Structural and Functional Characterization of a Novel Scorpion Toxin that Inhibits Na(V)1.8 via Interactions With the DI Voltage Sensor and DII Pore Module

Voltage-gated sodium channel Na(V)1.8 regulates transmission of pain signals to the brain. While Na(V)1.8 has the potential to serve as a drug target, the molecular mechanisms that shape Na(V)1.8 gating are not completely understood, particularly mechanisms that couple activation to inactivation. In...

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Autores principales: George, Kiran, Lopez-Mateos, Diego, Abd El-Aziz, Tarek Mohamed, Xiao, Yucheng, Kline, Jake, Bao, Hong, Raza, Syed, Stockand, James D., Cummins, Theodore R., Fornelli, Luca, Rowe, Matthew P., Yarov-Yarovoy, Vladimir, Rowe, Ashlee H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9160825/
https://www.ncbi.nlm.nih.gov/pubmed/35662692
http://dx.doi.org/10.3389/fphar.2022.846992
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author George, Kiran
Lopez-Mateos, Diego
Abd El-Aziz, Tarek Mohamed
Xiao, Yucheng
Kline, Jake
Bao, Hong
Raza, Syed
Stockand, James D.
Cummins, Theodore R.
Fornelli, Luca
Rowe, Matthew P.
Yarov-Yarovoy, Vladimir
Rowe, Ashlee H.
author_facet George, Kiran
Lopez-Mateos, Diego
Abd El-Aziz, Tarek Mohamed
Xiao, Yucheng
Kline, Jake
Bao, Hong
Raza, Syed
Stockand, James D.
Cummins, Theodore R.
Fornelli, Luca
Rowe, Matthew P.
Yarov-Yarovoy, Vladimir
Rowe, Ashlee H.
author_sort George, Kiran
collection PubMed
description Voltage-gated sodium channel Na(V)1.8 regulates transmission of pain signals to the brain. While Na(V)1.8 has the potential to serve as a drug target, the molecular mechanisms that shape Na(V)1.8 gating are not completely understood, particularly mechanisms that couple activation to inactivation. Interactions between toxin producing animals and their predators provide a novel approach for investigating Na(V) structure-function relationships. Arizona bark scorpions produce Na(+) channel toxins that initiate pain signaling. However, in predatory grasshopper mice, toxins inhibit Na(V)1.8 currents and block pain signals. A screen of synthetic peptide toxins predicted from bark scorpion venom showed that peptide NaTx36 inhibited Na(+) current recorded from a recombinant grasshopper mouse Na(V)1.8 channel (OtNa(V)1.8). Toxin NaTx36 hyperpolarized OtNa(V)1.8 activation, steady-state fast inactivation, and slow inactivation. Mutagenesis revealed that the first gating charge in the domain I (DI) S4 voltage sensor and an acidic amino acid (E) in the DII SS2 – S6 pore loop are critical for the inhibitory effects of NaTx36. Computational modeling showed that a DI S1 – S2 asparagine (N) stabilizes the NaTx36 – OtNa(V)1.8 complex while residues in the DI S3 – S4 linker and S4 voltage sensor form electrostatic interactions that allow a toxin glutamine (Q) to contact the first S4 gating charge. Surprisingly, the models predicted that NaTx36 contacts amino acids in the DII S5 – SS1 pore loop instead of the SS2 – S6 loop; the DII SS2 – S6 loop motif (QVSE) alters the conformation of the DII S5 – SS1 pore loop, enhancing allosteric interactions between toxin and the DII S5 – SS1 pore loop. Few toxins have been identified that modify Na(V)1.8 gating. Moreover, few toxins have been described that modify sodium channel gating via the DI S4 voltage sensor. Thus, NaTx36 and OtNa(V)1.8 provide tools for investigating the structure-activity relationship between channel activation and inactivation gating, and the connection to alternative pain phenotypes.
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spelling pubmed-91608252022-06-03 Structural and Functional Characterization of a Novel Scorpion Toxin that Inhibits Na(V)1.8 via Interactions With the DI Voltage Sensor and DII Pore Module George, Kiran Lopez-Mateos, Diego Abd El-Aziz, Tarek Mohamed Xiao, Yucheng Kline, Jake Bao, Hong Raza, Syed Stockand, James D. Cummins, Theodore R. Fornelli, Luca Rowe, Matthew P. Yarov-Yarovoy, Vladimir Rowe, Ashlee H. Front Pharmacol Pharmacology Voltage-gated sodium channel Na(V)1.8 regulates transmission of pain signals to the brain. While Na(V)1.8 has the potential to serve as a drug target, the molecular mechanisms that shape Na(V)1.8 gating are not completely understood, particularly mechanisms that couple activation to inactivation. Interactions between toxin producing animals and their predators provide a novel approach for investigating Na(V) structure-function relationships. Arizona bark scorpions produce Na(+) channel toxins that initiate pain signaling. However, in predatory grasshopper mice, toxins inhibit Na(V)1.8 currents and block pain signals. A screen of synthetic peptide toxins predicted from bark scorpion venom showed that peptide NaTx36 inhibited Na(+) current recorded from a recombinant grasshopper mouse Na(V)1.8 channel (OtNa(V)1.8). Toxin NaTx36 hyperpolarized OtNa(V)1.8 activation, steady-state fast inactivation, and slow inactivation. Mutagenesis revealed that the first gating charge in the domain I (DI) S4 voltage sensor and an acidic amino acid (E) in the DII SS2 – S6 pore loop are critical for the inhibitory effects of NaTx36. Computational modeling showed that a DI S1 – S2 asparagine (N) stabilizes the NaTx36 – OtNa(V)1.8 complex while residues in the DI S3 – S4 linker and S4 voltage sensor form electrostatic interactions that allow a toxin glutamine (Q) to contact the first S4 gating charge. Surprisingly, the models predicted that NaTx36 contacts amino acids in the DII S5 – SS1 pore loop instead of the SS2 – S6 loop; the DII SS2 – S6 loop motif (QVSE) alters the conformation of the DII S5 – SS1 pore loop, enhancing allosteric interactions between toxin and the DII S5 – SS1 pore loop. Few toxins have been identified that modify Na(V)1.8 gating. Moreover, few toxins have been described that modify sodium channel gating via the DI S4 voltage sensor. Thus, NaTx36 and OtNa(V)1.8 provide tools for investigating the structure-activity relationship between channel activation and inactivation gating, and the connection to alternative pain phenotypes. Frontiers Media S.A. 2022-05-19 /pmc/articles/PMC9160825/ /pubmed/35662692 http://dx.doi.org/10.3389/fphar.2022.846992 Text en Copyright © 2022 George, Lopez-Mateos, Abd El-Aziz, Xiao, Kline, Bao, Raza, Stockand, Cummins, Fornelli, Rowe, Yarov-Yarovoy and Rowe. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
George, Kiran
Lopez-Mateos, Diego
Abd El-Aziz, Tarek Mohamed
Xiao, Yucheng
Kline, Jake
Bao, Hong
Raza, Syed
Stockand, James D.
Cummins, Theodore R.
Fornelli, Luca
Rowe, Matthew P.
Yarov-Yarovoy, Vladimir
Rowe, Ashlee H.
Structural and Functional Characterization of a Novel Scorpion Toxin that Inhibits Na(V)1.8 via Interactions With the DI Voltage Sensor and DII Pore Module
title Structural and Functional Characterization of a Novel Scorpion Toxin that Inhibits Na(V)1.8 via Interactions With the DI Voltage Sensor and DII Pore Module
title_full Structural and Functional Characterization of a Novel Scorpion Toxin that Inhibits Na(V)1.8 via Interactions With the DI Voltage Sensor and DII Pore Module
title_fullStr Structural and Functional Characterization of a Novel Scorpion Toxin that Inhibits Na(V)1.8 via Interactions With the DI Voltage Sensor and DII Pore Module
title_full_unstemmed Structural and Functional Characterization of a Novel Scorpion Toxin that Inhibits Na(V)1.8 via Interactions With the DI Voltage Sensor and DII Pore Module
title_short Structural and Functional Characterization of a Novel Scorpion Toxin that Inhibits Na(V)1.8 via Interactions With the DI Voltage Sensor and DII Pore Module
title_sort structural and functional characterization of a novel scorpion toxin that inhibits na(v)1.8 via interactions with the di voltage sensor and dii pore module
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9160825/
https://www.ncbi.nlm.nih.gov/pubmed/35662692
http://dx.doi.org/10.3389/fphar.2022.846992
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