Incretin-Based Therapies: A Novel Pathway in Addiction Treatment
Abstract
1. Epidemiology of Addiction
2. Literature Search Methodology
3. Incretins
3.1. History
3.2. Drug Classes and Their Therapeutic Indications
3.3. Mechanism of Action and Therapeutic Potential in Addiction Treatment
4. Incretins and Alcohol
4.1. Preclinical Study
4.2. Human Studies
5. Incretins and Nicotine Use
6. Incretins and Psychoactive Substances
6.1. Psychostimulants
6.2. Opioids
6.3. Cannabinoids
7. Clinical Perspectives and Future Research Directions
8. Conclusions
Author Contributions
Funding
Data Availability Statement
Acknowledgments
Conflicts of Interest
Abbreviations
| 2-OG | 2-oleoylglycerol |
| ACC | anterior cingulate cortex |
| AMPH | amphetamine |
| AUD | alcohol use disorders |
| AUDIT | Alcohol Use Disorder Identification Test |
| BMI | Body mass index |
| BNST | bed nucleus of the stria terminalis |
| CAP | controlled attenuation parameter |
| CB1 | cannabinoid receptor type 1 |
| CBT | Cognitive–Behavioral Therapy |
| CI | confidence interval |
| CPP | conditioned place preference |
| CUD | cannabis use disorder |
| CVD | cardiovascular disease |
| cAMP | cyclic adenosine monophosphate |
| DA | dopamine |
| DALYs | disability-adjusted life years |
| DAT | dopamine transporter |
| D1R | dopamine D1 receptor |
| D2R | dopamine D2 receptor |
| DMS | dorsomedial striatum |
| DPP-IV | dipeptidyl peptidase-4 |
| EMA | European Medicines Agency |
| EU | European Union |
| EX-4 | exendin-4 |
| FDA | Food and Drug Administration |
| GABA | gamma-aminobutyric acid |
| GEP44 | dual glucagon-like peptide-1 receptor/neuropeptide Y2 receptor agonist |
| GIP | glucose-dependent insulinotropic polypeptide |
| GLP-1 | glucagon-like peptide-1 |
| GLP-1R | glucagon-like peptide-1 receptor |
| GLP-1RA | glucagon-like peptide-1 receptor agonist |
| HIV | Human Immunodeficiency Virus |
| HR | hazard ratio |
| IL | interleukin |
| IPN | interpeduncular nucleus |
| LDTg | laterodorsal tegmental nucleus |
| LS | lateral septum |
| MHb | medial habenula |
| MetALD | metabolic dysfunction and alcohol-associated liver disease |
| MSNs | medium spiny neurons |
| NAc | nucleus accumbens |
| ND | no data |
| NF-κB | nuclear factor κB |
| NRT | nicotine replacement therapy |
| NTS | nucleus tractus solitarius |
| OEA | oleoylethanolamide |
| OFC | orbitofrontal cortex |
| OX1 | orexin receptor type 1 |
| PFC | prefrontal cortex |
| Po | per os |
| RCT | randomized clinical trial |
| SA | self-administration |
| Sc | subcutaneously |
| SNPs | single-nucleotide polymorphisms |
| T2D | type 2 diabetes |
| THC | Δ9-tetrahydrocannabinol |
| TLFB | Timeline Follow Back |
| TLR4 | Toll-like receptor 4 |
| TNF | tumor necrosis factor |
| VTA | ventral tegmental area |
| WHO | World Health Organization |
| Y2R | neuropeptide Y2 receptor |
| ↑ | increased |
| ↓ | decreased |
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| NCT Identifier | Drug | Administration | n = | Study Group | Comparator | Primary Outcome | Expected End Date |
|---|---|---|---|---|---|---|---|
| NCT05895643 | Semaglutide | sc, 2.4 mg once weekly | 108 | individuals diagnosed with alcohol use disorder and comorbid obesity (BMI > 30 kg/m2). | placebo | Change in heavy drinking days | December 2025 |
| NCT05891587 | Semaglutide | sc, 1.0 mg once weekly | 80 | individuals who endorse symptoms consistent with alcohol use disorder | placebo | Change in alcohol drinking measured per week | December 2025 |
| NCT05892432 | Semaglutide | po, 7.0 mg once daily | 50 | treatment-seeking individuals with AUD | placebo | Change in alcohol craving | October 2025 |
| NCT06015893 | Semaglutide | sc, 2.4 mg once weekly | 52 | individuals with AUD | placebo | Change in alcohol consumption | December 2030 |
| NCT07249554 | Semaglutide + Naltrexone | po, 7.0 mg once daily | 45 | individuals with AUD | placebo + placebo, placebo + GLP-1, GLP-1 + Naltrexone | Participant-reported Adverse Events | June 2028 |
| NCT07218354 | Semaglutide | sc, 2.4 mg once weekly | 438 | veterans with AUD | placebo | Two-level reduction in the WHO risk drinking level | January 2029 |
| NCT06546384 | Semaglutide | sc, 2.4 mg once weekly | 64 | individuals with obesity and fatty liver disease | nutritional and exercise recommendations | Proportion of patients achieving total alcohol abstinence (measured by negative PEth test) | April 2027 |
| NCT06994338 | Tirzepatide | sc, 5 mg once weekly | 42 | individuals with AUD and overweight or obesity | placebo | Number of heavy drinking days | August 2026 |
| NCT07221214 | Semaglutide | po, 7.0 mg once daily | 200 | individuals living with HIV | placebo | Average drinks/week past 30 days at 3 months | July 2030 |
| NCT06939088 | Tirzepatide | sc, 15 mg once weekly | 108 | individuals with a dual diagnosis of AUD and schizophrenia | placebo | Change in heavy drinking days | December 2028 |
| NCT06727331 | Tirzepatide | sc, 2.5 mg once weekly | 20 | individuals with AUD | placebo | Cue-induced Cravings for Alcohol and Incidence and Severity of Adverse Events | July 2026 |
| NCT07046819 | Tirzepatide | sc, 7.5 mg once weekly | 120 | individuals with AUD and MetALD | placebo | Metabolic improvement from baseline as measured by percentage reduction in body weight and reduction in liver steatosis from baseline as measured by percentage reduction in Fibroscan controlled attenuation parameter (CAP) score. | July 2026 |
| NCT06987513 | Pemvidutide | sc, 2.4 mg once weekly | 100 | individuals with AUD and overweight or obesity | placebo | Change from baseline in the average number of heavy drinking days per week, with a heavy drinking day defined as 5 or more drinks in the day for men and 4 or more drinks in the day for women, using the TLFB method | June 2026 |
| NCT07292519 | Tirzepatide + Take Control CBT Module | sc, 5 mg once weekly | 46 | individuals with co-occurring AUD and overweight/obesity | placebo + Take Control CBT Module | Reduction in heavy drinking days, defined as 4 or more drinks in a day for women and 5 or more drinks in a day for men, using the TLFB method | January 2028 |
| NCT07040592 | Semaglutide | ND | 30 | individuals with AUD living with HIV | No control group | Proportion of participants who complete enrollment and duration of sessions. Number of sessions completed. Adherence to Medication. Safety of study assessed by adverse event reporting | June 2027 |
| NCT07223983 | Semaglutide | sc, 1 mg once weekly | 10 | individuals with AUD after metabolic and bariatric surgery with overweight or obesity | No intervention: wait-list control | Percent weight change. Mean drinks per calendar day to assess alcohol use. Mean drinks per drinking day to assess Alcohol use. Mean number of heavy drinking days to assess Alcohol use. Mean number of drinking vs. abstinent days to assess Alcohol use | October 2026 |
| NCT06817356 | Mazdutide | Administered sc, ND | 300 | individuals with AUD | placebo | Behaviors associated with AUD as assessed TLFB method | August 2026 |
| Drug Class | Substance | GLP-1RA | Key Brain Regions | Behavioral Effects | Mechanistic Insight | Ref. |
|---|---|---|---|---|---|---|
| Psychostimulants | Amphetamine | Ex-4 | NAc | ↓ AMPH-induced CPP. ↓ AMPH-induced locomotor activity | ↓ AMPH-induced accumbal DA release | [112,113,114] |
| Cocaine | Ex-4 | VTA, NAc, LDTg, LS | ↓ SA of cocaine ↓ cocaine-induced locomotor activity ↓ cocaine-induced CPP ↓ cocaine-induced reinforcement ↓ cocaine-seeking | ↑ GABAergic inhibition ↓ cocaine-induced DA release ↑ DAT surface expression and function ↓ synthesis of pro-inflammatory cytokines by suppression of TLR4-dependent neuroimmune signaling | [112,113,114,115,116,117,118,119,120,121,124] | |
| Semaglutide | NAc | ↓reinstatement of cocaine seeking ↓ SA of cocaine | ↓ cocaine-induced DA levels in the NAc shell | [122] | ||
| Opioids | Oxycodone | Ex-4 | NAc | ↓ SA and reinstatement of oxycodone-seeking without diminishing its antinonciceptive effects | Modulation of D1R- and D2R-expressing MSNs | [129] |
| Heroin | Liraglutide | NAc, VTA | ↑ the latency to take heroin ↓ SA of heroin ↓ reinstatement of heroin-seeking | Putative central modulation of relapse-related motivational circuits | [130,131] | |
| Ex-4 | NAc, VTA | ↓ cue-induced heroin seeking ↓ reinstatement of heroin seeking (time-dependent) * | Modulation of orexin signaling in the NAc shell ** | [134] | ||
| Fentanyl | GEP44 | ND | ↓ fentanyl seeking without malaise during abstinence ↓ SA of fentanyl | Dual GLP-1R/Y2R activation | [133] | |
| Ex-4 | ND | ↓ reinstatement of fentanyl seeking ↓ SA of fentanyl | GLP-1R activation | [133] | ||
| Cannabinoids | Cannabis | Semaglutide | ND | ↓ incident and recurrent CUD | CB1–GLP-1 interaction (observational) | [144] |
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Dawid, R.; Joanna, M.; Justyna, M.; Bogdańska, A.; Błażejewska, W.; Szulińska, M. Incretin-Based Therapies: A Novel Pathway in Addiction Treatment. J. Clin. Med. 2026, 15, 1613. https://doi.org/10.3390/jcm15041613
Dawid R, Joanna M, Justyna M, Bogdańska A, Błażejewska W, Szulińska M. Incretin-Based Therapies: A Novel Pathway in Addiction Treatment. Journal of Clinical Medicine. 2026; 15(4):1613. https://doi.org/10.3390/jcm15041613
Chicago/Turabian StyleDawid, Rosiejka, Michałowska Joanna, Marcickiewicz Justyna, Adela Bogdańska, Wiktoria Błażejewska, and Monika Szulińska. 2026. "Incretin-Based Therapies: A Novel Pathway in Addiction Treatment" Journal of Clinical Medicine 15, no. 4: 1613. https://doi.org/10.3390/jcm15041613
APA StyleDawid, R., Joanna, M., Justyna, M., Bogdańska, A., Błażejewska, W., & Szulińska, M. (2026). Incretin-Based Therapies: A Novel Pathway in Addiction Treatment. Journal of Clinical Medicine, 15(4), 1613. https://doi.org/10.3390/jcm15041613

