Obesity, the primary health threat in the 21st century, affects the quality of life physiologically, economically and psychologically, irrespective of cultural, financial or ethnic background. Prevalence of obesity has been increasing steadily during the past 30 years worldwide, especially in developed countries. In America, almost one-third of adult population are obese (BMI ≥30 kg/m2)1 and healthcare expenditure for obesity had reached nearly 75 billion USD in 20032. A similar picture has been seen in developing countries as well where incidence of obesity is rising at an alarming speed. In China, according to one report, 12.1% and 2.6% of the urban population are either overweight (25 kg/m2≤ BMI ≤30 kg/m2) or clinically obese (BMI ≥30 kg/m2)3. The situation in children is more disturbing: a 2005 study conducted in northern coastal large cities of China shows that the combined prevalence of obesity had reached 32.5% in boys and 17.6% in girls, respectively4. Possible contributing factors may include steady economic growth, lifestyle changes and significantly reduced family size since the late 1970's.

From a medical stand point, obesity contributes to a broad range of health issues, involving type 2 diabetes mellitus, cardiovascular and kidney diseases (see review by Barton), as well as certain cancers, etc5. It significantly increases mortality, causes physical impairment and psychological stigma, and results in economic burden that is largely unmanageable even in many affluent societies. Therefore, prevention and treatment of obesity are a common challenge with extraordinary urgency to both developed and developing nations, and all-out efforts are required to exploit efficient strategies, from policy to education, from research to industry, and from physicians to patients.

Obesity is generally recognized as disturbances in energy homeostasis between nutrient intake and expenditure. The balance is controlled by the central nervous system (CNS), mainly the neurons located in hypothalamus. They sense nutrient molecules in circulation and peripheral signaling proteins released by organs in order to regulate energy homeostasis6. However, the exact molecular mechanisms relative to pathogenesis of obesity remain elusive (see review by Herbst), and may include interaction of different genes (see article by Ke et al), environmental factors, life style, social status and even intrauterine or neonatal nutritional states7. It is believed that a chronic, low grade inflammation, in response to excess nutrients or energy, in the metabolic tissues is involved in the development of obesity (see review by Gao and Ye). A cascade may exist starting from release of inflammatory cytokines [tumor necrosis factor (TNF)-α, interleukin-1(IL-1)β, CCL2, etc] and activation of inflammatory kinases (JNK, IKK, PKR etc) by metabolic cells, progressing towards tissue malfunction (eg insulin resistance), and eventually linking inflammation to obesity-related diseases, such as type 2 diabetes8.

While prevention is largely dependent upon change of life style, therapeutic approaches are dominated by medications that result in weight loss, covering both small molecules and peptides aiming at a variety of drug targets (Tables 1 and 2)9, 10, 11. Of which, sibutramine, phentermine, rimonabant, lorcaserin, contrave, qnexa, liraglutide, tesofensine and velneperit, etc, target the CNS and decrease energy intake via reducing appetite or increasing satiety, whereas orlistat and cetilistat interfere with nutrient absorption in the digestive system. Although the pipeline looks prosperous, only one drug (orlistat) is available at present for long-term weight control because sibutramine was withdrawn last year due to an increased cardiovascular risk12. Others that were approved for short-term treatment (eg phentermine, diethylpropion, benzphetamine and phendimetrazine) all have the limitation of controlled use because of potential drug abuse13.

Table 1 Anti-obesity drugs approved, rejected, withdrawn or revised by the FDA.
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Table 2 A glance of new anti-obesity drugs in the pipeline.
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With worldwide demands for a “magic bullet” to loose body weight, major pharmaceutical companies are chasing after the multibillion-dollar obesity market even under extremely high risks. In 2010, Sanofi-Avantis decided to discontinue all ongoing clinical trials and to suspend sales of its cannabinoid 1 receptor (CB1R) blocker, rimonabant, following the recommendation from the European Medicines Agency in response to serious psychiatric side-effects14. Merck and Pfizer wasted no time to cease the development of their versions of CB1R antagonists, taranabant and CP-945598, respectively, making CB1R as a drug target dubious. Thus, a new strategy to discover selective CB1R blockers that predominantly interact with the receptor in the periphery has been debated14.

Haunted by the withdrawal of sibutramine and the end of CB1R blockers, the developers of anti-obesity drugs experienced further setbacks. Apart from rejecting regulatory approval of Vivus's combination product qnexa and Arena's locaserin15, the Food and Drug Administration requested a cardiovascular outcome study for another combination therapy, Orexigen's contrave10. Obviously, the paramount concern on therapeutics against obesity is safety because it is not a fatal disease and requires long-term management. In comparison with physical exercise and diet control that demand for active participation, the advantage of a safe and efficacious pill is unquestionable albeit it is passive in terms of patient efforts.

The multi-facet actions of the gut hormone, glucagon-like peptide-1 (GLP-1), render it ideal as a target for drug intervention16. Encouraged by early success with a GLP-1 mimetic, exenatide, in diabetic weight loss17, liraglutide, a long-acting GLP-1 analog, was shown to reduce body weight in both animal models of obesity (see article by Hansen et al) and human clinical studies18. Similar effects in animal models were also seen with a non-peptidic GLP-1 receptor agonist Boc519 and one of its analogs (see review by He et al).

As demonstrated in the treatment of many other diseases, combination therapy is more effective than a single agent. Of the four such products (qnexa, contrave, empatic and pramlintide), qnexa and contrave were previously approved for other indications. Clinical trials revealed that qnexa (phentermine plus topiramate) and contrave (bupropion plus naltrexone) administration induced a net weight loss of 12.2 kg and 6.2 kg, respectively, compared with a reduction of 4.0 kg or 3.2 kg when phentermine or bupropion was administered alone10.

Facing such an unprecedented challenge on a global scale, it is far from adequate in terms of novel approaches to obesity management. Clearly, the most important task lies in education that alters social behavior capable of preventing the prevalence of obesity from rising. In this special issue, several topics that relate to obesity etiology, animal models (see review by Nilsson et al), therapeutics and clinical implications are covered in order to provide a glance of the latest developments in this important field.