A cryptic pocket in CB1 drives peripheral and functional selectivity

Vipin Ashok Rangari; Evan S. O’Brien; Alexander S. Powers; Richard A. Slivicki; Zachariah Bertels; Kevin Appourchaux; Deniz Aydin; Nokomis Ramos-Gonzalez; Juliet Mwirigi; Li Lin; Elizaveta Mangutov; Briana L. Sobecks; Yaseen Awad-Agbaria; Manoj B. Uphade; Jhoan Aguilar; Teja Nikhil Peddada; Yuki Shiimura; Xi Ping Huang; Jakayla Folarin-Hines; Maria Payne; Anirudh Kalathil; Balazs R. Varga; Brian K. Kobilka; Amynah A. Pradhan; Michael D. Cameron; Kaavya Krishna Kumar; Ron O. Dror; Robert W. Gereau; Susruta Majumdar

doi:10.1038/s41586-025-08618-7

A cryptic pocket in CB1 drives peripheral and functional selectivity

Vipin Ashok Rangari, Evan S. O’Brien, Alexander S. Powers, Richard A. Slivicki, Zachariah Bertels, Kevin Appourchaux, Deniz Aydin, Nokomis Ramos-Gonzalez, Juliet Mwirigi, Li Lin, Elizaveta Mangutov, Briana L. Sobecks, Yaseen Awad-Agbaria, Manoj B. Uphade, Jhoan Aguilar, Teja Nikhil Peddada, Yuki Shiimura, Xi Ping Huang, Jakayla Folarin-Hines, Maria PayneAnirudh Kalathil, Balazs R. Varga, Brian K. Kobilka, Amynah A. Pradhan, Michael D. Cameron, Kaavya Krishna Kumar, Ron O. Dror, Robert W. Gereau, Susruta Majumdar

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

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Abstract

The current opioid overdose epidemic highlights the urgent need to develop safer and more effective treatments for chronic pain¹. Cannabinoid receptor type 1 (CB1) is a promising non-opioid target for pain relief, but its clinical use has been limited by centrally mediated psychoactivity and tolerance. We overcame both issues by designing peripherally restricted CB1 agonists that minimize arrestin recruitment. We achieved these goals by computationally designing positively charged derivatives of the potent CB1 agonist MDMB-Fubinaca². We designed these ligands to occupy a cryptic pocket identified through molecular dynamics simulations—an extended binding pocket that opens rarely and leads to the conserved signalling residue D^2.50 (ref. ³). We used structure determination, pharmacological assays and molecular dynamics simulations to verify the binding modes of these ligands and to determine the molecular mechanism by which they achieve this dampening of arrestin recruitment. Our lead ligand, VIP36, is highly peripherally restricted and demonstrates notable efficacy in three mouse pain models, with 100-fold dose separation between analgesic efficacy and centrally mediated side effects. VIP36 exerts analgesic efficacy through peripheral CB1 receptors and shows limited analgesic tolerance. These results show how targeting a cryptic pocket in a G-protein-coupled receptor can lead to enhanced peripheral selectivity, biased signalling, desired in vivo pharmacology and reduced adverse effects. This has substantial implications for chronic pain treatment but could also revolutionize the design of drugs targeting other G-protein-coupled receptors.

Original language	English
Article number	107847
Pages (from-to)	265-273
Number of pages	9
Journal	Nature
Volume	640
Issue number	8057
DOIs	https://doi.org/10.1038/s41586-025-08618-7
State	Published - Apr 3 2025

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Rangari, V. A., O’Brien, E. S., Powers, A. S., Slivicki, R. A., Bertels, Z., Appourchaux, K., Aydin, D., Ramos-Gonzalez, N., Mwirigi, J., Lin, L., Mangutov, E., Sobecks, B. L., Awad-Agbaria, Y., Uphade, M. B., Aguilar, J., Peddada, T. N., Shiimura, Y., Huang, X. P., Folarin-Hines, J., ... Majumdar, S. (2025). A cryptic pocket in CB1 drives peripheral and functional selectivity. Nature, 640(8057), 265-273. Article 107847. https://doi.org/10.1038/s41586-025-08618-7

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title = "A cryptic pocket in CB1 drives peripheral and functional selectivity",

abstract = "The current opioid overdose epidemic highlights the urgent need to develop safer and more effective treatments for chronic pain1. Cannabinoid receptor type 1 (CB1) is a promising non-opioid target for pain relief, but its clinical use has been limited by centrally mediated psychoactivity and tolerance. We overcame both issues by designing peripherally restricted CB1 agonists that minimize arrestin recruitment. We achieved these goals by computationally designing positively charged derivatives of the potent CB1 agonist MDMB-Fubinaca2. We designed these ligands to occupy a cryptic pocket identified through molecular dynamics simulations—an extended binding pocket that opens rarely and leads to the conserved signalling residue D2.50 (ref. 3). We used structure determination, pharmacological assays and molecular dynamics simulations to verify the binding modes of these ligands and to determine the molecular mechanism by which they achieve this dampening of arrestin recruitment. Our lead ligand, VIP36, is highly peripherally restricted and demonstrates notable efficacy in three mouse pain models, with 100-fold dose separation between analgesic efficacy and centrally mediated side effects. VIP36 exerts analgesic efficacy through peripheral CB1 receptors and shows limited analgesic tolerance. These results show how targeting a cryptic pocket in a G-protein-coupled receptor can lead to enhanced peripheral selectivity, biased signalling, desired in vivo pharmacology and reduced adverse effects. This has substantial implications for chronic pain treatment but could also revolutionize the design of drugs targeting other G-protein-coupled receptors.",

author = "Rangari, {Vipin Ashok} and O{\textquoteright}Brien, {Evan S.} and Powers, {Alexander S.} and Slivicki, {Richard A.} and Zachariah Bertels and Kevin Appourchaux and Deniz Aydin and Nokomis Ramos-Gonzalez and Juliet Mwirigi and Li Lin and Elizaveta Mangutov and Sobecks, {Briana L.} and Yaseen Awad-Agbaria and Uphade, {Manoj B.} and Jhoan Aguilar and Peddada, {Teja Nikhil} and Yuki Shiimura and Huang, {Xi Ping} and Jakayla Folarin-Hines and Maria Payne and Anirudh Kalathil and Varga, {Balazs R.} and Kobilka, {Brian K.} and Pradhan, {Amynah A.} and Cameron, {Michael D.} and Kumar, {Kaavya Krishna} and Dror, {Ron O.} and Gereau, {Robert W.} and Susruta Majumdar",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature Limited 2025.",

year = "2025",

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doi = "10.1038/s41586-025-08618-7",

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Rangari, VA, O’Brien, ES, Powers, AS, Slivicki, RA, Bertels, Z, Appourchaux, K, Aydin, D, Ramos-Gonzalez, N, Mwirigi, J, Lin, L, Mangutov, E, Sobecks, BL, Awad-Agbaria, Y, Uphade, MB, Aguilar, J, Peddada, TN, Shiimura, Y, Huang, XP, Folarin-Hines, J, Payne, M, Kalathil, A, Varga, BR, Kobilka, BK, Pradhan, AA, Cameron, MD, Kumar, KK, Dror, RO, Gereau, RW & Majumdar, S 2025, 'A cryptic pocket in CB1 drives peripheral and functional selectivity', Nature, vol. 640, no. 8057, 107847, pp. 265-273. https://doi.org/10.1038/s41586-025-08618-7

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T1 - A cryptic pocket in CB1 drives peripheral and functional selectivity

AU - Rangari, Vipin Ashok

AU - O’Brien, Evan S.

AU - Powers, Alexander S.

AU - Slivicki, Richard A.

AU - Bertels, Zachariah

AU - Appourchaux, Kevin

AU - Aydin, Deniz

AU - Ramos-Gonzalez, Nokomis

AU - Mwirigi, Juliet

AU - Lin, Li

AU - Mangutov, Elizaveta

AU - Sobecks, Briana L.

AU - Awad-Agbaria, Yaseen

AU - Uphade, Manoj B.

AU - Aguilar, Jhoan

AU - Peddada, Teja Nikhil

AU - Shiimura, Yuki

AU - Huang, Xi Ping

AU - Folarin-Hines, Jakayla

AU - Payne, Maria

AU - Kalathil, Anirudh

AU - Varga, Balazs R.

AU - Kobilka, Brian K.

AU - Pradhan, Amynah A.

AU - Cameron, Michael D.

AU - Kumar, Kaavya Krishna

AU - Dror, Ron O.

AU - Gereau, Robert W.

AU - Majumdar, Susruta

PY - 2025/4/3

Y1 - 2025/4/3

N2 - The current opioid overdose epidemic highlights the urgent need to develop safer and more effective treatments for chronic pain1. Cannabinoid receptor type 1 (CB1) is a promising non-opioid target for pain relief, but its clinical use has been limited by centrally mediated psychoactivity and tolerance. We overcame both issues by designing peripherally restricted CB1 agonists that minimize arrestin recruitment. We achieved these goals by computationally designing positively charged derivatives of the potent CB1 agonist MDMB-Fubinaca2. We designed these ligands to occupy a cryptic pocket identified through molecular dynamics simulations—an extended binding pocket that opens rarely and leads to the conserved signalling residue D2.50 (ref. 3). We used structure determination, pharmacological assays and molecular dynamics simulations to verify the binding modes of these ligands and to determine the molecular mechanism by which they achieve this dampening of arrestin recruitment. Our lead ligand, VIP36, is highly peripherally restricted and demonstrates notable efficacy in three mouse pain models, with 100-fold dose separation between analgesic efficacy and centrally mediated side effects. VIP36 exerts analgesic efficacy through peripheral CB1 receptors and shows limited analgesic tolerance. These results show how targeting a cryptic pocket in a G-protein-coupled receptor can lead to enhanced peripheral selectivity, biased signalling, desired in vivo pharmacology and reduced adverse effects. This has substantial implications for chronic pain treatment but could also revolutionize the design of drugs targeting other G-protein-coupled receptors.

AB - The current opioid overdose epidemic highlights the urgent need to develop safer and more effective treatments for chronic pain1. Cannabinoid receptor type 1 (CB1) is a promising non-opioid target for pain relief, but its clinical use has been limited by centrally mediated psychoactivity and tolerance. We overcame both issues by designing peripherally restricted CB1 agonists that minimize arrestin recruitment. We achieved these goals by computationally designing positively charged derivatives of the potent CB1 agonist MDMB-Fubinaca2. We designed these ligands to occupy a cryptic pocket identified through molecular dynamics simulations—an extended binding pocket that opens rarely and leads to the conserved signalling residue D2.50 (ref. 3). We used structure determination, pharmacological assays and molecular dynamics simulations to verify the binding modes of these ligands and to determine the molecular mechanism by which they achieve this dampening of arrestin recruitment. Our lead ligand, VIP36, is highly peripherally restricted and demonstrates notable efficacy in three mouse pain models, with 100-fold dose separation between analgesic efficacy and centrally mediated side effects. VIP36 exerts analgesic efficacy through peripheral CB1 receptors and shows limited analgesic tolerance. These results show how targeting a cryptic pocket in a G-protein-coupled receptor can lead to enhanced peripheral selectivity, biased signalling, desired in vivo pharmacology and reduced adverse effects. This has substantial implications for chronic pain treatment but could also revolutionize the design of drugs targeting other G-protein-coupled receptors.

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A cryptic pocket in CB1 drives peripheral and functional selectivity

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