Phenotypic effects of leptin replacement on morbid obesity, diabetes mellitus, hypogonadism, and behavior in leptin-deficient adults

Licinio, Júlio; Çağlayan, Suat; Özata, Metịn; Yildiz, Bülent O.; Miranda, Patrícia; O'Kirwan, Fiona; Whitby, R Michael; Liang, Liyin; Cohen, Pinchas; Bhasin, Shalender; Krauss, Ronald M.; Veldhuis, Johannes D.; Wagner, A.; DePaoli, Alex M.; McCann, Samuel M.; Wong, Ma-Li

doi:10.1073/pnas.0308767101

Cited by 441 publications

(397 citation statements)

References 45 publications

(44 reference statements)

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“…3, OMIM #164160) has been found mutated in very rare forms of human obesity. 2,3 The identification of a polymorphic tetranucleotide repeat in the 3 0 flanking region of the LEP gene (LEP-tet) provided an useful marker for linkage and association studies between this gene and a number of phenotypes other that obesity, such as noninsulin-dependent diabetes mellitus, hypertension and insulin resistance syndrome. 4,5 LEP-tet is composed by 15 alleles, which can be divided into two groups with different size distribution: a shorter one (class I) and a longer one (class II).…”

Section: Introductionmentioning

confidence: 99%

Microsatellite polymorphism of the human leptin gene (LEP) and risk of cardiovascular disease

et al. 2005

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Background: No data have been so far reported on the relationship between polymorphisms of LEP gene and cardiovascular disease. Patients and methods: We genotyped a tetranucleotide repeat mapped in the 3 0 UTR of the LEP gene (LEP-tet) in 109 subjects with cardiovascular events and in 109 control subjects. Results: Univariate analysis and multivariate logistic regression analysis adjusted for age, gender, smoking status, history of hyperlipidemia, hypertension or diabetes showed not significant association between the genotype of the LEP-tet and cardiovascular diseases. Moreover, no differences were observed in the plasma leptin concentrations between cases and control subjects (22719 vs 22714 ng/ml, P ¼ 0.52) and in relation to the LEP-tet classes or carriage of specific allelels (P ¼ 0.76 for the association between LEP-tet classes and leptin levels in overall analysis). Conclusions: In conclusion, our data do not support an association between the LEP-tet microsatellite polymorphism of the human LEP gene and cardiovascular diseases.

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Section: Introductionmentioning

confidence: 99%

Microsatellite polymorphism of the human leptin gene (LEP) and risk of cardiovascular disease

et al. 2005

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“…Accordingly, mutations in the ob gene encoding leptin produce hyperphagia and morbid obesity in mice (ob/ob mice) 5,17 and humans. [36][37][38][39][40] Similar to states of starvation, leptin deficiency also leads to deficits in the reproductive, thyroid, and adrenal axes. [41][42][43][44] Moreover, exogenous leptin corrects these manifestations in leptin-deficient mice [45][46][47][48] and humans.…”

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confidence: 99%

“…[41][42][43][44] Moreover, exogenous leptin corrects these manifestations in leptin-deficient mice [45][46][47][48] and humans. 38,40 Finally, the significance of leptin in adaptive endocrine and metabolic responses to fasting was demonstrated in healthy subjects. 49 In this study, a replacement dose of recombinant human leptin administered during fasting prevented the starvation-induced changes of endocrine axes.…”

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confidence: 99%

Body weight is regulated by the brain: a link between feeding and emotion

2005

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Regulated energy homeostasis is fundamental for maintaining life. Unfortunately, this critical process is affected in a high number of mentally ill patients. Eating disorders such as anorexia nervosa are prevalent in modern societies. Impaired appetite and weight loss are common in patients with depression. In addition, the use of neuroleptics frequently produces obesity and diabetes mellitus. However, the neural mechanisms underlying the pathophysiology of these behavioral and metabolic conditions are largely unknown. In this review, we first concentrate on the established brain machinery of food intake and body weight, especially on the melanocortin and neuropeptide Y (NPY) systems as illustration. These systems play a critical role in receiving and processing critical peripheral metabolic cues such as leptin and ghrelin. It is also notable that both systems modulate emotion and motivated behavior as well. Secondly, we discuss the significance and potential promise of multidisciplinary molecular and neuroanatomic techniques that will likely increase the understanding of brain circuitries coordinating energy homeostasis and emotion. Finally, we introduce several lines of evidence suggesting a link between the melanocortin/NPY systems and several neurotransmitter systems on which many of the psychotropic agents exert their influence. Maintaining energy homeostasis is fundamental for survival. However, obesity due to over-nutrition is an increasing worldwide public health problem. 1 In psychiatric practice, on the other hand, impaired appetite is one of the crucial issues. Anorexia and weight loss are common, for example, in patients suffering from depression. Eating disorders are medically intractable and life threatening. In addition, the so-called 'atypical' antipsychotic agents, currently and widely used to treat psychoses, often induce hyperphagia, obesity, and diabetes mellitus. [2][3][4] In the past decade, fortunately, there has been remarkable progress in understanding the molecular mechanisms of food intake and body weight. This is due in large part to increased research activity towards combating the rising incidences of obesity and associated metabolic disorders. As a result, it is now established that the central nervous system (CNS) senses and processes peripheral metabolic cues including leptin 5 and ghrelin, 6,7 resulting in coordinated energy homeostasis. However, the pathophysiology of the disequilibrium between energy intake and expenditure in psychiatric disorders remains largely unknown. Nevertheless, evidence suggests that several CNS systems regulating energy balance may be dysregulated in patients with mental illnesses, for example, eating disorders, and drug addiction. [8][9][10][11][12][13][14] In the current review, we will illustrate the neuroanatomic and molecular genetic aspects of the melanocortin and neuropeptide Y (NPY) systems residing in the CNS downstream of leptin and ghrelin, to discuss the neural bases of feeding, metabolism, and emotion. Additionally, we point the reader to...

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“…The doses of leptin were determined on the basis of a previous experiment in a rodent stroke model 17 and a leptin replacement study in leptin-deficient adults. 18 …”

Section: Induction Of Intracerebral Hemorrhage and The Injection Of Lmentioning

confidence: 99%

Detrimental Effects of Leptin on Intracerebral Hemorrhage via the STAT3 Signal Pathway

Kim

Ryu

Choi

et al. 2013

J Cereb Blood Flow Metab

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Leptin, one of the most important adipokines, is not only an energy regulator but also a regulator of innate immunity. Inflammation plays a key role in the tissue damage after intracerebral hemorrhage (ICH), and we sought to investigate whether leptin has a detrimental effect on ICH. After the injection of a high replacement dose (0.04 mg/kg) and two pharmacologic doses (4 and 8 mg/kg) of leptin, brain water contents increased significantly compared with that of control mice (Po0.05), which was confirmed when comparing the results with leptin-deficient ob/ob and wild-type (WT) mice (78.8% ± 0.6% versus 79.7% ± 0.6%, Po0.05). The number of Ox6-positive microglia/macrophages was increased in the leptin-injected group and decreased in ob/ob compared with WT mice. Among the candidate signal transducers, an increase in signal transduction and activator of transcription 3 (STAT3) levels was found after leptin injection. When we administered NSC74859, a specific inhibitor of phosphorylated STAT3 (pSTAT3), the water content became normalized. Activity of pSTAT3 was found mainly in Ox6-positive microglia/macrophages, but not in either neurons or astrocytes. We demonstrate that leptin plays a critical role in the secondary brain injury around a hematoma and is a novel mediator of the inflammation. This detrimental effect of leptin on ICH is mediated by the STAT3 signaling pathway in inflammatory cells.

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Phenotypic effects of leptin replacement on morbid obesity, diabetes mellitus, hypogonadism, and behavior in leptin-deficient adults

Cited by 441 publications

References 45 publications

Microsatellite polymorphism of the human leptin gene (LEP) and risk of cardiovascular disease

Microsatellite polymorphism of the human leptin gene (LEP) and risk of cardiovascular disease

Body weight is regulated by the brain: a link between feeding and emotion

Detrimental Effects of Leptin on Intracerebral Hemorrhage via the STAT3 Signal Pathway

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