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Nontoxic, double-deletion-mutant rabies viral vectors for retrograde targeting of projection neurons

Recombinant rabies viral vectors have proven useful for applications including retrograde targeting of projection neurons and monosynaptic tracing, but their cytotoxicity has limited their use to short-term experiments. Here we introduce a new class of double-deletion-mutant rabies viral vectors tha...

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Autores principales: Chatterjee, Soumya, Sullivan, Heather A., MacLennan, Bryan J., Xu, Ran, Hou, YuanYuan, Lavin, Thomas K., Lea, Nicholas E., Michalski, Jacob E., Babcock, Kelsey R., Dietrich, Stephan, Matthews, Gillian A., Beyeler, Anna, Calhoon, Gwendolyn G., Glober, Gordon, Whitesell, Jennifer D., Yao, Shenqin, Cetin, Ali, Harris, Julie A., Zeng, Hongkui, Tye, Kay M., Reid, R. Clay, Wickersham, Ian R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6503322/
https://www.ncbi.nlm.nih.gov/pubmed/29507411
http://dx.doi.org/10.1038/s41593-018-0091-7
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author Chatterjee, Soumya
Sullivan, Heather A.
MacLennan, Bryan J.
Xu, Ran
Hou, YuanYuan
Lavin, Thomas K.
Lea, Nicholas E.
Michalski, Jacob E.
Babcock, Kelsey R.
Dietrich, Stephan
Matthews, Gillian A.
Beyeler, Anna
Calhoon, Gwendolyn G.
Glober, Gordon
Whitesell, Jennifer D.
Yao, Shenqin
Cetin, Ali
Harris, Julie A.
Zeng, Hongkui
Tye, Kay M.
Reid, R. Clay
Wickersham, Ian R.
author_facet Chatterjee, Soumya
Sullivan, Heather A.
MacLennan, Bryan J.
Xu, Ran
Hou, YuanYuan
Lavin, Thomas K.
Lea, Nicholas E.
Michalski, Jacob E.
Babcock, Kelsey R.
Dietrich, Stephan
Matthews, Gillian A.
Beyeler, Anna
Calhoon, Gwendolyn G.
Glober, Gordon
Whitesell, Jennifer D.
Yao, Shenqin
Cetin, Ali
Harris, Julie A.
Zeng, Hongkui
Tye, Kay M.
Reid, R. Clay
Wickersham, Ian R.
author_sort Chatterjee, Soumya
collection PubMed
description Recombinant rabies viral vectors have proven useful for applications including retrograde targeting of projection neurons and monosynaptic tracing, but their cytotoxicity has limited their use to short-term experiments. Here we introduce a new class of double-deletion-mutant rabies viral vectors that leave transduced cells alive and healthy indefinitely. Deletion of the viral polymerase gene abolishes cytotoxicity and reduces transgene expression to trace levels but leaves vectors still able to retrogradely infect projection neurons and express recombinases, allowing downstream expression of other transgene products such as fluorophores and calcium indicators. The morphology of retrogradely targeted cells appears unperturbed at one year postinjection. Whole-cell patch-clamp recordings show no physiological abnormalities at eight weeks. Longitudinal two-photon structural and functional imaging in vivo, tracking thousands of individual neurons for up to four months, shows that transduced neurons do not die and retain stable visual response properties even at the longest time points imaged.
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spelling pubmed-65033222019-05-07 Nontoxic, double-deletion-mutant rabies viral vectors for retrograde targeting of projection neurons Chatterjee, Soumya Sullivan, Heather A. MacLennan, Bryan J. Xu, Ran Hou, YuanYuan Lavin, Thomas K. Lea, Nicholas E. Michalski, Jacob E. Babcock, Kelsey R. Dietrich, Stephan Matthews, Gillian A. Beyeler, Anna Calhoon, Gwendolyn G. Glober, Gordon Whitesell, Jennifer D. Yao, Shenqin Cetin, Ali Harris, Julie A. Zeng, Hongkui Tye, Kay M. Reid, R. Clay Wickersham, Ian R. Nat Neurosci Article Recombinant rabies viral vectors have proven useful for applications including retrograde targeting of projection neurons and monosynaptic tracing, but their cytotoxicity has limited their use to short-term experiments. Here we introduce a new class of double-deletion-mutant rabies viral vectors that leave transduced cells alive and healthy indefinitely. Deletion of the viral polymerase gene abolishes cytotoxicity and reduces transgene expression to trace levels but leaves vectors still able to retrogradely infect projection neurons and express recombinases, allowing downstream expression of other transgene products such as fluorophores and calcium indicators. The morphology of retrogradely targeted cells appears unperturbed at one year postinjection. Whole-cell patch-clamp recordings show no physiological abnormalities at eight weeks. Longitudinal two-photon structural and functional imaging in vivo, tracking thousands of individual neurons for up to four months, shows that transduced neurons do not die and retain stable visual response properties even at the longest time points imaged. 2018-03-05 2018-04 /pmc/articles/PMC6503322/ /pubmed/29507411 http://dx.doi.org/10.1038/s41593-018-0091-7 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Chatterjee, Soumya
Sullivan, Heather A.
MacLennan, Bryan J.
Xu, Ran
Hou, YuanYuan
Lavin, Thomas K.
Lea, Nicholas E.
Michalski, Jacob E.
Babcock, Kelsey R.
Dietrich, Stephan
Matthews, Gillian A.
Beyeler, Anna
Calhoon, Gwendolyn G.
Glober, Gordon
Whitesell, Jennifer D.
Yao, Shenqin
Cetin, Ali
Harris, Julie A.
Zeng, Hongkui
Tye, Kay M.
Reid, R. Clay
Wickersham, Ian R.
Nontoxic, double-deletion-mutant rabies viral vectors for retrograde targeting of projection neurons
title Nontoxic, double-deletion-mutant rabies viral vectors for retrograde targeting of projection neurons
title_full Nontoxic, double-deletion-mutant rabies viral vectors for retrograde targeting of projection neurons
title_fullStr Nontoxic, double-deletion-mutant rabies viral vectors for retrograde targeting of projection neurons
title_full_unstemmed Nontoxic, double-deletion-mutant rabies viral vectors for retrograde targeting of projection neurons
title_short Nontoxic, double-deletion-mutant rabies viral vectors for retrograde targeting of projection neurons
title_sort nontoxic, double-deletion-mutant rabies viral vectors for retrograde targeting of projection neurons
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6503322/
https://www.ncbi.nlm.nih.gov/pubmed/29507411
http://dx.doi.org/10.1038/s41593-018-0091-7
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