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Synthetic Self-Assembling Clostridial Chimera for Modulation of Sensory Functions

[Image: see text] Clostridial neurotoxins reversibly block neuronal communication for weeks and months. While these proteolytic neurotoxins hold great promise for clinical applications and the investigation of brain function, their paralytic activity at neuromuscular junctions is a stumbling block....

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Autores principales: Ferrari, Enrico, Gu, Chunjing, Niranjan, Dhevahi, Restani, Laura, Rasetti-Escargueil, Christine, Obara, Ilona, Geranton, Sandrine M., Arsenault, Jason, Goetze, Tom A., Harper, Callista B., Nguyen, Tam H., Maywood, Elizabeth, O’Brien, John, Schiavo, Giampietro, Wheeler, Daniel W., Meunier, Frederic A., Hastings, Michael, Edwardson, J. Michael, Sesardic, Dorothea, Caleo, Matteo, Hunt, Stephen P., Davletov, Bazbek
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2013
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3901392/
https://www.ncbi.nlm.nih.gov/pubmed/24011174
http://dx.doi.org/10.1021/bc4003103
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author Ferrari, Enrico
Gu, Chunjing
Niranjan, Dhevahi
Restani, Laura
Rasetti-Escargueil, Christine
Obara, Ilona
Geranton, Sandrine M.
Arsenault, Jason
Goetze, Tom A.
Harper, Callista B.
Nguyen, Tam H.
Maywood, Elizabeth
O’Brien, John
Schiavo, Giampietro
Wheeler, Daniel W.
Meunier, Frederic A.
Hastings, Michael
Edwardson, J. Michael
Sesardic, Dorothea
Caleo, Matteo
Hunt, Stephen P.
Davletov, Bazbek
author_facet Ferrari, Enrico
Gu, Chunjing
Niranjan, Dhevahi
Restani, Laura
Rasetti-Escargueil, Christine
Obara, Ilona
Geranton, Sandrine M.
Arsenault, Jason
Goetze, Tom A.
Harper, Callista B.
Nguyen, Tam H.
Maywood, Elizabeth
O’Brien, John
Schiavo, Giampietro
Wheeler, Daniel W.
Meunier, Frederic A.
Hastings, Michael
Edwardson, J. Michael
Sesardic, Dorothea
Caleo, Matteo
Hunt, Stephen P.
Davletov, Bazbek
author_sort Ferrari, Enrico
collection PubMed
description [Image: see text] Clostridial neurotoxins reversibly block neuronal communication for weeks and months. While these proteolytic neurotoxins hold great promise for clinical applications and the investigation of brain function, their paralytic activity at neuromuscular junctions is a stumbling block. To redirect the clostridial activity to neuronal populations other than motor neurons, we used a new self-assembling method to combine the botulinum type A protease with the tetanus binding domain, which natively targets central neurons. The two parts were produced separately and then assembled in a site-specific way using a newly introduced ‘protein stapling’ technology. Atomic force microscopy imaging revealed dumbbell shaped particles which measure ∼23 nm. The stapled chimera inhibited mechanical hypersensitivity in a rat model of inflammatory pain without causing either flaccid or spastic paralysis. Moreover, the synthetic clostridial molecule was able to block neuronal activity in a defined area of visual cortex. Overall, we provide the first evidence that the protein stapling technology allows assembly of distinct proteins yielding new biomedical properties.
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spelling pubmed-39013922014-01-24 Synthetic Self-Assembling Clostridial Chimera for Modulation of Sensory Functions Ferrari, Enrico Gu, Chunjing Niranjan, Dhevahi Restani, Laura Rasetti-Escargueil, Christine Obara, Ilona Geranton, Sandrine M. Arsenault, Jason Goetze, Tom A. Harper, Callista B. Nguyen, Tam H. Maywood, Elizabeth O’Brien, John Schiavo, Giampietro Wheeler, Daniel W. Meunier, Frederic A. Hastings, Michael Edwardson, J. Michael Sesardic, Dorothea Caleo, Matteo Hunt, Stephen P. Davletov, Bazbek Bioconjug Chem [Image: see text] Clostridial neurotoxins reversibly block neuronal communication for weeks and months. While these proteolytic neurotoxins hold great promise for clinical applications and the investigation of brain function, their paralytic activity at neuromuscular junctions is a stumbling block. To redirect the clostridial activity to neuronal populations other than motor neurons, we used a new self-assembling method to combine the botulinum type A protease with the tetanus binding domain, which natively targets central neurons. The two parts were produced separately and then assembled in a site-specific way using a newly introduced ‘protein stapling’ technology. Atomic force microscopy imaging revealed dumbbell shaped particles which measure ∼23 nm. The stapled chimera inhibited mechanical hypersensitivity in a rat model of inflammatory pain without causing either flaccid or spastic paralysis. Moreover, the synthetic clostridial molecule was able to block neuronal activity in a defined area of visual cortex. Overall, we provide the first evidence that the protein stapling technology allows assembly of distinct proteins yielding new biomedical properties. American Chemical Society 2013-09-06 2013-10-16 /pmc/articles/PMC3901392/ /pubmed/24011174 http://dx.doi.org/10.1021/bc4003103 Text en Copyright © 2013 American Chemical Society Terms of Use CC-BY (http://pubs.acs.org/page/policy/authorchoice_ccby_termsofuse.html)
spellingShingle Ferrari, Enrico
Gu, Chunjing
Niranjan, Dhevahi
Restani, Laura
Rasetti-Escargueil, Christine
Obara, Ilona
Geranton, Sandrine M.
Arsenault, Jason
Goetze, Tom A.
Harper, Callista B.
Nguyen, Tam H.
Maywood, Elizabeth
O’Brien, John
Schiavo, Giampietro
Wheeler, Daniel W.
Meunier, Frederic A.
Hastings, Michael
Edwardson, J. Michael
Sesardic, Dorothea
Caleo, Matteo
Hunt, Stephen P.
Davletov, Bazbek
Synthetic Self-Assembling Clostridial Chimera for Modulation of Sensory Functions
title Synthetic Self-Assembling Clostridial Chimera for Modulation of Sensory Functions
title_full Synthetic Self-Assembling Clostridial Chimera for Modulation of Sensory Functions
title_fullStr Synthetic Self-Assembling Clostridial Chimera for Modulation of Sensory Functions
title_full_unstemmed Synthetic Self-Assembling Clostridial Chimera for Modulation of Sensory Functions
title_short Synthetic Self-Assembling Clostridial Chimera for Modulation of Sensory Functions
title_sort synthetic self-assembling clostridial chimera for modulation of sensory functions
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3901392/
https://www.ncbi.nlm.nih.gov/pubmed/24011174
http://dx.doi.org/10.1021/bc4003103
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