Magic mushroom extracts in lipid membranes

Teresa Quynh Tram Nguyen; Frederik Wendelboe Lund; Ali Asghar Hakami Zanjani; Himanshu Khandelia

doi:10.1016/j.bbamem.2022.183957

Magic mushroom extracts in lipid membranes

Teresa Quynh Tram Nguyen, Frederik Wendelboe Lund, Ali Asghar Hakami Zanjani^*, Himanshu Khandelia

^*Corresponding author for this work

University of Southern Denmark

Research output: Contribution to journal › Journal article › Research › peer-review

49 Downloads (Pure)

Abstract

The active hallucinogen of magic mushrooms, psilocin, is being repurposed to treat nicotine addiction and treatment-resistant depression. Psilocin belongs to the tryptamine class of psychedelic compounds which include the hormone serotonin. It is believed that psilocin exerts its effect by binding to the serotonin 5-HT_2A receptor. However, recent in-vivo evidence suggests that psilocin may employ a different mechanism to exert its effects. Membrane-mediated receptor desensitization of neurotransmitter receptors is one such mechanism. We compare the impact of the neutral and charged versions of psilocin and serotonin on the properties of zwitterionic and anionic lipid membranes using molecular dynamics simulations and calorimetry. Both compounds partition to the lipid interface and induce membrane thinning. The tertiary amine in psilocin, as opposed to the primary amine in serotonin, limits psilocin's impact on the membrane although more psilocin partitions into the membrane than serotonin. Calorimetry corroborates that both compounds induce a classical melting point depression like anesthetics do. Our results also lend support to a membrane-mediated receptor-binding mechanism for both psilocin and serotonin and provide physical insights into subtle chemical changes that can alter the membrane-binding of psychedelic compounds.

Original language	English
Article number	183957
Journal	Biochimica et Biophysica Acta - Biomembranes
Volume	1864
Issue number	9
ISSN	0005-2736
DOIs	https://doi.org/10.1016/j.bbamem.2022.183957
Publication status	Published - 1. Sep 2022

Keywords

Lipid-drug interactions
Magic mushrooms
Molecular dynamics (MD) simulations
Psilocin
Psychedelic drugs
Serotonin

Documents & Links

10.1016/j.bbamem.2022.183957Licence: CC BY

Open access versionFinal published version, 2.3 MBLicence: CC BY

Cite this

@article{e02a74b750d04f6ea05d6891967a175f,

title = "Magic mushroom extracts in lipid membranes",

abstract = "The active hallucinogen of magic mushrooms, psilocin, is being repurposed to treat nicotine addiction and treatment-resistant depression. Psilocin belongs to the tryptamine class of psychedelic compounds which include the hormone serotonin. It is believed that psilocin exerts its effect by binding to the serotonin 5-HT2A receptor. However, recent in-vivo evidence suggests that psilocin may employ a different mechanism to exert its effects. Membrane-mediated receptor desensitization of neurotransmitter receptors is one such mechanism. We compare the impact of the neutral and charged versions of psilocin and serotonin on the properties of zwitterionic and anionic lipid membranes using molecular dynamics simulations and calorimetry. Both compounds partition to the lipid interface and induce membrane thinning. The tertiary amine in psilocin, as opposed to the primary amine in serotonin, limits psilocin's impact on the membrane although more psilocin partitions into the membrane than serotonin. Calorimetry corroborates that both compounds induce a classical melting point depression like anesthetics do. Our results also lend support to a membrane-mediated receptor-binding mechanism for both psilocin and serotonin and provide physical insights into subtle chemical changes that can alter the membrane-binding of psychedelic compounds.",

keywords = "Lipid-drug interactions, Magic mushrooms, Molecular dynamics (MD) simulations, Psilocin, Psychedelic drugs, Serotonin",

author = "Nguyen, {Teresa Quynh Tram} and Lund, {Frederik Wendelboe} and Zanjani, {Ali Asghar Hakami} and Himanshu Khandelia",

note = "Funding Information: The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Himanshu khandelia reports financial support was provided by Lundbeck Foundation. Ali Asghar Hakami Zanjani reports financial support was provided by Novo Nordisk Foundation. Funding Information: We acknowledge PRACE for awarding us access to Marconi supercomputer at CINECA, Italy. HK is funded by a Lundbeckfonden Ascending Investigator grant number R344-2020-1023 . AAHZ is funded by a Novo Nordisk Foundation Synergy grant # NNF18OC0034936 . We thank Peter Reinholdt for help with force field optimization. Funding Information: We acknowledge PRACE for awarding us access to Marconi supercomputer at CINECA, Italy. HK is funded by a Lundbeckfonden Ascending Investigator grant number R344-2020-1023. AAHZ is funded by a Novo Nordisk Foundation Synergy grant # NNF18OC0034936. We thank Peter Reinholdt for help with force field optimization. Publisher Copyright: {\textcopyright} 2022 The Authors",

year = "2022",

month = sep,

day = "1",

doi = "10.1016/j.bbamem.2022.183957",

language = "English",

volume = "1864",

journal = "BBA Biomembranes",

issn = "0005-2736",

publisher = "Elsevier",

number = "9",

}

TY - JOUR

T1 - Magic mushroom extracts in lipid membranes

AU - Nguyen, Teresa Quynh Tram

AU - Lund, Frederik Wendelboe

AU - Zanjani, Ali Asghar Hakami

AU - Khandelia, Himanshu

N1 - Funding Information: The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Himanshu khandelia reports financial support was provided by Lundbeck Foundation. Ali Asghar Hakami Zanjani reports financial support was provided by Novo Nordisk Foundation. Funding Information: We acknowledge PRACE for awarding us access to Marconi supercomputer at CINECA, Italy. HK is funded by a Lundbeckfonden Ascending Investigator grant number R344-2020-1023 . AAHZ is funded by a Novo Nordisk Foundation Synergy grant # NNF18OC0034936 . We thank Peter Reinholdt for help with force field optimization. Funding Information: We acknowledge PRACE for awarding us access to Marconi supercomputer at CINECA, Italy. HK is funded by a Lundbeckfonden Ascending Investigator grant number R344-2020-1023. AAHZ is funded by a Novo Nordisk Foundation Synergy grant # NNF18OC0034936. We thank Peter Reinholdt for help with force field optimization. Publisher Copyright: © 2022 The Authors

PY - 2022/9/1

Y1 - 2022/9/1

N2 - The active hallucinogen of magic mushrooms, psilocin, is being repurposed to treat nicotine addiction and treatment-resistant depression. Psilocin belongs to the tryptamine class of psychedelic compounds which include the hormone serotonin. It is believed that psilocin exerts its effect by binding to the serotonin 5-HT2A receptor. However, recent in-vivo evidence suggests that psilocin may employ a different mechanism to exert its effects. Membrane-mediated receptor desensitization of neurotransmitter receptors is one such mechanism. We compare the impact of the neutral and charged versions of psilocin and serotonin on the properties of zwitterionic and anionic lipid membranes using molecular dynamics simulations and calorimetry. Both compounds partition to the lipid interface and induce membrane thinning. The tertiary amine in psilocin, as opposed to the primary amine in serotonin, limits psilocin's impact on the membrane although more psilocin partitions into the membrane than serotonin. Calorimetry corroborates that both compounds induce a classical melting point depression like anesthetics do. Our results also lend support to a membrane-mediated receptor-binding mechanism for both psilocin and serotonin and provide physical insights into subtle chemical changes that can alter the membrane-binding of psychedelic compounds.

AB - The active hallucinogen of magic mushrooms, psilocin, is being repurposed to treat nicotine addiction and treatment-resistant depression. Psilocin belongs to the tryptamine class of psychedelic compounds which include the hormone serotonin. It is believed that psilocin exerts its effect by binding to the serotonin 5-HT2A receptor. However, recent in-vivo evidence suggests that psilocin may employ a different mechanism to exert its effects. Membrane-mediated receptor desensitization of neurotransmitter receptors is one such mechanism. We compare the impact of the neutral and charged versions of psilocin and serotonin on the properties of zwitterionic and anionic lipid membranes using molecular dynamics simulations and calorimetry. Both compounds partition to the lipid interface and induce membrane thinning. The tertiary amine in psilocin, as opposed to the primary amine in serotonin, limits psilocin's impact on the membrane although more psilocin partitions into the membrane than serotonin. Calorimetry corroborates that both compounds induce a classical melting point depression like anesthetics do. Our results also lend support to a membrane-mediated receptor-binding mechanism for both psilocin and serotonin and provide physical insights into subtle chemical changes that can alter the membrane-binding of psychedelic compounds.

KW - Lipid-drug interactions

KW - Magic mushrooms

KW - Molecular dynamics (MD) simulations

KW - Psilocin

KW - Psychedelic drugs

KW - Serotonin

U2 - 10.1016/j.bbamem.2022.183957

DO - 10.1016/j.bbamem.2022.183957

M3 - Journal article

C2 - 35561790

AN - SCOPUS:85131122129

VL - 1864

JO - BBA Biomembranes

JF - BBA Biomembranes

SN - 0005-2736

IS - 9

M1 - 183957

ER -

Magic mushroom extracts in lipid membranes

Abstract

Keywords

Documents & Links

Fingerprint

Cite this