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Chemically targeting the redox switch in AP1 transcription factor ΔFOSB

The AP1 transcription factor ΔFOSB, a splice variant of FOSB, accumulates in the brain in response to chronic insults such as exposure to drugs of abuse, depression, Alzheimer's disease and tardive dyskinesias, and mediates subsequent long-term neuroadaptations. ΔFOSB forms heterodimers with ot...

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Autores principales: Kumar, Ashwani, Aglyamova, Galina, Yim, Yun Young, Bailey, Aaron O, Lynch, Haley M, Powell, Reid T, Nguyen, Nghi D, Rosenthal, Zachary, Zhao, Wen-Ning, Li, Yi, Chen, Jianping, Fan, Shanghua, Lee, Hubert, Russell, William K, Stephan, Clifford, Robison, Alfred J, Haggarty, Stephen J, Nestler, Eric J, Zhou, Jia, Machius, Mischa, Rudenko, Gabby
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9458432/
https://www.ncbi.nlm.nih.gov/pubmed/36039764
http://dx.doi.org/10.1093/nar/gkac710
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author Kumar, Ashwani
Aglyamova, Galina
Yim, Yun Young
Bailey, Aaron O
Lynch, Haley M
Powell, Reid T
Nguyen, Nghi D
Rosenthal, Zachary
Zhao, Wen-Ning
Li, Yi
Chen, Jianping
Fan, Shanghua
Lee, Hubert
Russell, William K
Stephan, Clifford
Robison, Alfred J
Haggarty, Stephen J
Nestler, Eric J
Zhou, Jia
Machius, Mischa
Rudenko, Gabby
author_facet Kumar, Ashwani
Aglyamova, Galina
Yim, Yun Young
Bailey, Aaron O
Lynch, Haley M
Powell, Reid T
Nguyen, Nghi D
Rosenthal, Zachary
Zhao, Wen-Ning
Li, Yi
Chen, Jianping
Fan, Shanghua
Lee, Hubert
Russell, William K
Stephan, Clifford
Robison, Alfred J
Haggarty, Stephen J
Nestler, Eric J
Zhou, Jia
Machius, Mischa
Rudenko, Gabby
author_sort Kumar, Ashwani
collection PubMed
description The AP1 transcription factor ΔFOSB, a splice variant of FOSB, accumulates in the brain in response to chronic insults such as exposure to drugs of abuse, depression, Alzheimer's disease and tardive dyskinesias, and mediates subsequent long-term neuroadaptations. ΔFOSB forms heterodimers with other AP1 transcription factors, e.g. JUND, that bind DNA under control of a putative cysteine-based redox switch. Here, we reveal the structural basis of the redox switch by determining a key missing crystal structure in a trio, the ΔFOSB/JUND bZIP domains in the reduced, DNA-free form. Screening a cysteine-focused library containing 3200 thiol-reactive compounds, we identify specific compounds that target the redox switch, validate their activity biochemically and in cell-based assays, and show that they are well tolerated in different cell lines despite their general potential to bind to cysteines covalently. A crystal structure of the ΔFOSB/JUND bZIP domains in complex with a redox-switch-targeting compound reveals a deep compound-binding pocket near the DNA-binding site. We demonstrate that ΔFOSB, and potentially other, related AP1 transcription factors, can be targeted specifically and discriminately by exploiting unique structural features such as the redox switch and the binding partner to modulate biological function despite these proteins previously being thought to be undruggable.
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spelling pubmed-94584322022-09-09 Chemically targeting the redox switch in AP1 transcription factor ΔFOSB Kumar, Ashwani Aglyamova, Galina Yim, Yun Young Bailey, Aaron O Lynch, Haley M Powell, Reid T Nguyen, Nghi D Rosenthal, Zachary Zhao, Wen-Ning Li, Yi Chen, Jianping Fan, Shanghua Lee, Hubert Russell, William K Stephan, Clifford Robison, Alfred J Haggarty, Stephen J Nestler, Eric J Zhou, Jia Machius, Mischa Rudenko, Gabby Nucleic Acids Res Structural Biology The AP1 transcription factor ΔFOSB, a splice variant of FOSB, accumulates in the brain in response to chronic insults such as exposure to drugs of abuse, depression, Alzheimer's disease and tardive dyskinesias, and mediates subsequent long-term neuroadaptations. ΔFOSB forms heterodimers with other AP1 transcription factors, e.g. JUND, that bind DNA under control of a putative cysteine-based redox switch. Here, we reveal the structural basis of the redox switch by determining a key missing crystal structure in a trio, the ΔFOSB/JUND bZIP domains in the reduced, DNA-free form. Screening a cysteine-focused library containing 3200 thiol-reactive compounds, we identify specific compounds that target the redox switch, validate their activity biochemically and in cell-based assays, and show that they are well tolerated in different cell lines despite their general potential to bind to cysteines covalently. A crystal structure of the ΔFOSB/JUND bZIP domains in complex with a redox-switch-targeting compound reveals a deep compound-binding pocket near the DNA-binding site. We demonstrate that ΔFOSB, and potentially other, related AP1 transcription factors, can be targeted specifically and discriminately by exploiting unique structural features such as the redox switch and the binding partner to modulate biological function despite these proteins previously being thought to be undruggable. Oxford University Press 2022-08-30 /pmc/articles/PMC9458432/ /pubmed/36039764 http://dx.doi.org/10.1093/nar/gkac710 Text en © The Author(s) 2022. Published by Oxford University Press on behalf of Nucleic Acids Research. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Structural Biology
Kumar, Ashwani
Aglyamova, Galina
Yim, Yun Young
Bailey, Aaron O
Lynch, Haley M
Powell, Reid T
Nguyen, Nghi D
Rosenthal, Zachary
Zhao, Wen-Ning
Li, Yi
Chen, Jianping
Fan, Shanghua
Lee, Hubert
Russell, William K
Stephan, Clifford
Robison, Alfred J
Haggarty, Stephen J
Nestler, Eric J
Zhou, Jia
Machius, Mischa
Rudenko, Gabby
Chemically targeting the redox switch in AP1 transcription factor ΔFOSB
title Chemically targeting the redox switch in AP1 transcription factor ΔFOSB
title_full Chemically targeting the redox switch in AP1 transcription factor ΔFOSB
title_fullStr Chemically targeting the redox switch in AP1 transcription factor ΔFOSB
title_full_unstemmed Chemically targeting the redox switch in AP1 transcription factor ΔFOSB
title_short Chemically targeting the redox switch in AP1 transcription factor ΔFOSB
title_sort chemically targeting the redox switch in ap1 transcription factor δfosb
topic Structural Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9458432/
https://www.ncbi.nlm.nih.gov/pubmed/36039764
http://dx.doi.org/10.1093/nar/gkac710
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