Centrally Acting Agents for Obesity: Past, Present, and Future.
Drugs · 2018
Last updated 2026-07-06Obesity was only recognized as a chronic disease in 1985 by scientists and 2013 by doctors, leading to a shift from short-term to long-term treatments. Current weight-loss drugs like phentermine/topiramate, bupropion/naltrexone, lorcaserin, and liraglutide work by targeting brain pathways to reduce appetite. Future options in development include tesofensine (a triple reuptake inhibitor) and semaglutide (an oral GLP-1 drug), while setmelanotide targets a specific brain receptor. Research is also exploring drugs that act outside the brain, focusing on gut, fat, and other tissues.
AI summary of the abstract below.
| Journal | Drugs, 2018 |
|---|---|
| Citations | 101 |
| Relative citation ratio | 4.47 |
| NIH percentile | 91 |
| Molecules | — |
Abstract
For many years, obesity was believed to be a condition of overeating that could be resolved through counseling and short-term drug treatment. Obesity was not recognized as a chronic disease until 1985 by the scientific community, and 2013 by the medical community. Pharmacotherapy for obesity has advanced remarkably since the first class of drugs, amphetamines, were approved for short-term use. Most amphetamines were removed from the obesity market due to adverse events and potential for addiction, and it became apparent that obesity pharmacotherapies were needed that could safely be administered over the long term. This review of central nervous system (CNS) acting anti-obesity drugs evaluates current therapies such as phentermine/topiramate, which act through multiple neurotransmitter pathways to reduce appetite. In the synergistic mechanism of bupropion/naltrexone, naltrexone blocks the feed-back inhibitory circuit of bupropion to give greater weight loss. Lorcaserin, a selective agonist of a serotonin receptor that regulates food intake, and the glucagon-like-peptide-1 (GLP-1) receptor agonist liraglutide are reviewed. Future drugs include tesofensine, a potent triple reuptake inhibitor in Phase III trials for obesity, and semaglutide, an oral GLP-1 analog approved for diabetes and currently in trials for obesity. Another potential new pharmacotherapy, setmelanotide, is a melanocortin-4 receptor agonist, which is still in an early stage of development. As our understanding of the communication between the CNS, gut, adipose tissue, and other organs evolves, it is anticipated that obesity drug development will move toward new centrally acting combinations and then to drugs acting on peripheral target tissues.
Verbatim abstract via PubMed 30014268 ↗