Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy

Botulinum neurotoxins (BoNTs) are a family of bacterial toxins with seven major serotypes (BoNT/A–G). The ability of these toxins to target and bind to motor nerve terminals is a key factor determining their potency and efficacy. Among these toxins, BoNT/B is one of the two types approved for medica...

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Autores principales: Yin, Linxiang, Masuyer, Geoffrey, Zhang, Sicai, Zhang, Jie, Miyashita, Shin-Ichiro, Burgin, David, Lovelock, Laura, Coker, Shu-Fen, Fu, Tian-min, Stenmark, Pål, Dong, Min
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2020
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7077807/
https://www.ncbi.nlm.nih.gov/pubmed/32182233
http://dx.doi.org/10.1371/journal.pbio.3000618
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author Yin, Linxiang
Masuyer, Geoffrey
Zhang, Sicai
Zhang, Jie
Miyashita, Shin-Ichiro
Burgin, David
Lovelock, Laura
Coker, Shu-Fen
Fu, Tian-min
Stenmark, Pål
Dong, Min
author_facet Yin, Linxiang
Masuyer, Geoffrey
Zhang, Sicai
Zhang, Jie
Miyashita, Shin-Ichiro
Burgin, David
Lovelock, Laura
Coker, Shu-Fen
Fu, Tian-min
Stenmark, Pål
Dong, Min
author_sort Yin, Linxiang
collection PubMed
description Botulinum neurotoxins (BoNTs) are a family of bacterial toxins with seven major serotypes (BoNT/A–G). The ability of these toxins to target and bind to motor nerve terminals is a key factor determining their potency and efficacy. Among these toxins, BoNT/B is one of the two types approved for medical and cosmetic uses. Besides binding to well-established receptors, an extended loop in the C-terminal receptor-binding domain (H(C)) of BoNT/B (H(C)/B) has been proposed to also contribute to toxin binding to neurons by interacting with lipid membranes (termed lipid-binding loop [LBL]). Analogous loops exist in the H(C)s of BoNT/C, D, G, and a chimeric toxin DC. However, it has been challenging to detect and characterize binding of LBLs to lipid membranes. Here, using the nanodisc system and biolayer interferometry assays, we find that H(C)/DC, C, and G, but not H(C)/B and H(C)/D, are capable of binding to receptor-free lipids directly, with H(C)/DC having the highest level of binding. Mutagenesis studies demonstrate the critical role of consecutive aromatic residues at the tip of the LBL for binding of H(C)/DC to lipid membranes. Taking advantage of this insight, we then create a “gain-of-function” mutant H(C)/B by replacing two nonaromatic residues at the tip of its LBL with tryptophan. Cocrystallization studies confirm that these two tryptophan residues do not alter the structure of H(C)/B or the interactions with its receptors. Such a mutated H(C)/B gains the ability to bind receptor-free lipid membranes and shows enhanced binding to cultured neurons. Finally, full-length BoNT/B containing two tryptophan mutations in its LBL, together with two additional mutations (E1191M/S1199Y) that increase binding to human receptors, is produced and evaluated in mice in vivo using Digit Abduction Score assays. This mutant toxin shows enhanced efficacy in paralyzing local muscles at the injection site and lower systemic diffusion, thus extending both safety range and duration of paralysis compared with the control BoNT/B. These findings establish a mechanistic understanding of LBL–lipid interactions and create a modified BoNT/B with improved therapeutic efficacy.
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spelling pubmed-70778072020-03-23 Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy Yin, Linxiang Masuyer, Geoffrey Zhang, Sicai Zhang, Jie Miyashita, Shin-Ichiro Burgin, David Lovelock, Laura Coker, Shu-Fen Fu, Tian-min Stenmark, Pål Dong, Min PLoS Biol Research Article Botulinum neurotoxins (BoNTs) are a family of bacterial toxins with seven major serotypes (BoNT/A–G). The ability of these toxins to target and bind to motor nerve terminals is a key factor determining their potency and efficacy. Among these toxins, BoNT/B is one of the two types approved for medical and cosmetic uses. Besides binding to well-established receptors, an extended loop in the C-terminal receptor-binding domain (H(C)) of BoNT/B (H(C)/B) has been proposed to also contribute to toxin binding to neurons by interacting with lipid membranes (termed lipid-binding loop [LBL]). Analogous loops exist in the H(C)s of BoNT/C, D, G, and a chimeric toxin DC. However, it has been challenging to detect and characterize binding of LBLs to lipid membranes. Here, using the nanodisc system and biolayer interferometry assays, we find that H(C)/DC, C, and G, but not H(C)/B and H(C)/D, are capable of binding to receptor-free lipids directly, with H(C)/DC having the highest level of binding. Mutagenesis studies demonstrate the critical role of consecutive aromatic residues at the tip of the LBL for binding of H(C)/DC to lipid membranes. Taking advantage of this insight, we then create a “gain-of-function” mutant H(C)/B by replacing two nonaromatic residues at the tip of its LBL with tryptophan. Cocrystallization studies confirm that these two tryptophan residues do not alter the structure of H(C)/B or the interactions with its receptors. Such a mutated H(C)/B gains the ability to bind receptor-free lipid membranes and shows enhanced binding to cultured neurons. Finally, full-length BoNT/B containing two tryptophan mutations in its LBL, together with two additional mutations (E1191M/S1199Y) that increase binding to human receptors, is produced and evaluated in mice in vivo using Digit Abduction Score assays. This mutant toxin shows enhanced efficacy in paralyzing local muscles at the injection site and lower systemic diffusion, thus extending both safety range and duration of paralysis compared with the control BoNT/B. These findings establish a mechanistic understanding of LBL–lipid interactions and create a modified BoNT/B with improved therapeutic efficacy. Public Library of Science 2020-03-17 /pmc/articles/PMC7077807/ /pubmed/32182233 http://dx.doi.org/10.1371/journal.pbio.3000618 Text en © 2020 Yin et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Yin, Linxiang
Masuyer, Geoffrey
Zhang, Sicai
Zhang, Jie
Miyashita, Shin-Ichiro
Burgin, David
Lovelock, Laura
Coker, Shu-Fen
Fu, Tian-min
Stenmark, Pål
Dong, Min
Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy
title Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy
title_full Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy
title_fullStr Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy
title_full_unstemmed Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy
title_short Characterization of a membrane binding loop leads to engineering botulinum neurotoxin B with improved therapeutic efficacy
title_sort characterization of a membrane binding loop leads to engineering botulinum neurotoxin b with improved therapeutic efficacy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7077807/
https://www.ncbi.nlm.nih.gov/pubmed/32182233
http://dx.doi.org/10.1371/journal.pbio.3000618
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