CRL4 antagonizes SCF(Fbxo7)-mediated turnover of cereblon and BK channel to regulate learning and memory

Intellectual disability (ID), one of the most common human developmental disorders, can be caused by genetic mutations in Cullin 4B (Cul4B) and cereblon (CRBN). CRBN is a substrate receptor for the Cul4A/B-DDB1 ubiquitin ligase (CRL4) and can target voltage- and calcium-activated BK channel for ER r...

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Autores principales: Song, Tianyu, Liang, Shenghui, Liu, Jiye, Zhang, Tingyue, Yin, Yifei, Geng, Chenlu, Gao, Shaobing, Feng, Yan, Xu, Hao, Guo, Dongqing, Roberts, Amanda, Gu, Yuchun, Cang, Yong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5800687/
https://www.ncbi.nlm.nih.gov/pubmed/29370161
http://dx.doi.org/10.1371/journal.pgen.1007165
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author Song, Tianyu
Liang, Shenghui
Liu, Jiye
Zhang, Tingyue
Yin, Yifei
Geng, Chenlu
Gao, Shaobing
Feng, Yan
Xu, Hao
Guo, Dongqing
Roberts, Amanda
Gu, Yuchun
Cang, Yong
author_facet Song, Tianyu
Liang, Shenghui
Liu, Jiye
Zhang, Tingyue
Yin, Yifei
Geng, Chenlu
Gao, Shaobing
Feng, Yan
Xu, Hao
Guo, Dongqing
Roberts, Amanda
Gu, Yuchun
Cang, Yong
author_sort Song, Tianyu
collection PubMed
description Intellectual disability (ID), one of the most common human developmental disorders, can be caused by genetic mutations in Cullin 4B (Cul4B) and cereblon (CRBN). CRBN is a substrate receptor for the Cul4A/B-DDB1 ubiquitin ligase (CRL4) and can target voltage- and calcium-activated BK channel for ER retention. Here we report that ID-associated CRL4(CRBN) mutations abolish the interaction of the BK channel with CRL4, and redirect the BK channel to the SCF(Fbxo7) ubiquitin ligase for proteasomal degradation. Glioma cell lines harbouring CRBN mutations record density-dependent decrease of BK currents, which can be restored by blocking Cullin ubiquitin ligase activity. Importantly, mice with neuron-specific deletion of DDB1 or CRBN express reduced BK protein levels in the brain, and exhibit similar impairment in learning and memory, a deficit that can be partially rescued by activating the BK channel. Our results reveal a competitive targeting of the BK channel by two ubiquitin ligases to achieve exquisite control of its stability, and support changes in neuronal excitability as a common pathogenic mechanism underlying CRL4(CRBN)–associated ID.
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spelling pubmed-58006872018-02-23 CRL4 antagonizes SCF(Fbxo7)-mediated turnover of cereblon and BK channel to regulate learning and memory Song, Tianyu Liang, Shenghui Liu, Jiye Zhang, Tingyue Yin, Yifei Geng, Chenlu Gao, Shaobing Feng, Yan Xu, Hao Guo, Dongqing Roberts, Amanda Gu, Yuchun Cang, Yong PLoS Genet Research Article Intellectual disability (ID), one of the most common human developmental disorders, can be caused by genetic mutations in Cullin 4B (Cul4B) and cereblon (CRBN). CRBN is a substrate receptor for the Cul4A/B-DDB1 ubiquitin ligase (CRL4) and can target voltage- and calcium-activated BK channel for ER retention. Here we report that ID-associated CRL4(CRBN) mutations abolish the interaction of the BK channel with CRL4, and redirect the BK channel to the SCF(Fbxo7) ubiquitin ligase for proteasomal degradation. Glioma cell lines harbouring CRBN mutations record density-dependent decrease of BK currents, which can be restored by blocking Cullin ubiquitin ligase activity. Importantly, mice with neuron-specific deletion of DDB1 or CRBN express reduced BK protein levels in the brain, and exhibit similar impairment in learning and memory, a deficit that can be partially rescued by activating the BK channel. Our results reveal a competitive targeting of the BK channel by two ubiquitin ligases to achieve exquisite control of its stability, and support changes in neuronal excitability as a common pathogenic mechanism underlying CRL4(CRBN)–associated ID. Public Library of Science 2018-01-25 /pmc/articles/PMC5800687/ /pubmed/29370161 http://dx.doi.org/10.1371/journal.pgen.1007165 Text en © 2018 Song 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
Song, Tianyu
Liang, Shenghui
Liu, Jiye
Zhang, Tingyue
Yin, Yifei
Geng, Chenlu
Gao, Shaobing
Feng, Yan
Xu, Hao
Guo, Dongqing
Roberts, Amanda
Gu, Yuchun
Cang, Yong
CRL4 antagonizes SCF(Fbxo7)-mediated turnover of cereblon and BK channel to regulate learning and memory
title CRL4 antagonizes SCF(Fbxo7)-mediated turnover of cereblon and BK channel to regulate learning and memory
title_full CRL4 antagonizes SCF(Fbxo7)-mediated turnover of cereblon and BK channel to regulate learning and memory
title_fullStr CRL4 antagonizes SCF(Fbxo7)-mediated turnover of cereblon and BK channel to regulate learning and memory
title_full_unstemmed CRL4 antagonizes SCF(Fbxo7)-mediated turnover of cereblon and BK channel to regulate learning and memory
title_short CRL4 antagonizes SCF(Fbxo7)-mediated turnover of cereblon and BK channel to regulate learning and memory
title_sort crl4 antagonizes scf(fbxo7)-mediated turnover of cereblon and bk channel to regulate learning and memory
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5800687/
https://www.ncbi.nlm.nih.gov/pubmed/29370161
http://dx.doi.org/10.1371/journal.pgen.1007165
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