Cannabinoid receptor 1 ligands: Biased signaling mechanisms driving functionally selective drug discovery

Lei Tian¹, Taotao Qiang², Sundian Liu³, Boxin Zhang³, Yunfei Zhang³, Bingxing Zhang³, Jinrong Hu³, Jiayun Zhang³, Qi Lu³, Changhua Ke³, Juan Xia⁴, Chengyuan Liang⁵

Affiliations

¹ College of Bioresources Chemical and Materials Engineering, Shaanxi University of Science & Technology, Xi'an 710021, China; Xi'an Key Laboratory for Antiviral and Antimicrobial-Resistant Bacteria Therapeutics Research, Shaanxi University of Science & Technology, Xi'an 710021, China.
² College of Bioresources Chemical and Materials Engineering, Shaanxi University of Science & Technology, Xi'an 710021, China.
³ Xi'an Key Laboratory for Antiviral and Antimicrobial-Resistant Bacteria Therapeutics Research, Shaanxi University of Science & Technology, Xi'an 710021, China; School of Biological and Pharmaceutical Sciences, Shaanxi University of Science & Technology, Xi'an 710021, China.
⁴ Zhanjiang Institute of Clinical Medicine, Central People's Hospital of Zhanjiang, Zhanjiang 524045, China.
⁵ Xi'an Key Laboratory for Antiviral and Antimicrobial-Resistant Bacteria Therapeutics Research, Shaanxi University of Science & Technology, Xi'an 710021, China; School of Biological and Pharmaceutical Sciences, Shaanxi University of Science & Technology, Xi'an 710021, China. Electronic address: chengyuanliang@gmail.com.

PMID: 39828030
DOI: 10.1016/j.pharmthera.2025.108795

Review

Cannabinoid receptor 1 ligands: Biased signaling mechanisms driving functionally selective drug discovery

Lei Tian et al. Pharmacol Ther. 2025 Mar.

. 2025 Mar:267:108795.

doi: 10.1016/j.pharmthera.2025.108795. Epub 2025 Jan 17.

Authors

Lei Tian¹, Taotao Qiang², Sundian Liu³, Boxin Zhang³, Yunfei Zhang³, Bingxing Zhang³, Jinrong Hu³, Jiayun Zhang³, Qi Lu³, Changhua Ke³, Juan Xia⁴, Chengyuan Liang⁵

Affiliations

¹ College of Bioresources Chemical and Materials Engineering, Shaanxi University of Science & Technology, Xi'an 710021, China; Xi'an Key Laboratory for Antiviral and Antimicrobial-Resistant Bacteria Therapeutics Research, Shaanxi University of Science & Technology, Xi'an 710021, China.
² College of Bioresources Chemical and Materials Engineering, Shaanxi University of Science & Technology, Xi'an 710021, China.
³ Xi'an Key Laboratory for Antiviral and Antimicrobial-Resistant Bacteria Therapeutics Research, Shaanxi University of Science & Technology, Xi'an 710021, China; School of Biological and Pharmaceutical Sciences, Shaanxi University of Science & Technology, Xi'an 710021, China.
⁴ Zhanjiang Institute of Clinical Medicine, Central People's Hospital of Zhanjiang, Zhanjiang 524045, China.
⁵ Xi'an Key Laboratory for Antiviral and Antimicrobial-Resistant Bacteria Therapeutics Research, Shaanxi University of Science & Technology, Xi'an 710021, China; School of Biological and Pharmaceutical Sciences, Shaanxi University of Science & Technology, Xi'an 710021, China. Electronic address: chengyuanliang@gmail.com.

PMID: 39828030
DOI: 10.1016/j.pharmthera.2025.108795

Abstract

G protein-coupled receptors (GPCRs) adopt conformational states that activate or inhibit distinct signaling pathways, including those mediated by G proteins or β-arrestins. Biased signaling through GPCRs may offer a promising strategy to enhance therapeutic efficacy while reducing adverse effects. Cannabinoid receptor 1 (CB1), a key GPCR in the endocannabinoid system, presents therapeutic potential for conditions such as pain, anxiety, cognitive impairment, psychiatric disorders, and metabolic diseases. This review examines the structural conformations of CB1 coupling to different signaling pathways and explores the mechanisms underlying biased signaling, which are critical for the design of functionally selective ligands. We discuss the structure-function relationships of endogenous cannabinoids (eCBs), phytocannabinoids, and synthetic cannabinoid ligands with biased properties. Challenges such as the complexity of ligand bias screening, the limited availability of distinctly biased ligands, and the variability in receptor signaling profiles in vivo have hindered clinical progress. Although the therapeutic potential of biased ligands in various clinical conditions remains in its infancy, retrospective identification of such molecules provides a strong foundation for further development. Recent advances in CB1 crystallography, particularly insights into its conformations with G proteins and β-arrestins, now offer a framework for structure-based drug design. While there is still a long way to go before biased CB1 ligands can be widely used in clinical practice, ongoing multidisciplinary research shows promise for achieving functional selectivity in targeting specific pathways. These progress could lead to the development of safer and more effective cannabinoid-based therapies in the future.

Keywords: Biased ligand design; Biased signaling; Cannabinoid receptor 1 (CB1); Crystal structure; Drug discovery; Functional selectivity; G protein-coupled receptors (GPCRs).

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Conflict of interest statement

Declaration of competing interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests. Chengyuan Liang reports financial support was provided by National Natural Science Foundation of China. Taotao Qiang reports financial support was provided by National Natural Science Foundation of China. Juan Xia reports financial support was provided by National Natural Science Foundation of China. Chengyuan Liang reports financial support was provided by Natural Science Foundation of Shaanxi Province. Chengyuan Liang reports financial support was provided by Scientific Research Fund of Shaanxi Provincial Education Department. Chengyuan Liang reports financial support was provided by Shaanxi Administration of Traditional Chinese Medicine. Chengyuan Liang reports financial support was provided by Shaanxi Province Department of Science and Technology. Taotao Qiang reports financial support was provided by Shaanxi Province Technology Innovation Guidance Project. Chengyuan Liang reports financial support was provided by Xi'an Science and Technology Bureau. Taotao Qiang reports financial support was provided by Qin Chuangyuan Team Construction Project of Shaanxi Science and Technology Department. Chengyuan Liang reports financial support was provided by Xi'an Science and Technology Bureau. Chengyuan Liang reports financial support was provided by Xianyang Science and Technology Bureau. Chengyuan Liang reports financial support was provided by Research Center for the Development of Therapeutic Drugs for Serious Infectious Diseases in Shaanxi Province's Universities and Colleges. Chengyuan Liang reports financial support was provided by Xi'an International Science and Technology Cooperation Base for Anti-Infective Drug Research and Development. Chengyuan Liang reports financial support was provided by Xi'an Engineering Research Center for Development and Application of New Veterinary and Poultry Antibiotics. Taotao Qiang reports financial support was provided by Youth Innovation Team of Shaanxi Universities. If there are other authors, they declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper.

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Cannabinoid receptor 1 ligands: Biased signaling mechanisms driving functionally selective drug discovery

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Cannabinoid receptor 1 ligands: Biased signaling mechanisms driving functionally selective drug discovery

Authors

Affiliations

Abstract

Conflict of interest statement

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