AI Article Synopsis
- GLP-1-producing neurons in the brain, specifically in the nucleus tractus solitarii (NTS), are key for producing endogenous GLP-1, which is known to suppress food intake.
- Despite this, experiments showed that removing these neurons did not significantly impact normal feeding or body weight in mice, indicating they play a secondary role in food intake regulation.
- However, when faced with larger challenges, like fasting, these neurons became important for controlling food intake, suggesting a potential role for targeting PPG neurons in obesity treatments.
Article Abstract
Centrally administered glucagon-like peptide 1 (GLP-1) supresses food intake. Here we demonstrate that GLP-1-producing (PPG) neurons in the nucleus tractus solitarii (NTS) are the predominant source of endogenous GLP-1 within the brain. Selective ablation of NTS PPG neurons by viral expression of diphtheria toxin subunit A substantially reduced active GLP-1 concentrations in brain and spinal cord. Contrary to expectations, this loss of central GLP-1 had no significant effect on the ad libitum feeding of mice, affecting neither daily chow intake nor body weight or glucose tolerance. Only after bigger challenges to homeostasis were PPG neurons necessary for food intake control. PPG-ablated mice increased food intake after a prolonged fast and after a liquid diet preload. Consistent with our ablation data, acute inhibition of hMDi-expressing PPG neurons did not affect ad libitum feeding; however, it increased refeeding intake after fast and blocked stress-induced hypophagia. Additionally, chemogenetic PPG neuron activation through hMDq caused a strong acute anorectic effect. We conclude that PPG neurons are not involved in primary intake regulation but form part of a secondary satiation/satiety circuit, which is activated by both psychogenic stress and large meals. Given their hypophagic capacity, PPG neurons might be an attractive drug target in obesity treatment.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6314470 | PMC |
| http://dx.doi.org/10.2337/db18-0729 | DOI Listing |
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