of leptin resistance which plays a major role in the pathogenesis of obesity (3). Polycystic ovary syndrome (PCOS) is among the most common endocrine disorders, affecting more than 5% of women of reproductive age (4, 5). An association of PCOS with peripheral insulin resistance, compensatory hyperinsulinemia and alterations in ß-cell function as the cause of its predisposition to develop a metabolic syndrome (type 2 diabetes mellitus, hypertension, lipid disorders, obesity) has been established (6). According to the majority of studies, most PCOS women are insulin resistant and overweight or obese (7-11). In mice, a genetic defect in the ob gene results in severe obesity and type 2 diabetes mellitus, as well as in infertility (6).
In this mouse model, leptin injections restore fertility. Leptin treatment in normal female mice accelerates puberty (12). In humans, granulosa cells have been shown to secrete leptin (13) and leptin seems to influence adrenal androgen formation (14).
However, the role of leptin in ovarian function or on the reproductive system remains unclear. It was shown that leptin levels did not influence follicular maturation and ovulation in PCOS patients (10) while Carmina et al demonstrated a negative correlation between leptin and dehydroepiandrosterone sulphate (DHEAS) levels in 21 lean PCOS women, suggesting that androgens may play a role in suppressing serum leptin (15).
Another study showed that leptin concentrations correlated inversely with luteinizing hormone (LH) levels, independent of body weight and insulin resistance (16). In contrast again, Laughlin et al (17) proposed that leptin is neither involved in the hypersecretion of LH nor in the regulation of LH pulsatility. During lactational amenorrhea Sir-Petermann et al (18) also showed that leptin secretion is not related to LH secretion. Plasma leptin is in free and bound forms in circulation (19).
The free leptin has been shown to correlate with total serum leptin levels and BMI in women of reproductive age. Kado et al (20) hypothesized that obese women are able to conversely increase their leptin activity by minimizing the bound leptin fraction, thus influencing the biological activity of leptin. In line with this, Sinha et al (21) reported that in lean subjects, leptin circulates predominantly in the bound form, whereas in obese patients, leptin circulates mostly in the free form. Similar results were found for Japanese men and women, showing a direct correlation between free leptin level and BMI and parameters of insulin resistance (22).
Weight loss, following gastric restrictive surgery, leads to a reduction in circulating leptin levels and to a decrease free leptin (23). In adolescent girls with anorexia nervosa, free leptin and Free Leptin Index (FLI) but not total leptin levels were closely related to parameters of sexual maturation and the onset of puberty (26). Therefore, to elucidate the free leptin role in PCOS, we purified the free leptin in PCOS patients and healthy control and analyzed the interrelations between serum total leptin and free forms with insulin and insulin resistance and the other metabolic factors.
Materials and methods
Study population
The study was carried out on 54 women (27 PCOS subjects and 27 voluntary BMI, and age matched healthy women with normal menstrual cycle as controls). Clinical diagnosis of PCOS was made from the 1990 National Institutes of Health (NIH) conference, when either oligomenorrhea (cycles lasting longer than 35 days) or amenorrhea (less than two menstrual cycles in the past 6 months) and either clinical signs of hyperandrogenism (hirsutism or obvious acne or alopecia and/or an elevated total testosterone) were found, and other pituitary, adrenal or ovarian diseases could be excluded. PCOS as well as control subjects had not taken any medication known to affect carbohydrate metabolism or endocrine parameters for at least 3 months before entering the study. In controls, LH, FSH and insulin levels were estimated in the early follicular phase (second or third day of menstruation) from fasting blood samples.
Data collection
In PCOS subjects and control women, clinical parameters were assessed by physical examination, and BMI was calculated as (weight/height2) (kg/m2).
Insulin resistance was calculated by homeostasis assessment model (HOMA) using the formula HOMA-IR = Fasting insulin (μU/ml) × Fasting glucose (mg/dl)/22.5 (27). Low-IR values indicate high insulin sensitivity, whereas high-HOMA values indicate low insulin sensitivity (insulin resistance).
Biochemical assays
Leptin were measured using ELISA kits [Diagnostic Systems Laboratories (DSL), Webster, TX, USA]. The DSL ACTIVE Human Leptin ELISA is an enzymatically amplified ‘two-step’ sandwich-type immunoassay. The theoretical sensitivity or minimum detection limit as calculated by interpolation of the mean plus two standard deviations of 12 replicants of the zero standard was 0.05 ng/ml. Intra-assay variation was <5% and interassay variation was <8% for all measured parameters. Insulin concentrations were measured by sandwich ELISA (Webster, Texas 77598-4217 USA, DSL).
Free leptin form was purified by Gel filtration methods as bellow (20). This study was approved by the local ethical committee and each patient gave written informed consent.
Purification of free leptin form in serum
To obtain a standard curve, one vial containing 1 mg lyophilized leptin (Sigma) was dissolved in 0.5 ml HCL (1.5mM) and neutralized with 0.25 ml NaOH (7.5 mM) and applied with Marker Gel filtration Bludextran (Product Brand: Sigma Product Number: D4772) to Sephadex G-100 column chromatography (Amersham Biosource (1908-7101) (9/30 column).
The leptin was eluted with 0.25 mM phosphate buffer (Ph=7.4). Fractions eluting were collected and assayed by a Sensitive ELISA Kit (Catalogue Number: kap 2281: 96 determinations. Manufactured by: Biosource Europe S-A). It showed a single bound indicating free leptin fraction.
Serum sample (0.5ml) was fractionated by Sephadex G-100 gel filtration chromatogheraphy. Fractions eluting between void and bed volumes were assayed by the ELISA kit.
Statistical analysis
Data are presented as median plus range for non-parametric data. For better comparison, means ±S.D. is also shown. Correlations between
variables were examined by Spearman’s correlation coefficient (rs) because analyzed data were not normally distributed. Differences between the groups were evaluated with the Mann–Whitney U test. p values <0.05 were considered significant.
Results
Patients with PCOS showed significantly higher concentrations of leptin (mean 21±9 ng/ml) vs. control (16±10 ng/ml, p=0.042), free leptin (mean 7.3±1.2) vs. control (mean 4.3±1.3 ng/ml, p=0.011) and LH (mean 76±18 IU/ml) vs. control (mean 2.87±1.93, p=0.001) in plasma (Table I).
We observed no marked difference in insulin level between patients with PCOS (mean 26±13µIU/ml) vs. control (mean 25±13) and FSH level between patients with PCOS (8.69±15 IU/ml) vs. control (mean 6.56±1.46) (Table I). Furthermore, we analyzed the relationships between leptin, free leptin with BMI, insulin, insulin resistance and LH in PCOS and control groups.
Significant correlations were observed between free leptin and BMI (rs=0.78, p=0.000), insulin resistance (IR) (r=0.53, p=0.004) and insulin (r=0.93, p=0.000) in PCOS patients. Significant correlations were also observed between free leptin and BMI (r=0.86, p=0.00), IR (r=0.57, p=0.003) and insulin (r=0.91, p=0.000) in control group (Table `II). No significant correlation was observed between total and free leptin with LH.
Table I. Characteristic of control (n=27) and PCOS patients (n=27). Values are means ±SD (median and range).
_87-63/Table_1.jpg)
Table II. Correlation of leptin and free leptin levels with metabolic parameters in PCOS and control women.
_87-63/Table_2.jpg)
Discussion
Leptin levels are increased in obesity and may play a role in the development of insulin resistance (7). Our study showed a significant high total and free leptin in PCOS patients as it is compared with controls (Table I) (p<0.05). Total leptin levels correlated significantly with BMI in both PCOS women and controls. Leptin correlated with other metabolic parameters including insulin resistance and insulin level in both groups. Similar results were found in PCOS patients from Australia (29), Brazil (16), Canada (10), Finland (30), Italy (15), Sweden (8), Turkey (11) and USA (17, 31). Significant correlation of total leptin with HOMA IR reflected a degree of insulin resistance in both controls and test groups (Table II). We can place our results along the large group of studies, which declare an important role of leptin in pathogenesis of insulin resistance (1, 2, 4, 6, 8, 11, 15, 20, 28, 29).
In addition, we found free leptin levels in PCOS patient and control group correlate with parameters of insulin, and insulin resistance (Table II).
Thus free leptin appears to be the appropriate form of leptin which it contributes to insulin resistance and leptin resistance. Potential mechanisms that may mediate leptin resistance include impairment of brain leptin transport or leptin receptor internalization, and receptor post-receptor signaling defects. Furthermore, the active hormone may be reduced by binding proteins or soluble receptors (32). Soluble leptin receptor represents the main leptin-binding compound in plasma, thus regulating its free fraction in the circulation (33).
A considerable portion of circulating leptin is free form which is affected by the degree of adiposity and nutritional state (35-37). We found a positive correlation between free leptin with BMI in PCOS patients and controls. Yannakoulia and co-workers (24) demonstrated that Free leptin index is correlated with total energy intake and inversely correlated with energy intake from dietary fat. They speculated that the macronutrient composition of the diet influences serum concentrations of free leptin. The authors hypothesized that the increase of free leptin levels represents a compensatory mechanism to overcome leptin resistance.
A recently published twin study of pubertal females studying the genetic and environmental influences on the variations of leptin and free form levels showed that leptin is mostly influenced by body composition (25, 34). We have demonstrated the correlation of free leptin with insulin resistance in diabetes patients (38). In conclusion, a considerable part of plasma leptin is in free form in circulation.
Although the physiological function of bound and free leptin are not well understood, it has been hypothesized that leptin is more active in its free form because this form is present in cerebrospinal fluid (CSF) (34). We found a relationship between total leptin levels, and free leptin with BMI, insulin resistance, and insulin levels in overweight PCOS patients and their matched control group.
However, further studies are needed to investigate the effect of factors including food or body composition, and genetic on high level of free leptin in PCOS patients.
Acknowledgement
We thank Members of the Dept. of Biochemistry and Molecular Biology for helpful discussins. This research was supported by Shahid Sadoughi University of Medical Science and Research and Clinical Center for Infertility, Shahid Sadoughi University of Medical Sciences, Yazd, Iran.
Leptin, the gene product of the ob gene, is thought to provide the central nervous system with feed-back information about fat storage of the body (1). Thus, leptin is thought to be a part of the regulation of appetite, food intake and the lipid metabolism (2).
Obese humans present with hyperleptinemia as an indicator of leptin resistance which plays a major role in the pathogenesis of obesity (3). Polycystic ovary syndrome (PCOS) is among the most common endocrine disorders, affecting more than 5% of women of reproductive age (4, 5). An association of PCOS with peripheral insulin resistance, compensatory hyperinsulinemia and alterations in ß-cell function as the cause of its predisposition to develop a metabolic syndrome (type 2 diabetes mellitus, hypertension, lipid disorders, obesity) has been established (6). According to the majority of studies, most PCOS women are insulin resistant and overweight or obese (7-11). In mice, a genetic defect in the ob gene results in severe obesity and type 2 diabetes mellitus, as well as in infertility (6).
In this mouse model, leptin injections restore fertility. Leptin treatment in normal female mice accelerates puberty (12). In humans, granulosa cells have been shown to secrete leptin (13) and leptin seems to influence adrenal androgen formation (14).
However, the role of leptin in ovarian function or on the reproductive system remains unclear. It was shown that leptin levels did not influence follicular maturation and ovulation in PCOS patients (10) while Carmina et al demonstrated a negative correlation between leptin and dehydroepiandrosterone sulphate (DHEAS) levels in 21 lean PCOS women, suggesting that androgens may play a role in suppressing serum leptin (15).
Another study showed that leptin concentrations correlated inversely with luteinizing hormone (LH) levels, independent of body weight and insulin resistance (16). In contrast again, Laughlin et al (17) proposed that leptin is neither involved in the hypersecretion of LH nor in the regulation of LH pulsatility. During lactational amenorrhea Sir-Petermann et al (18) also showed that leptin secretion is not related to LH secretion. Plasma leptin is in free and bound forms in circulation (19).
The free leptin has been shown to correlate with total serum leptin levels and BMI in women of reproductive age. Kado et al (20) hypothesized that obese women are able to conversely increase their leptin activity by minimizing the bound leptin fraction, thus influencing the biological activity of leptin. In line with this, Sinha et al (21) reported that in lean subjects, leptin circulates predominantly in the bound form, whereas in obese patients, leptin circulates mostly in the free form. Similar results were found for Japanese men and women, showing a direct correlation between free leptin level and BMI and parameters of insulin resistance (22).
Weight loss, following gastric restrictive surgery, leads to a reduction in circulating leptin levels and to a decrease free leptin (23). In adolescent girls with anorexia nervosa, free leptin and Free Leptin Index (FLI) but not total leptin levels were closely related to parameters of sexual maturation and the onset of puberty (26). Therefore, to elucidate the free leptin role in PCOS, we purified the free leptin in PCOS patients and healthy control and analyzed the interrelations between serum total leptin and free forms with insulin and insulin resistance and the other metabolic factors.
Materials and methods
Study population
The study was carried out on 54 women (27 PCOS subjects and 27 voluntary BMI, and age matched healthy women with normal menstrual cycle as controls). Clinical diagnosis of PCOS was made from the 1990 National Institutes of Health (NIH) conference, when either oligomenorrhea (cycles lasting longer than 35 days) or amenorrhea (less than two menstrual cycles in the past 6 months) and either clinical signs of hyperandrogenism (hirsutism or obvious acne or alopecia and/or an elevated total testosterone) were found, and other pituitary, adrenal or ovarian diseases could be excluded. PCOS as well as control subjects had not taken any medication known to affect carbohydrate metabolism or endocrine parameters for at least 3 months before entering the study. In controls, LH, FSH and insulin levels were estimated in the early follicular phase (second or third day of menstruation) from fasting blood samples.
Data collection
In PCOS subjects and control women, clinical parameters were assessed by physical examination, and BMI was calculated as (weight/height2) (kg/m2).
Insulin resistance was calculated by homeostasis assessment model (HOMA) using the formula HOMA-IR = Fasting insulin (μU/ml) × Fasting glucose (mg/dl)/22.5 (27). Low-IR values indicate high insulin sensitivity, whereas high-HOMA values indicate low insulin sensitivity (insulin resistance).
Biochemical assays
Leptin were measured using ELISA kits [Diagnostic Systems Laboratories (DSL), Webster, TX, USA]. The DSL ACTIVE Human Leptin ELISA is an enzymatically amplified ‘two-step’ sandwich-type immunoassay. The theoretical sensitivity or minimum detection limit as calculated by interpolation of the mean plus two standard deviations of 12 replicants of the zero standard was 0.05 ng/ml. Intra-assay variation was <5% and interassay variation was <8% for all measured parameters. Insulin concentrations were measured by sandwich ELISA (Webster, Texas 77598-4217 USA, DSL).
Free leptin form was purified by Gel filtration methods as bellow (20). This study was approved by the local ethical committee and each patient gave written informed consent.
Purification of free leptin form in serum
To obtain a standard curve, one vial containing 1 mg lyophilized leptin (Sigma) was dissolved in 0.5 ml HCL (1.5mM) and neutralized with 0.25 ml NaOH (7.5 mM) and applied with Marker Gel filtration Bludextran (Product Brand: Sigma Product Number: D4772) to Sephadex G-100 column chromatography (Amersham Biosource (1908-7101) (9/30 column).
The leptin was eluted with 0.25 mM phosphate buffer (Ph=7.4). Fractions eluting were collected and assayed by a Sensitive ELISA Kit (Catalogue Number: kap 2281: 96 determinations. Manufactured by: Biosource Europe S-A). It showed a single bound indicating free leptin fraction.
Serum sample (0.5ml) was fractionated by Sephadex G-100 gel filtration chromatogheraphy. Fractions eluting between void and bed volumes were assayed by the ELISA kit.
Statistical analysis
Data are presented as median plus range for non-parametric data. For better comparison, means ±S.D. is also shown. Correlations between
variables were examined by Spearman’s correlation coefficient (rs) because analyzed data were not normally distributed. Differences between the groups were evaluated with the Mann–Whitney U test. p values <0.05 were considered significant.
Results
Patients with PCOS showed significantly higher concentrations of leptin (mean 21±9 ng/ml) vs. control (16±10 ng/ml, p=0.042), free leptin (mean 7.3±1.2) vs. control (mean 4.3±1.3 ng/ml, p=0.011) and LH (mean 76±18 IU/ml) vs. control (mean 2.87±1.93, p=0.001) in plasma (Table I).
We observed no marked difference in insulin level between patients with PCOS (mean 26±13µIU/ml) vs. control (mean 25±13) and FSH level between patients with PCOS (8.69±15 IU/ml) vs. control (mean 6.56±1.46) (Table I). Furthermore, we analyzed the relationships between leptin, free leptin with BMI, insulin, insulin resistance and LH in PCOS and control groups.
Significant correlations were observed between free leptin and BMI (rs=0.78, p=0.000), insulin resistance (IR) (r=0.53, p=0.004) and insulin (r=0.93, p=0.000) in PCOS patients. Significant correlations were also observed between free leptin and BMI (r=0.86, p=0.00), IR (r=0.57, p=0.003) and insulin (r=0.91, p=0.000) in control group (Table `II). No significant correlation was observed between total and free leptin with LH.
Table I. Characteristic of control (n=27) and PCOS patients (n=27). Values are means ±SD (median and range).
Table II. Correlation of leptin and free leptin levels with metabolic parameters in PCOS and control women.
Discussion
Leptin levels are increased in obesity and may play a role in the development of insulin resistance (7). Our study showed a significant high total and free leptin in PCOS patients as it is compared with controls (Table I) (p<0.05). Total leptin levels correlated significantly with BMI in both PCOS women and controls. Leptin correlated with other metabolic parameters including insulin resistance and insulin level in both groups. Similar results were found in PCOS patients from Australia (29), Brazil (16), Canada (10), Finland (30), Italy (15), Sweden (8), Turkey (11) and USA (17, 31). Significant correlation of total leptin with HOMA IR reflected a degree of insulin resistance in both controls and test groups (Table II). We can place our results along the large group of studies, which declare an important role of leptin in pathogenesis of insulin resistance (1, 2, 4, 6, 8, 11, 15, 20, 28, 29).
In addition, we found free leptin levels in PCOS patient and control group correlate with parameters of insulin, and insulin resistance (Table II).
Thus free leptin appears to be the appropriate form of leptin which it contributes to insulin resistance and leptin resistance. Potential mechanisms that may mediate leptin resistance include impairment of brain leptin transport or leptin receptor internalization, and receptor post-receptor signaling defects. Furthermore, the active hormone may be reduced by binding proteins or soluble receptors (32). Soluble leptin receptor represents the main leptin-binding compound in plasma, thus regulating its free fraction in the circulation (33).
A considerable portion of circulating leptin is free form which is affected by the degree of adiposity and nutritional state (35-37). We found a positive correlation between free leptin with BMI in PCOS patients and controls. Yannakoulia and co-workers (24) demonstrated that Free leptin index is correlated with total energy intake and inversely correlated with energy intake from dietary fat. They speculated that the macronutrient composition of the diet influences serum concentrations of free leptin. The authors hypothesized that the increase of free leptin levels represents a compensatory mechanism to overcome leptin resistance.
A recently published twin study of pubertal females studying the genetic and environmental influences on the variations of leptin and free form levels showed that leptin is mostly influenced by body composition (25, 34). We have demonstrated the correlation of free leptin with insulin resistance in diabetes patients (38). In conclusion, a considerable part of plasma leptin is in free form in circulation.
Although the physiological function of bound and free leptin are not well understood, it has been hypothesized that leptin is more active in its free form because this form is present in cerebrospinal fluid (CSF) (34). We found a relationship between total leptin levels, and free leptin with BMI, insulin resistance, and insulin levels in overweight PCOS patients and their matched control group.
However, further studies are needed to investigate the effect of factors including food or body composition, and genetic on high level of free leptin in PCOS patients.
Acknowledgement
We thank Members of the Dept. of Biochemistry and Molecular Biology for helpful discussins. This research was supported by Shahid Sadoughi University of Medical Science and Research and Clinical Center for Infertility, Shahid Sadoughi University of Medical Sciences, Yazd, Iran.
Type of Study: Original Article |
References
1. Hang Y, Proenca R, Maffei M, Barone M, Leopold L, Friedman JM. Positional cloning of the mouse obese gene and its human homologue. Nature 1994; 372: 425-432. [DOI:10.1038/372425a0]
2. Janeckova R. The role of leptin in human physiology and pathophysiology. Physiological Research 2001; 50: 443-459.
3. Considine RV, Sinha MK, Heiman ML, Kriauciunas A, Stephens TW, Nyce MR, et al. Serum immunoreactive leptin concentrations in normal-weight and obese humans. New England Journal of Medicine 1996; 334: 292-295. [DOI:10.1056/NEJM199602013340503]
4. Asuncion M, Calvo RM, San Millan JL, Sancho J, Avila S, Escobar-Morreale HF. A prospective study of the prevalence of the polycystic ovary syndrome in unselected Caucasian women from Spain. Journal of Clinical Endocrinology and Metabolism 2000; 85: 2434-2438. [DOI:10.1210/jc.85.7.2434]
5. Azziz R, Woods KS, Reyna R, Key TJ, Knochenhauer ES, Yildiz BO. The prevalence and features of the polycystic ovary syndrome in an unselected population. Journal of Clinical Endocrinology and Metabolism 2004: 89: 2745-2749. [DOI:10.1210/jc.2003-032046]
6. Dunaif A, Segal KR, Futterweit W, Dobrjansky A. Profound peripheral insulin resistance, independent of obesity, in polycystic ovary syndrome. Diabetes 1989; 38: 1165-1174. [DOI:10.2337/diab.38.9.1165]
7. Loverro G, Lorusso F, Mei L, Depalo R, Cormio G, Selvaggi L. The plasma homocysteine levels are increased in polycystic ovary syndrome. Gynecologic and Obstetric Investigation 2002; 53: 157-162. [DOI:10.1159/000058367]
8. Gennarelli G, Holte J, Wide L, Berne C, Lithell H. Is there a role for leptin in the endocrine and metabolic aberrations of polycystic ovary syndrome? Human Reproduction 1998; 13: 535-541. [DOI:10.1093/humrep/13.3.535]
9. Maliqueo M, Perez-Bravo F, Calvillan M, Piwonka V, Castillo T, Sir-Petermann T. Relationship between leptin and insulin sensitivity in patients with polycystic ovary syndrome. Medicina Clinica 1999; 113: 526-530.
10. Pirwany IR, Fleming R, Sattar N, Greer IA, Wallace AM. Circulating leptin concentrations and ovarian function in polycystic ovary syndrome. European Journal of Endocrinology 2001; 145: 289-294. [DOI:10.1530/eje.0.1450289]
11. Telli MH, Yildirim M, Noyan V. Serum leptin levels in patients with polycystic ovary syndrome. Fertility and Sterility 2002; 77: 932-935. [DOI:10.1016/S0015-0282(02)02995-3]
12. Ahima RS, Dushay J, Flier SN, Prabakaran D, Flier JS. Leptin accelerates the onset of puberty in normal female mice. Journal of Clinical Investigation 1997; 99: 391-395. [DOI:10.1172/JCI119172]
13. Agarwal SK, Vogel K, Weitsman SR, Magoffin DA. Leptin antagonizes the insulin-like growth factor-I augmentation of steroidogenesis in granulosa and theca cells of the human ovary. Journal of Clinical Endocrinology and Metabolism 1999; 84: 1072-1076. [DOI:10.1210/jc.84.3.1072]
14. Biason-Lauber A, Zachmann M, Schoenle EJ. Effect of leptin on CYP17 enzymatic activities in human adrenal cells: new insight in the onset of adrenarche. Endocrinology 2000; 141: 1446-1454. [DOI:10.1210/endo.141.4.7402]
15. Carmina E, Ferin M, Gonzalez F, Lobo RA. Evidence that insulin and androgens may participate in the regulation of serum leptin levels in women. Fertility and Sterility 1999; 72: 926-931. [DOI:10.1016/S0015-0282(99)00387-8]
16. Spritzer PM, Poy M, Wiltgen D, Mylius LS, Capp E. Leptin concentrations in hirsute women with polycystic ovary syndrome or idiopathic hirsutism: influence on LH and relationship with hormonal, metabolic, and anthropometric measurements. Human Reproduction 2001; 16: 1340-1346. [DOI:10.1093/humrep/16.7.1340]
17. Laughlin GA, Morales AJ, Yen SS. Serum leptin levels in women with polycystic ovary syndrome: the role of insulin resistance/hyperinsulinemia. Journal of Clinical Endocrinology and Metabolism 1997; 82:1692-1696. [DOI:10.1210/jc.82.6.1692]
18. Sir-Petermann T, Recabarren SE, Lobos A, Maliqueo M , Wildt L. Secretory pattern of leptin and LH during lactational amenorrhoea in breastfeeding normal and polycystic ovarian syndrome women. Human Reproduction 2001; 16: 244-249. [DOI:10.1093/humrep/16.2.244]
19. Lammert A, Kiess W, Bottner A, Glasow A , Kratzsch J. Soluble leptin receptor represents the main leptin binding activity in human blood. Biochemical and Biophysical Research Communications 2001; 283: 982-988. [DOI:10.1006/bbrc.2001.4885]
20. Kado N, Kitawaki J, Koshiba H, Ishihara H, Kitaoka Y, Teramoto M, et al. Relationships between the serum levels of soluble leptin receptor and free and bound leptin in non-pregnant women of reproductive age and women undergoing controlled ovarian hyper-stimulation. Human Reproduction 2003; 18: 715-720. [DOI:10.1093/humrep/deg186]
21. Sinha MK, Opentanova I, Ohannesian JP, Kolaczynski JW, Heiman ML, Hale J, et al. Evidence of free and bound leptin in human circulation. Studies in lean and obese subjects and during short-term fasting. Journal of Clinical Investigation 1996; 98: 1277-1282. [DOI:10.1172/JCI118913]
22. Ogawa T, Hirose H, Yamamoto Y, Nishikai K, Miyashita K, Nakamura H, et al. Relationships between serum soluble leptin receptor level and serum leptin and adiponectin levels, insulin resistance index, lipid profile, and leptin receptor gene polymorphisms in the Japanese population. Metabolism 2004; 53: 879-885. [DOI:10.1016/j.metabol.2004.02.009]
23. Van Dielen FM, van't Veer C, Buurman WA, Greve JW. Leptin and soluble leptin receptor levels in obese and weight-losing individuals. Journal of Clinical Endocrinology and Metabolism 2002; 87: 1708-1716. [DOI:10.1210/jcem.87.4.8381]
24. Yannakoulia M, Yiannakouris N, Bluher S, Matalas AL, Klimis-Zacas D , Mantzoros CS. Body fat mass and macronutrient intake in relation to circulating soluble leptin receptor, free leptin index, adiponectin, and resistin concentrations in healthy humans. Journal of Clinical Endocrinology and Metabolism 2003; 88: 1730-1736. [DOI:10.1210/jc.2002-021604]
25. Misra M, Miller KK, Almazan C, Ramaswamy K, Aggarwal A, Herzog DB, et al. Hormonal and body composition predictors of soluble leptin receptor, leptin, and free leptin index in adolescent girls with anorexia nervosa and controls and relation to insulin sensitivity. Journal of Clinical Endocrinology and Metabolism 2004; 89: 3486-3495. [DOI:10.1210/jc.2003-032251]
26. Li HJ, Ji CY, Wang W, Hu YH. A twin study for serum leptin, soluble leptin receptor and free insulin-like growth factor-1 in pub-ertal females. Journal of Clinical Endocrinology and Metabolism 2005; 90: 3659-3664. [DOI:10.1210/jc.2004-2079]
27. Matthews D, Hosker J, Rudenski A, Naylor B, Treacher D, Turner R. Homeostasis model assessment: insulin resistance and beta-cell function from fasting plasma glucose and insulin concentrations in man. Diabetologia 1985; 28: 412-419. [DOI:10.1007/BF00280883]
28. Sepilian VP, Crochet JR, Nagamani M. Serum soluble leptin receptor levels and free leptin index in woman with polycystic ovary syndrome: relationship to insulin resistance and androgens. Fertile sterile 2006; 85: 1441-1447. [DOI:10.1016/j.fertnstert.2005.10.038]
29. Chapman IM, Wittert GA, Norman RJ. Circulating leptin concentrations in polycystic ovary syndrome: relation to anthropometric and metabolic parameters. Clinical Endocrinology 1997; 46: 175-181. [DOI:10.1046/j.1365-2265.1997.1200936.x]
30. Rouru J, Anttila L, Koskinen P, Penttila TA, Irjala K, Huupponen R, et al. Serum leptin concentrations in women with polycystic ovary syndrome. Journal of Clinical Endocrinology and Metabolism 1997; 82: 1697-1700. [DOI:10.1210/jcem.82.6.3996]
31. Mantzorous CS, Dunaif A, Fiiler S. Leptin concentration in the polysistic ovary syndroume. Hounal of Clinical Endocrinology and Metabolism 1997; 82: 1697-1700. [DOI:10.1210/jcem.82.6.3996]
32. Houseknecht KL, Baile CA, Matteri RL, Spurlock ME. The biology of leptin: a review. Journal of Animal Science 1998; 76: 1405-1420. [DOI:10.2527/1998.7651405x]
33. Landt M, Parvin CA, Wong M. Leptin in cerebrospinal fluid from children: correlation with plasma leptin, sexual dimorphism, and lack of protein binding. Clinical Chemistry 2000; 46: 854-858.
34. Shimizu H, Shimomura K, Negishi M, Masunaga M, Uehara Y, Sato N, et al. Circulating concentrations of soluble leptin receptor: influence of menstrual cycle and diet therapy. Nutrition 2002; 18: 309-312. [DOI:10.1016/S0899-9007(01)00787-0]
35. Kado N, Kitawaki J, Koshiba H, Ishihara H, Kitaoka Y, Teramoto M, et al. Relationships between the serum levels of soluble leptin receptor and free and bound leptin in non-pregnant women of reproductive age and women undergoing controlled ovarian hyperstimulation. Human Reproduction 2003; 18: 715-720. [DOI:10.1093/humrep/deg186]
36. Jordan J, Brabant G, Brinsuk M, Tank J, Horn R, Luft FC, et al. Heritability of free and receptor-bound leptin in normal twins. Am J Physiol Regul Integr Comp Physiol 2005; 288: 411- 416. [DOI:10.1152/ajpregu.00446.2004]
37. Nobili V, Manco M, Ciampalini P, Diciommo V, Devito R, Piemonte F, et al. Leptin, free leptin index, insulin resistance and liver fibrosis in children with non-alcoholic fatty liver disease. European Journal of Endocrinolog 2006; 155: 735-743. [DOI:10.1530/eje.1.02288]
38. Mohiti-Ardekani J, Talebi F, Afkhami M. Free leptin in diabetic patients and its correlation to insulin level. Pakestan J of Biological Sci 2009; 12: 397-400. [DOI:10.3923/pjbs.2009.397.400]
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