Submitted:
01 January 2025
Posted:
03 January 2025
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Abstract
Obesity remains a complex global health issue, necessitating multifaceted treatment approaches. Injectable pharmacotherapies have emerged as effective strategies to manage obesity by targeting metabolic pathways that regulate appetite, energy expenditure, and fat distribution. This review explores the mechanisms, clinical efficacy, and safety profiles of key injectable agents, including GLP-1 and GIP receptor agonists, pancreatic lipase inhibitors, and lipolytic compounds. Additionally, it highlights the aesthetic challenges following significant weight loss, such as skin laxity, and discusses the role of biostimulators and non-invasive technologies in mitigating these effects. Despite the therapeutic promise of injectable agents, their widespread application is hindered by adverse effects, high costs, and accessibility issues. This paper underscores the need for integrative treatment models that combine pharmacological interventions with aesthetic and behavioral therapies to optimize patient outcomes. Future research should focus on refining personalized protocols and expanding the accessibility of these treatments to diverse populations.
Keywords:
1. Introduction
2. Materials and Methods
3. Physiology of Obesity
4. Injectable Medications for Weight Loss
5. Injectable Metabolic Accelerators for Weight Loss
6. Common Drug Interactions
7. Safety and Toxicology
8. Injectable Weight Loss Agents and Aesthetic Dysfunctions: Strategies to Combat Skin Laxity with Biostimulators and Technologies
9. Discussion
10. Conclusions
Author Contributions
Funding
Institutional Review Board Statement
Data Availability Statement
Acknowledgments
Conflicts of Interest
References
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| Drug Class | Medication Name | Brand Name | Dosage | Administration Interval | Manufacturer | Country of Origin |
|---|---|---|---|---|---|---|
| GLP-1 Receptor Agonists | Liraglutide | Saxenda® | 0.6 mg to 3 mg per day, subcutaneous | Daily | Novo Nordisk | Denmark |
| GLP-1 Receptor Agonists | Semaglutide | Ozempic® | 0.25 mg to 2.4 mg per week, subcutaneous | Weekly | Novo Nordisk | Denmark |
| GLP-1 and GIP Receptor Agonists | Tirzepatide | Mounjaro® | 5 mg to 15 mg per week, subcutaneous | Weekly | Eli Lilly | United States |
| Pancreatic Lipase Inhibitors | Orlistat* | Xenical® | 120 mg three times per day, oral | Three times per day | Roche | Switzerland |
| Beta-3 Adrenergic Agonists | Mirabegron* | Betmiga® | 50 mg to 200 mg per day, oral | Daily | Astellas Pharma | Japan |
| Active Ingredient | Classification | Dosage | Mechanism of Action |
|---|---|---|---|
| Caffeine | Thermogenesis Stimulant | 50 mg to 100 mg/day | Adenosine antagonist; increases thermogenesis |
| Taurine | Thermogenesis Stimulant | 200 mg/day | Promotes lipid metabolism and antioxidant function |
| L-Carnitine | Lipolysis Modulator | 200 mg to 600 mg, 2-3 times/day | Transports fatty acids to the mitochondria |
| Chromium Picolinate | Lipolysis Modulator | 100 mcg/day | Improves insulin signaling |
| Inositol | Lipolysis Modulator | 100 mg to 200 mg/day | Supports lipid metabolism and reduces visceral fat |
| Choline | Lipolysis Modulator | 200 mg to 500 mg/day | Involved in lipid metabolism and reduces liver fat |
| N-Acetyl | Appetite Regulator | 20 mg to 50 mg/day | Modulates neurotransmitters for appetite control |
| L-Tyrosine | Appetite Regulator | 20 mg to 50 mg/day | Precursor of dopamine; increases energy expenditure |
| 5-HTP | Appetite Regulator | 4 mg to 20 mg/day | Precursor of serotonin; reduces food cravings |
| L-Theanine | Appetite Regulator | 10 mg to 20 mg/day | Modulates GABA receptors; reduces food-related anxiety |
| Phenylalanine | Appetite Regulator | 50 mg/day | Precursor of dopamine; controls appetite and mood |
| Vitamin B12 | Metabolic Optimizer | 2500 mcg/day | Improves energy metabolism and neurological function |
| L-Arginine | Metabolic Optimizer | 200 mg to 600 mg/day | Precursor of nitric oxide; improves vasodilation |
| Ornithine | Metabolic Optimizer | 200 mg/day | Involved in the urea cycle; reduces ammonia |
| Methionine | Metabolic Optimizer | 100 mg/day | Methyl group donor; reduces visceral fat |
| Drug/Class | Potential Interactions | Clinical Recommendations |
|---|---|---|
| Liraglutide (GLP-1 Agonist) | Risk of reduced absorption of oral medications; potential nausea enhancement with thermogenics. | Monitor gastrointestinal symptoms and adjust oral medication doses. |
| Semaglutide (GLP-1 Agonist) | Risk of interaction with hypoglycemics; enhancement of gastrointestinal symptoms with caffeine. | Avoid combinations with potent hypoglycemics; start with low doses. |
| Tirzepatide (GLP-1 and GIP Agonist) | Risk of pancreatitis; interaction with hypoglycemics can cause hypoglycemia. | Monitor blood glucose and signs of pancreatitis; avoid aggressive combinations. |
| Orlistat (Pancreatic Lipase Inhibitor) | Reduces absorption of fat-soluble vitamins; interactions with lipid modulators may exacerbate vitamin deficiencies. | Prescribe vitamin supplementation for long-term use. |
| Mirabegron (Beta-3 Agonist) | Interaction with thermogenics may cause tachycardia and increased blood pressure; interactions with CYP2D6. | Avoid combination with potent thermogenics in hypertensive patients. |
| L-Carnitine (Lipid Modulator) | Potential increase in ammonia with combined use; exacerbation of gastrointestinal disorders with thermogenics. | Monitor ammonia levels; adjust doses of synergistic agents. |
| Chromium Picolinate (Lipid Modulator) | Mild interactions; potential synergy with metabolic modulators. | Assess synergistic impacts; maintain adequate supplementation. |
| 5-HTP (Appetite Regulator) | Risk of serotonin syndrome with antidepressants; interaction with thermogenics may cause insomnia. | Avoid patients taking antidepressants; monitor insomnia. |
| L-Arginine (Metabolic Optimizer) | Hypotension in combination with antihypertensives; interaction with thermogenics may exacerbate cardiovascular effects. | Monitor hypotension; carefully adjust in combined protocols. |
| HMB (Metabolic Optimizer) | Generally safe; minimal metabolic interactions with accelerators. | General monitoring; considered safe for therapeutic combinations. |
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