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| November 2001, Volume 25, Number 11, Pages 1625-1632 |
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| Paper |
| Lack of heritability of circulating leptin concentration in humans after adjustment for body size and adiposity using a physiological approach |
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| A B Jenkins1, K Samaras2,3, M A Gordon1, H Snieder4,5, T Spector4 and L V Campbell6 |
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1Metabolic Research Centre and Department of Biomedical Science, University of Wollongong, Wollongong, NSW, Australia
2St Vincents Clinic, Darlinghurst, NSW, Australia
3Gemini Genomics plc, Cambridge, UK
4Twin Research Unit, St Thomas's Hospital, London, UK
5Georgia Prevention Institute, Medical College of Georgia, Augusta, Georgia, USA
6Diabetes Centre, St Vincents Hospital, Darlinghurst, NSW, Australia
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Correspondence to: A B Jenkins, Department of Biomedical Science, University of Wollongong, Wollongong, NSW, 2522 Australia. E-mail: arthur_jenkins@uow.edu.au
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| Abstract |
| OBJECTIVE: To construct a simple physiological model of leptin kinetics, based on measures of body size and composition, which is suitable for investigating the influence of genetic and other influences on circulating leptin levels in humans. METHODS: Consideration of the kinetics of the secretion and clearance of leptin led to a predicted linear relationship between ln(leptin), ln(fat mass), and a function of non-fat body compartments. Results obtained from this model were compared with those from two published empirical models based on adjustment for fat mass alone or for body mass index. Overnight fasted leptin levels, body composition data (dual-energy X-ray absorptiometry) and questionnaire responses were obtained from 527 twin pairs (127 monozygotic, 400 dizygotic; 37 male (age 18-68 y, BMI 18-32 kg/m2), 489 female (age 18-71, BMI 17-44) drawn from the St Thomas' UK Adult Twin Registry. RESULTS: In a partial correlation analysis ln(fat mass) and ln(height) (r=0.80, P<0.0001) and r=-0.22, P<0.0001 respectively) were independent predictors of ln(leptin) in females but ln(lean mass) was not (r=-0.01). A regression model incorporating ln(fat mass), ln(height) and a second order polynomial in age provided an adequate fit of the ln(leptin) data in females (r 2=71%). ln(Leptin) values adjusted for body size and composition using the model were not significantly heritable (P=0.11), were significantly related to gender (r 2=2.3%) and to ln(insulin) (r 2=5.7%), but not to menopausal status (r 2=0.7%), hormone replacement therapy (r 2=0.4%), past or current smoking (r 2=1.1%), or percentage trunk fat (r 2=0.5%). Both empirical models found significant heritability (h2=36-42%), overestimated the effect of gender in the data (r 2=14-16%), and produced significant relationships between adjusted ln(leptin) and percentage trunk fat (r 2=4-12%). CONCLUSIONS: We conclude that our physiologically based model provides an adequate description of the relationship between leptin and body composition and provides a more reliable framework than current empirical approaches for the investigation of other influences on circulating leptin levels. Heritable variations in the control of leptin secretion are unlikely to contribute significantly to variations in leptin levels at the population level. International Journal of Obesity (2001) 25, 1625-1632 |
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| Keywords |
| leptin; adiposity; body composition; model; heritability |
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| Received 25 September 2000; revised 17 April 2001; accepted 1 May 2001 |
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| November 2001, Volume 25, Number 11, Pages 1625-1632 |
| Table of contents Previous Abstract Next Full text PDF |
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