In Silico Pharmacogenomic Assessment of Glucagon-like Peptide-1 (GLP1) Agonists and the Genetic Addiction Risk Score (GARS) Related Pathways: Implications for Suicidal Ideation and Substance Use Disorder

Alireza Sharafshah; Kai Uwe Lewandrowski; Mark S. Gold; Brian Fuehrlein; John Wesson Ashford; Panayotis K. Thanos; Gene Jack Wang; Colin Hanna; Jean Lud Cadet; Eliot L. Gardner; Jag H. Khalsa; Eric R. Braverman; David Baron; Igor Elman; Catherine A. Dennen; Abdalla Bowirrat; Albert Pinhasov; Edward J. Modestino; Paul R. Carney; Rene Cortese; Rossano Kepler Alvim Fiorelli; Sergio Schmidt; Aryeh R. Pollack; Rajendra D. Badgaiyan; Kenneth Blum

doi:10.2174/011570159X349579241231080602

In Silico Pharmacogenomic Assessment of Glucagon-like Peptide-1 (GLP1) Agonists and the Genetic Addiction Risk Score (GARS) Related Pathways: Implications for Suicidal Ideation and Substance Use Disorder

Alireza Sharafshah
, Kai Uwe Lewandrowski
, Mark S. Gold
, Brian Fuehrlein
, John Wesson Ashford
, Panayotis K. Thanos
, Gene Jack Wang
, Colin Hanna
, Jean Lud Cadet
, Eliot L. Gardner
, Jag H. Khalsa
, Eric R. Braverman
, David Baron
, Igor Elman
, Catherine A. Dennen
, Abdalla Bowirrat
, Albert Pinhasov
, Edward J. Modestino
, Paul R. Carney
, Rene Cortese

Rossano Kepler Alvim Fiorelli, Sergio Schmidt, Aryeh R. Pollack, Rajendra D. Badgaiyan, Kenneth Blum

Research output: Contribution to journal › Article › peer-review

7 Scopus citations

Abstract

Introduction: Glucagon-Like Peptide-1 Receptor (GLP1R) agonists have become widespread anti-obesity/diabetes pharmaceuticals in the United States. Aim: This article aimed to provide our current knowledge on the plausible mechanisms linked to the role of Ozempic (Semaglutide), which is generalized as one of the anti-addiction compounds. Methods: The effects of GLP1R agonists in Alcohol Use Disorder (AUD) and substance use disorder (SUD) are mediated, in part, through the downregulation of dopamine signaling. We posit that while GLP1R agonism could offer therapeutic advantages in hyperdopaminergia, it may be detrimental in patients with hypodopaminergia, potentially leading to long-term induction of Suicidal Ideation (SI). The alleged posit of GLP1 agonists to induce dopamine homeostasis is incorrect. This study refined 31 genes based on the targets of Ozempic, GLP1R, and related enzymes for SI and 10 genes of the Genetic Addiction Risk Score (GARS) test. STRING-MODEL refined 29 genes, and further primary analyses indicated associations of GLP1R with DRD3, BDNF, CREB1, CRH, IL6, and DPP4. Results: In-depth silico enrichment analysis revealed an association between candidate genes and depressive phenotypes linked with dopaminergic signaling. Finally, through primary and in-depth silico analyses, we demonstrated multiple findings supporting that GLP1R agonists can induce depression phenotypes. Conclusion: Our findings suggest that associated polymorphisms seem to have overlapping effects with addictive behaviors of Reward Deficiency Syndrome (RDS) and dopamine regulation. Consequently, GLP1R agonists may represent a double-edged sword, potentially triggering both anti-addictive effects and SI by exacerbating depressive phenotypes. Thus, we encourage the scientific community to perform further empirical clinical studies to confirm this proposed pathway.

Original language	English
Pages (from-to)	974-995
Number of pages	22
Journal	Current Neuropharmacology
Volume	23
Issue number	8
DOIs	https://doi.org/10.2174/011570159X349579241231080602
State	Published - 2025

Keywords

GLP1
Ozempic
dopamine homeostasis
in-depth in silico
substance use disorder
suicide ideation

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10.2174/011570159X349579241231080602

Cite this

Sharafshah, A., Lewandrowski, K. U., Gold, M. S., Fuehrlein, B., Ashford, J. W., Thanos, P. K., Wang, G. J., Hanna, C., Cadet, J. L., Gardner, E. L., Khalsa, J. H., Braverman, E. R., Baron, D., Elman, I., Dennen, C. A., Bowirrat, A., Pinhasov, A., Modestino, E. J., Carney, P. R., ... Blum, K. (2025). In Silico Pharmacogenomic Assessment of Glucagon-like Peptide-1 (GLP1) Agonists and the Genetic Addiction Risk Score (GARS) Related Pathways: Implications for Suicidal Ideation and Substance Use Disorder. Current Neuropharmacology, 23(8), 974-995. https://doi.org/10.2174/011570159X349579241231080602

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title = "In Silico Pharmacogenomic Assessment of Glucagon-like Peptide-1 (GLP1) Agonists and the Genetic Addiction Risk Score (GARS) Related Pathways: Implications for Suicidal Ideation and Substance Use Disorder",

abstract = "Introduction: Glucagon-Like Peptide-1 Receptor (GLP1R) agonists have become widespread anti-obesity/diabetes pharmaceuticals in the United States. Aim: This article aimed to provide our current knowledge on the plausible mechanisms linked to the role of Ozempic (Semaglutide), which is generalized as one of the anti-addiction compounds. Methods: The effects of GLP1R agonists in Alcohol Use Disorder (AUD) and substance use disorder (SUD) are mediated, in part, through the downregulation of dopamine signaling. We posit that while GLP1R agonism could offer therapeutic advantages in hyperdopaminergia, it may be detrimental in patients with hypodopaminergia, potentially leading to long-term induction of Suicidal Ideation (SI). The alleged posit of GLP1 agonists to induce dopamine homeostasis is incorrect. This study refined 31 genes based on the targets of Ozempic, GLP1R, and related enzymes for SI and 10 genes of the Genetic Addiction Risk Score (GARS) test. STRING-MODEL refined 29 genes, and further primary analyses indicated associations of GLP1R with DRD3, BDNF, CREB1, CRH, IL6, and DPP4. Results: In-depth silico enrichment analysis revealed an association between candidate genes and depressive phenotypes linked with dopaminergic signaling. Finally, through primary and in-depth silico analyses, we demonstrated multiple findings supporting that GLP1R agonists can induce depression phenotypes. Conclusion: Our findings suggest that associated polymorphisms seem to have overlapping effects with addictive behaviors of Reward Deficiency Syndrome (RDS) and dopamine regulation. Consequently, GLP1R agonists may represent a double-edged sword, potentially triggering both anti-addictive effects and SI by exacerbating depressive phenotypes. Thus, we encourage the scientific community to perform further empirical clinical studies to confirm this proposed pathway.",

keywords = "GLP1, Ozempic, dopamine homeostasis, in-depth in silico, substance use disorder, suicide ideation",

author = "Alireza Sharafshah and Lewandrowski, \{Kai Uwe\} and Gold, \{Mark S.\} and Brian Fuehrlein and Ashford, \{John Wesson\} and Thanos, \{Panayotis K.\} and Wang, \{Gene Jack\} and Colin Hanna and Cadet, \{Jean Lud\} and Gardner, \{Eliot L.\} and Khalsa, \{Jag H.\} and Braverman, \{Eric R.\} and David Baron and Igor Elman and Dennen, \{Catherine A.\} and Abdalla Bowirrat and Albert Pinhasov and Modestino, \{Edward J.\} and Carney, \{Paul R.\} and Rene Cortese and Fiorelli, \{Rossano Kepler Alvim\} and Sergio Schmidt and Pollack, \{Aryeh R.\} and Badgaiyan, \{Rajendra D.\} and Kenneth Blum",

note = "Publisher Copyright: {\textcopyright} 2025 Bentham Science Publishers.",

year = "2025",

doi = "10.2174/011570159X349579241231080602",

language = "אנגלית",

volume = "23",

pages = "974--995",

journal = "Current Neuropharmacology",

issn = "1570-159X",

publisher = "Bentham Science Publishers",

number = "8",

}

Sharafshah, A, Lewandrowski, KU, Gold, MS, Fuehrlein, B, Ashford, JW, Thanos, PK, Wang, GJ, Hanna, C, Cadet, JL, Gardner, EL, Khalsa, JH, Braverman, ER, Baron, D, Elman, I, Dennen, CA, Bowirrat, A , Pinhasov, A, Modestino, EJ, Carney, PR, Cortese, R, Fiorelli, RKA, Schmidt, S, Pollack, AR, Badgaiyan, RD & Blum, K 2025, 'In Silico Pharmacogenomic Assessment of Glucagon-like Peptide-1 (GLP1) Agonists and the Genetic Addiction Risk Score (GARS) Related Pathways: Implications for Suicidal Ideation and Substance Use Disorder', Current Neuropharmacology, vol. 23, no. 8, pp. 974-995. https://doi.org/10.2174/011570159X349579241231080602

In Silico Pharmacogenomic Assessment of Glucagon-like Peptide-1 (GLP1) Agonists and the Genetic Addiction Risk Score (GARS) Related Pathways: Implications for Suicidal Ideation and Substance Use Disorder. / Sharafshah, Alireza; Lewandrowski, Kai Uwe; Gold, Mark S. et al.
In: Current Neuropharmacology, Vol. 23, No. 8, 2025, p. 974-995.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - In Silico Pharmacogenomic Assessment of Glucagon-like Peptide-1 (GLP1) Agonists and the Genetic Addiction Risk Score (GARS) Related Pathways

T2 - Implications for Suicidal Ideation and Substance Use Disorder

AU - Sharafshah, Alireza

AU - Lewandrowski, Kai Uwe

AU - Gold, Mark S.

AU - Fuehrlein, Brian

AU - Ashford, John Wesson

AU - Thanos, Panayotis K.

AU - Wang, Gene Jack

AU - Hanna, Colin

AU - Cadet, Jean Lud

AU - Gardner, Eliot L.

AU - Khalsa, Jag H.

AU - Braverman, Eric R.

AU - Baron, David

AU - Elman, Igor

AU - Dennen, Catherine A.

AU - Bowirrat, Abdalla

AU - Pinhasov, Albert

AU - Modestino, Edward J.

AU - Carney, Paul R.

AU - Cortese, Rene

AU - Fiorelli, Rossano Kepler Alvim

AU - Schmidt, Sergio

AU - Pollack, Aryeh R.

AU - Badgaiyan, Rajendra D.

AU - Blum, Kenneth

PY - 2025

Y1 - 2025

N2 - Introduction: Glucagon-Like Peptide-1 Receptor (GLP1R) agonists have become widespread anti-obesity/diabetes pharmaceuticals in the United States. Aim: This article aimed to provide our current knowledge on the plausible mechanisms linked to the role of Ozempic (Semaglutide), which is generalized as one of the anti-addiction compounds. Methods: The effects of GLP1R agonists in Alcohol Use Disorder (AUD) and substance use disorder (SUD) are mediated, in part, through the downregulation of dopamine signaling. We posit that while GLP1R agonism could offer therapeutic advantages in hyperdopaminergia, it may be detrimental in patients with hypodopaminergia, potentially leading to long-term induction of Suicidal Ideation (SI). The alleged posit of GLP1 agonists to induce dopamine homeostasis is incorrect. This study refined 31 genes based on the targets of Ozempic, GLP1R, and related enzymes for SI and 10 genes of the Genetic Addiction Risk Score (GARS) test. STRING-MODEL refined 29 genes, and further primary analyses indicated associations of GLP1R with DRD3, BDNF, CREB1, CRH, IL6, and DPP4. Results: In-depth silico enrichment analysis revealed an association between candidate genes and depressive phenotypes linked with dopaminergic signaling. Finally, through primary and in-depth silico analyses, we demonstrated multiple findings supporting that GLP1R agonists can induce depression phenotypes. Conclusion: Our findings suggest that associated polymorphisms seem to have overlapping effects with addictive behaviors of Reward Deficiency Syndrome (RDS) and dopamine regulation. Consequently, GLP1R agonists may represent a double-edged sword, potentially triggering both anti-addictive effects and SI by exacerbating depressive phenotypes. Thus, we encourage the scientific community to perform further empirical clinical studies to confirm this proposed pathway.

AB - Introduction: Glucagon-Like Peptide-1 Receptor (GLP1R) agonists have become widespread anti-obesity/diabetes pharmaceuticals in the United States. Aim: This article aimed to provide our current knowledge on the plausible mechanisms linked to the role of Ozempic (Semaglutide), which is generalized as one of the anti-addiction compounds. Methods: The effects of GLP1R agonists in Alcohol Use Disorder (AUD) and substance use disorder (SUD) are mediated, in part, through the downregulation of dopamine signaling. We posit that while GLP1R agonism could offer therapeutic advantages in hyperdopaminergia, it may be detrimental in patients with hypodopaminergia, potentially leading to long-term induction of Suicidal Ideation (SI). The alleged posit of GLP1 agonists to induce dopamine homeostasis is incorrect. This study refined 31 genes based on the targets of Ozempic, GLP1R, and related enzymes for SI and 10 genes of the Genetic Addiction Risk Score (GARS) test. STRING-MODEL refined 29 genes, and further primary analyses indicated associations of GLP1R with DRD3, BDNF, CREB1, CRH, IL6, and DPP4. Results: In-depth silico enrichment analysis revealed an association between candidate genes and depressive phenotypes linked with dopaminergic signaling. Finally, through primary and in-depth silico analyses, we demonstrated multiple findings supporting that GLP1R agonists can induce depression phenotypes. Conclusion: Our findings suggest that associated polymorphisms seem to have overlapping effects with addictive behaviors of Reward Deficiency Syndrome (RDS) and dopamine regulation. Consequently, GLP1R agonists may represent a double-edged sword, potentially triggering both anti-addictive effects and SI by exacerbating depressive phenotypes. Thus, we encourage the scientific community to perform further empirical clinical studies to confirm this proposed pathway.

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KW - Ozempic

KW - dopamine homeostasis

KW - in-depth in silico

KW - substance use disorder

KW - suicide ideation

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Sharafshah A, Lewandrowski KU, Gold MS, Fuehrlein B, Ashford JW, Thanos PK et al. In Silico Pharmacogenomic Assessment of Glucagon-like Peptide-1 (GLP1) Agonists and the Genetic Addiction Risk Score (GARS) Related Pathways: Implications for Suicidal Ideation and Substance Use Disorder. Current Neuropharmacology. 2025;23(8):974-995. doi: 10.2174/011570159X349579241231080602

In Silico Pharmacogenomic Assessment of Glucagon-like Peptide-1 (GLP1) Agonists and the Genetic Addiction Risk Score (GARS) Related Pathways: Implications for Suicidal Ideation and Substance Use Disorder

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