ALS-associated missense and nonsense TBK1 mutations can both cause loss of kinase function

Mutations in TANK binding kinase 1 (TBK1) have been linked to amyotrophic lateral sclerosis. Some TBK1 variants are nonsense and are predicted to cause disease through haploinsufficiency; however, many other mutations are missense with unknown functional effects. We exome sequenced 699 familial amyo...

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Autores principales: de Majo, Martina, Topp, Simon D., Smith, Bradley N., Nishimura, Agnes L., Chen, Han-Jou, Gkazi, Athina Soragia, Miller, Jack, Wong, Chun Hao, Vance, Caroline, Baas, Frank, ten Asbroek, Anneloor L.M.A., Kenna, Kevin P., Ticozzi, Nicola, Redondo, Alberto Garcia, Esteban-Pérez, Jesús, Tiloca, Cinzia, Verde, Federico, Duga, Stefano, Morrison, Karen E., Shaw, Pamela J., Kirby, Janine, Turner, Martin R., Talbot, Kevin, Hardiman, Orla, Glass, Jonathan D., de Belleroche, Jacqueline, Gellera, Cinzia, Ratti, Antonia, Al-Chalabi, Ammar, Brown, Robert H., Silani, Vincenzo, Landers, John E., Shaw, Christopher E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2018
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6983933/
https://www.ncbi.nlm.nih.gov/pubmed/30033073
http://dx.doi.org/10.1016/j.neurobiolaging.2018.06.015
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author de Majo, Martina
Topp, Simon D.
Smith, Bradley N.
Nishimura, Agnes L.
Chen, Han-Jou
Gkazi, Athina Soragia
Miller, Jack
Wong, Chun Hao
Vance, Caroline
Baas, Frank
ten Asbroek, Anneloor L.M.A.
Kenna, Kevin P.
Ticozzi, Nicola
Redondo, Alberto Garcia
Esteban-Pérez, Jesús
Tiloca, Cinzia
Verde, Federico
Duga, Stefano
Morrison, Karen E.
Shaw, Pamela J.
Kirby, Janine
Turner, Martin R.
Talbot, Kevin
Hardiman, Orla
Glass, Jonathan D.
de Belleroche, Jacqueline
Gellera, Cinzia
Ratti, Antonia
Al-Chalabi, Ammar
Brown, Robert H.
Silani, Vincenzo
Landers, John E.
Shaw, Christopher E.
author_facet de Majo, Martina
Topp, Simon D.
Smith, Bradley N.
Nishimura, Agnes L.
Chen, Han-Jou
Gkazi, Athina Soragia
Miller, Jack
Wong, Chun Hao
Vance, Caroline
Baas, Frank
ten Asbroek, Anneloor L.M.A.
Kenna, Kevin P.
Ticozzi, Nicola
Redondo, Alberto Garcia
Esteban-Pérez, Jesús
Tiloca, Cinzia
Verde, Federico
Duga, Stefano
Morrison, Karen E.
Shaw, Pamela J.
Kirby, Janine
Turner, Martin R.
Talbot, Kevin
Hardiman, Orla
Glass, Jonathan D.
de Belleroche, Jacqueline
Gellera, Cinzia
Ratti, Antonia
Al-Chalabi, Ammar
Brown, Robert H.
Silani, Vincenzo
Landers, John E.
Shaw, Christopher E.
author_sort de Majo, Martina
collection PubMed
description Mutations in TANK binding kinase 1 (TBK1) have been linked to amyotrophic lateral sclerosis. Some TBK1 variants are nonsense and are predicted to cause disease through haploinsufficiency; however, many other mutations are missense with unknown functional effects. We exome sequenced 699 familial amyotrophic lateral sclerosis patients and identified 16 TBK1 novel or extremely rare protein-changing variants. We characterized a subset of these: p.G217R, p.R357X, and p.C471Y. Here, we show that the p.R357X and p.G217R both abolish the ability of TBK1 to phosphorylate 2 of its kinase targets, IRF3 and optineurin, and to undergo phosphorylation. They both inhibit binding to optineurin and the p.G217R, within the TBK1 kinase domain, reduces homodimerization, essential for TBK1 activation and function. Finally, we show that the proportion of TBK1 that is active (phosphorylated) is reduced in 5 lymphoblastoid cell lines derived from patients harboring heterozygous missense or in-frame deletion TBK1 mutations. We conclude that missense mutations in functional domains of TBK1 impair the binding and phosphorylation of its normal targets, implicating a common loss of function mechanism, analogous to truncation mutations.
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spelling pubmed-69839332020-01-30 ALS-associated missense and nonsense TBK1 mutations can both cause loss of kinase function de Majo, Martina Topp, Simon D. Smith, Bradley N. Nishimura, Agnes L. Chen, Han-Jou Gkazi, Athina Soragia Miller, Jack Wong, Chun Hao Vance, Caroline Baas, Frank ten Asbroek, Anneloor L.M.A. Kenna, Kevin P. Ticozzi, Nicola Redondo, Alberto Garcia Esteban-Pérez, Jesús Tiloca, Cinzia Verde, Federico Duga, Stefano Morrison, Karen E. Shaw, Pamela J. Kirby, Janine Turner, Martin R. Talbot, Kevin Hardiman, Orla Glass, Jonathan D. de Belleroche, Jacqueline Gellera, Cinzia Ratti, Antonia Al-Chalabi, Ammar Brown, Robert H. Silani, Vincenzo Landers, John E. Shaw, Christopher E. Neurobiol Aging Article Mutations in TANK binding kinase 1 (TBK1) have been linked to amyotrophic lateral sclerosis. Some TBK1 variants are nonsense and are predicted to cause disease through haploinsufficiency; however, many other mutations are missense with unknown functional effects. We exome sequenced 699 familial amyotrophic lateral sclerosis patients and identified 16 TBK1 novel or extremely rare protein-changing variants. We characterized a subset of these: p.G217R, p.R357X, and p.C471Y. Here, we show that the p.R357X and p.G217R both abolish the ability of TBK1 to phosphorylate 2 of its kinase targets, IRF3 and optineurin, and to undergo phosphorylation. They both inhibit binding to optineurin and the p.G217R, within the TBK1 kinase domain, reduces homodimerization, essential for TBK1 activation and function. Finally, we show that the proportion of TBK1 that is active (phosphorylated) is reduced in 5 lymphoblastoid cell lines derived from patients harboring heterozygous missense or in-frame deletion TBK1 mutations. We conclude that missense mutations in functional domains of TBK1 impair the binding and phosphorylation of its normal targets, implicating a common loss of function mechanism, analogous to truncation mutations. Elsevier 2018-11 /pmc/articles/PMC6983933/ /pubmed/30033073 http://dx.doi.org/10.1016/j.neurobiolaging.2018.06.015 Text en © 2018 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
de Majo, Martina
Topp, Simon D.
Smith, Bradley N.
Nishimura, Agnes L.
Chen, Han-Jou
Gkazi, Athina Soragia
Miller, Jack
Wong, Chun Hao
Vance, Caroline
Baas, Frank
ten Asbroek, Anneloor L.M.A.
Kenna, Kevin P.
Ticozzi, Nicola
Redondo, Alberto Garcia
Esteban-Pérez, Jesús
Tiloca, Cinzia
Verde, Federico
Duga, Stefano
Morrison, Karen E.
Shaw, Pamela J.
Kirby, Janine
Turner, Martin R.
Talbot, Kevin
Hardiman, Orla
Glass, Jonathan D.
de Belleroche, Jacqueline
Gellera, Cinzia
Ratti, Antonia
Al-Chalabi, Ammar
Brown, Robert H.
Silani, Vincenzo
Landers, John E.
Shaw, Christopher E.
ALS-associated missense and nonsense TBK1 mutations can both cause loss of kinase function
title ALS-associated missense and nonsense TBK1 mutations can both cause loss of kinase function
title_full ALS-associated missense and nonsense TBK1 mutations can both cause loss of kinase function
title_fullStr ALS-associated missense and nonsense TBK1 mutations can both cause loss of kinase function
title_full_unstemmed ALS-associated missense and nonsense TBK1 mutations can both cause loss of kinase function
title_short ALS-associated missense and nonsense TBK1 mutations can both cause loss of kinase function
title_sort als-associated missense and nonsense tbk1 mutations can both cause loss of kinase function
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6983933/
https://www.ncbi.nlm.nih.gov/pubmed/30033073
http://dx.doi.org/10.1016/j.neurobiolaging.2018.06.015
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