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Journal of
eISSN: 2374-6947

Diabetes, Metabolic Disorders & Control

Editorial Volume 2 Issue 1

Management of pediatric obesity

Pedro Marques

Department of Endocrinology, Portuguese Institute of Oncology of Lisbon, Portugal

Correspondence: Pedro Marques, Department of Endocrinology, Portuguese Institute of Oncology of Lisbon, Rua Professor Lima Basto, 1099-023, Lisbon, Portugal, Tel +351 916573936, Fax +351 217 229 880

Received: January 12, 2015 | Published: January 13, 2015

Citation: Marques P. Management of pediatric obesity. J Diabetes Metab Disord Control. 2015;2(1):14-15. DOI: 10.15406/jdmdc.2015.02.00027

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Abbreviations

BMI, body mass index; T2DM, type 2 diabetes mellitus

Editorial

The prevalence of childhood and adolescent obesity is increasing worldwide and constitutes a major public health concern.1 Pediatric obesity is defined as body mass index (BMI) equal to or greater than 95th percentiles adjusted for age and sex; the children or adolescents are considered overweight for BMIs between 85th to 95th percentiles.2 Weight excess in childhood has increased the prevalence of some conditions practically only found in adulthood some years ago, such as impaired glucose tolerance and type 2 diabetes mellitus (T2DM), dyslipidemia, hypertension and liver steatosis.3 The early development of these conditions is associated with cardiometabolic mordibity and premature death.4 Intervention may prevent those complications or avoid further deterioration of cardiovascular and metabolic status.

The mainstay approach of pediatric obesity is lifestyle modification, which includes dietary changes and stimulation of physical activity, ideally involving also patient’s parents, family, friends or even the school.5 Dietary and nutritional education must emphasize the reduction or avoidance of calorie-dense, nutrition-poor foods, such as sugar beverages, juices, fast food and moderate to vigorous physical exercise must be promoted, at daily basis with duration of 30 to 60minutes.6 Lifestyle interventions often fail in achieving weight loss and some patients will continue to gain weight and develop metabolic comorbidities. In these circumstances, pharmacotherapy combined with lifestyle measures should be considered only for obese children or adolescents, especially in the presence of cardiovascular risk factors or strong family history of cardiometabolic diseases, such T2DM. Currently, the only FDA-approved drug for obese children (over 12years) is orlistat. However, some other drugs have been studied and used off label to treat pediatric obesity.7 Orlistat is a reversible pancreatic lipase inhibitor that limits the absorption of dietary cholesterol in approximately 30%.5 The orlistat largest randomized trial, where 539 obese adolescents were randomized to receive either orlistat (n=357) or placebo (n=182) combined with lifestyle intervention, has shown a significant decrease of BMI after 12months in the orlistat group (ΔBMI -0.55kg/m2 vs +0.31kg/m2; p=0.001).8 Pooling the available data together, 120mg of orlistat three times daily combined with lifestyle intervention may significantly decrease BMI from 0.5 to 4.09kg/m2. The frequent gastrointestinal side effects, occurring in 65 to 100% of the patients under orlistat, may limit therapy adherence and efficacy.7

Metformin stimulates AMP-activated protein kinase, reducing hepatic glucose production, decreasing intestinal glucose absorption and improving the peripheral insulin sensitivity.9,10 This drug, well-established and FDA-approved for T2DM in children older than 10years of age, has been used off labelin pediatric obesity.9 Some randomized trials were conducted in order to clarify metformin role in nondiabetic overweight/obese pediatric patients, and the majority of them suggest metformin beneficial in terms of weight loss and insulin resistance improvement; metformin has also been well-tolerated and safe, with no severe side effects or fatal events described so far.9,11?13 Thus, metformin is seen as a promising agent to treat obese pediatric patients with impaired glucose tolerance, although its use remains controversial due to the lack of data, especially at long term basis as there are no trials conducted for more than 12months.11,12

The increasing incidence of obesity in the pediatric setting, has led to additional investigation on alternative pharmacological therapies to manage this condition. In the past, sibutramine was approved from FDA to treat pediatric obesity due to its capacity to promote satiety and stimulate the energy expenditure.14 It was regarded as an effective drug and extensively used, demonstrating significant decreases of BMI up to 4kg/m2 and improvement of metabolic risk factors when compared to placebo groups.15 However, issues regarding cardiovascular safety led to sibutramine’s withdraw in 2010.16 Other experimental drugs have been studied in childhood obesity, such as octreotide, topiramate, growth hormone, leptin but conclusive data or significant trials are not available, therefore those cannot be recommended.5

Ultimately, selected cases of severe pediatric obesity may be considered for bariatric surgery. This approach, highly effective to treat adult obesity, has several potential complications in the pediatric setting. Bariatric surgery may be considered only if the children has BMI>50kg/m2 or BMI>40kg/m2 with comorbidities, if lifestyle modification with or without pharmacological intervention fails and if a pubertal Tanner 4/5 status and final/near-final adult height was already achieved.5,17

Summarizing, the increasing incidence of pediatric obesity and its cardiometabolic impact, the disappointing effectiveness of lifestyle intervention and the lack of pharmacological alternatives to treat this condition, justifies the efforts from medical community to find effective (new) drugs and to expand the knowledge on the available drugs to treat this entity. Thus, considering the high relevance of this topic, we hope to have contributors and original research data to expand the scientific knowledge on this matter.

Acknowledgements

None.

Conflict of interest

Author declares that there is no conflict of interest.

References

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©2015 Marques. This is an open access article distributed under the terms of the, which permits unrestricted use, distribution, and build upon your work non-commercially.

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