Department of Epidemiology, Division of Cancer Prevention and Population Sciences, The University of Texas M.D. Anderson Cancer Center, Houston, TX, USA
US Department of Agriculture, Agricultural Research Service, Beltsville, MD, USA
National Center for Complementary and Alternative Medicine, National Institutes of Health, Bethesda, MD, USA
Nutritional Epidemiology Branch, Division of Cancer Epidemiology and Genetics, National Institutes of Health, Bethesda, MD, USA
Genetic Epidemiology Branch, Division of Cancer Epidemiology and Genetics, National Institutes of Health, Bethesda, MD, USA
Abstract
Background
The relationship between BMI and leptin has been studied extensively in the past, but previous reports in postmenopausal women have not been conducted under carefully controlled dietary conditions of weight maintenance using precise measures of body fat distribution. The aim of the present study was to examine the association between serum leptin concentration and adiposity as estimated by BMI and dual energy x-ray absorptiometry (DEXA) measures (percent body fat, central and peripheral fat, and lean mass) in postmenopausal women.
Methods
This study was conducted as a cross-sectional analysis within the control segment of a randomized, crossover trial in which postmenopausal women (n = 51) consumed 0 (control), 15 (one drink), and 30 (two drinks) g alcohol (ethanol)/d for 8 weeks as part of a controlled diet. BMIs were determined and DEXA scans were administered to the women during the 0 g alcohol treatment, and a blood sample was collected at baseline and week 8 of each study period for leptin analysis.
Results and discussion
In multivariate analysis, women who were overweight (BMI > 25 to ≤ 30 kg/m2) had a 2-fold increase, and obese women (BMI > 30 kg/m2) had more than a 3-fold increase in serum leptin concentrations compared to normal weight (BMI ≤25 kg/m2) women. When the models for the different measures of adiposity were assessed by multiple R2, models which included percent body fat explained the highest proportion (approximately 80%) of the serum leptin variance.
Conclusion
Under carefully controlled dietary conditions, we confirm that higher levels of adiposity were associated with higher concentrations of serum leptin. It appears that percent body fat in postmenopausal women may be the best adiposity-related predictor of serum leptin.
Background
Natural menopause, a normal aspect of aging, may influence risk of breast cancer
In various
Materials and methods
Study design
This study was part of a randomized, crossover, intervention trial of moderate alcohol supplementation in postmenopausal women (n = 51). Details of the study design and procedures have been published previously
Subjects
Postmenopausal women were recruited by advertisement from the communities surrounding the Beltsville Human Nutrition Research Center, Beltsville, MD. The eligibility criteria were:
This study was approved by the National Cancer Institute's Institutional Review Board and the Committee on Human Research of the Johns Hopkins University Bloomberg School of Hygiene and Public Health. All subjects were fully informed of the study requirements and were required to read and sign a consent form detailing the objectives, risks, and benefits of the study. The subjects were compensated for their participation.
Diets and feeding
All meals were prepared at the Beltsville Human Nutrition Research Center from typical U.S. foods and served in a seven-day menu cycle. Each day's diet provided 15% energy as protein, 50% energy as carbohydrate, and 35% energy as fat, with a polyunsaturated/monounsaturated/saturated fat ratio of 0.6:1:1. Daily fiber intake was 10 g/1,000 kcal, and daily cholesterol intake was 150 mg/1,000 kcal. Diets provided 100% of the U.S. recommended dietary allowances for vitamins and minerals
DEXA measurements
Body composition was determined by pencil beam dual energy x-ray absorptiometry (Lunar Corp., Model DPX-L, Madison, WI). Subjects were placed in a supine position with arms and legs close to their body for a whole body scan following the manufacturer's recommended protocol. Whole body and regional lean mass (mass of bone and nonfat soft tissue) and fat mass were determined using the manufacturer's algorithm (software version 1.33).
Biological sample collection and analysis
During the last week of the control treatment, blood samples for leptin analysis were collected from fasting (> 12 hours) subjects before breakfast (6:30 AM to 9:00 AM) on each of three non-consecutive days in each study period. An equal volume of serum from each day's blood draw was pooled for analysis. Serum was separated and aliquots were frozen at -70°C. The laboratory methods for the serum leptin measurements were described previously
Statistical analysis
Serum leptin concentrations were log transformed using the natural log. All estimates of means and the differences between means were made using the log transformed leptin values. In tables we report means and regression coefficients returned to the original (arithmetic) scale.
Pearson and Spearman correlations between the different DEXA measurements and BMI (kg/m2 calculated from measured weight and height) were determined. Mean serum leptin concentrations for BMI categories were estimated using linear regression models that included a series of indicator variables for three standard BMI categories (normal, ≤ 25 kg/m2; overweight, > 25 and ≤ 30 kg/m2; or obese, > 30 kg/m2). BMI categories were also modeled as ordinal variables with values 0, 1, and 2. Additional models estimated percent changes in serum leptin concentrations per one-unit change in BMI, one-percent change in total body fat (measured as percent body fat), and 1000 g change in central, peripheral, or lean mass modeled as continuous variables. All models included age (continuous), parity (continuous), race (example, African American, yes/no), age of menarche (less than 12, yes/no), and family history of breast cancer (mother or full sister with breast cancer, yes/no). One woman's breast cancer information was missing and she was excluded from models that included breast cancer history. Sensitivity models including her as having or not having a family history of breast cancer did not change analysis conclusions. In a second series of models (Model 2), we added BMI to Model 1 as a covariate The addition of alcohol group assignment order, study period, hysterectomy, duration of menses, years since last menses, nulliparity, and age at first birth (for those with children) did not improve the precision of the estimates and these terms were not included in the final models. There was no evidence of effect modification as assessed by likelihood ratio tests of model fit after the addition of cross-product terms to models that included main effects. Throughout the paper all
Results
Fifty-one women successfully completed the entire study and are included in the present analysis. The physical characteristics and reproductive history of the subjects at baseline are provided in Table
Characteristics of the subjects (N = 51) at baseline
Characteristics
Mean
Median
(range)
Age (y)
59.7
58.2
(49.2–78.8)
Height (cm)
163.9
163.1
(152.1–179.7)
Weight (kg)
74.8
73.2
(42.1–117.4)
BMI (kg/m2)
27.8
26.9
(17.7–42.5)
Total body fat (g)
29,744
26,808
(7,942–55,756)
Central fat (g)
13,830
13,234
(3,056–26,396)
Peripheral fat (g)
14,299
12,476
(4,163–29,507)
Lean mass (g)
39,608
38,973
(29,651–53,548)
% Body Fat
41.3%
42.5%
(17.8%–55.7%)
Age at menarche (yrs)
12.7
13
(10–16)
Duration of menses (yrs)
33.3
35
(12–45)
Years since last menses
13.1
12
(1–38)
Parity (# of children)
3
2
(0–8)
†Age at first birth (yrs)
23.2
22
(16–36)
Leptin, ng/dL
19.8
17.5
(2.9–78.2)
Characteristics
No
(%)
Race
White
38
(74.5%)
Black
11
(21.6%)
Asian
2
(3.9%)
Natural
39
(76.5%)
Hysterectomy
12
(23.5%)
Yes
11
(21.5%)
† Based on n = 43 subjects
Table
Geometric mean serum hormone concentrations by categories of BMI
BMI CATEGORY
BMI categories
(BMI ≤ 25)
(BMI > 25 to ≤ 30)
(BMI > 30)
N
20
17
14
Model
Mean, 95%, CI
Mean, 95%, CI
Mean, 95%, CI
Leptin, ng/mL
1†
8.59 (6.15–12.02)
16.32 (10.98–24.26)
30.09 (20.61–43.93)
< 0.0001
† Model 1 (n = 51) adjusted for age, race, family history of breast cancer, parity and menarche < 12 years.
Multiple R2 = 0.56
††
Table
Associations of BMI, percent body fat, central fat (trunk fat), peripheral fat, and lean mass with serum leptin concentrations
Leptin, ng/mL
Δ (95% C.I.)
Multiple R2
BMI
Model 1
10.65 (8.16–13.19)
< 0.0001
0.68
Model 2
% Fat
Model 1
7.77 (6.56–8.98)
< 0.0001
0.82
Model 2
7.20 (4.72–9.75)
< 0.0001
0.82
Central fat
Model 1
11.93 (9.72–14.18)
< 0.0001
0.77
Model 2
11.58 (5.87–17.61)
0.0002
0.77
Peripheral fat
Model 1
10.55 (8.33–12.81)
< 0.0001
0.72
Model 2
7.98 (2.13–14.16)
0.01
0.73
Lean mass
Model 1
8.61 (3.76–13.68)
0.001
0.31
Model 2
-0.85 (-4.81–3.25)
0.68
0.68
Δ - Percent change for serum leptin concentration for a one-unit change in each of the adiposity measures (i.e., percent change in leptin concentration per one-unit change in BMI, per 1% increase in total body fat, per 1 kg increase in central and peripheral fat and lean mass).
Model 1: Adjusted for age, race, family history of breast cancer, parity and menarche < 12 years
Model 2: Model 1 + BMI
When multiple R2 was used to assess the strength of the linear associations of the overall models to leptin (Table
Discussion
The objective of the study was to identify the relationship between well-defined measures of body fat distribution and lean body mass and circulating leptin concentrations in healthy postmenopausal women. Our results showing that postmenopausal women with higher levels of adiposity have higher concentrations of serum leptin confirm the findings from several previous reports which showed positive correlations between adiposity and leptin concentrations
Although our study showed that obese women, compared to normal weight women had a greater than three-fold increase in serum leptin concentrations, we also found evidence that both measures of central and peripheral body fat provided additional predictive information beyond that achieved by BMI and other breast cancer risk factors.
Our adiposity measures are on different scales and it is difficult for example, to compare changes of one percent in body fat versus one kg body fat versus one BMI unit, thus we also used multiple R2 values to summarize these associations. The multiple R2 values from the linear regression models reflect the percent variance explained by each of the adiposity variable models (BMI, percent body fat, central and peripheral fat, and lean mass), all adjusted for the covariates, so that they can be compared. Looking at the multiple R2 values, we found the percent body fat model explains a largest proportion (more than 80%) of the variance associated with serum leptin concentrations, and thus appear to be very strongly associated with serum leptin concentrations. However, all of the R2 values in Table
In addition to the previous studies which suffer from inadequate control of diet and energy balance (known confounders of leptin levels)
Since increased BMI
Although our study is limited by its cross-sectional design and modest sample size, the strengths of this study include a homogeneous study population (eg, smokers and women taking HRT were excluded) and measurement stability, which resulted from the use of a carefully controlled diet adjusted to maintain body weight. The DEXA scans employed are considered a reference method for body composition analysis
In conclusion, our study demonstrated that serum leptin concentrations showed striking differences by adiposity levels. Increased exposure to leptin was observed for increased adiposity determined by BMI, percent body fat, central and peripheral fat as well as lean body mass. Although BMI and DEXA adiposity (percent body fat, central fat and peripheral fat) are highly correlated in this cross-sectional study, it remains for further studies to confirm and refine our observations regarding: (i) percent body fat as the best adiposity-related predictor of serum leptin, and (ii) the independent value of central body fat in this prediction even after adjustment for BMI. Because of the well-known arguments for limitations in the use of BMI
Competing interests
The author(s) declare that they have no competing interests.
Acknowledgements
The present work was funded in part by the interagency agreement Y1-SC-8012. SM and LLJ were involved with data analysis, interpretation and writing of the manuscript. DB, WC, and BC were involved with the design and execution of the study, and the interpretation of the results. MR was involved with the laboratory analyses. PRT was the principal investigator, oversaw all aspects of the project, and was involved with data interpretation, and manuscript preparation.