Serpin neuropathology in the P497S UBQLN2 mouse model of ALS/FTD

Accumulating evidence suggests X‐linked dominant mutations in UBQLN2 cause amyotrophic lateral sclerosis (ALS) with frontotemporal dementia (FTD) through both loss‐ and gain‐of‐function mechanisms. However, the mechanisms by which the mutations cause disease are still unclear. The goal of the study...

Descripción completa

Detalles Bibliográficos
Autores principales: Higgins, Nicole R., Greenslade, Jessie E., Wu, Josephine J., Miranda, Elena, Galliciotti, Giovanna, Monteiro, Mervyn J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2021
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8387369/
https://www.ncbi.nlm.nih.gov/pubmed/33780087
http://dx.doi.org/10.1111/bpa.12948
_version_ 1783742442503143424
author Higgins, Nicole R.
Greenslade, Jessie E.
Wu, Josephine J.
Miranda, Elena
Galliciotti, Giovanna
Monteiro, Mervyn J.
author_facet Higgins, Nicole R.
Greenslade, Jessie E.
Wu, Josephine J.
Miranda, Elena
Galliciotti, Giovanna
Monteiro, Mervyn J.
author_sort Higgins, Nicole R.
collection PubMed
description Accumulating evidence suggests X‐linked dominant mutations in UBQLN2 cause amyotrophic lateral sclerosis (ALS) with frontotemporal dementia (FTD) through both loss‐ and gain‐of‐function mechanisms. However, the mechanisms by which the mutations cause disease are still unclear. The goal of the study was to uncover the possible pathomechanism(s) by which UBQLN2 mutations cause ALS/FTD. An analysis of proteomic changes in neuronal tissue was used to identify proteins with altered accumulation in the P497S UBQLN2 transgenic mouse model of ALS/FTD. We then used immunocytochemistry and biochemical techniques to confirm protein changes in the mutant P497S mice. Additionally, we used cell lines inactivated of UBQLN2 expression to determine whether its loss underlies the alteration in the proteins seen in P497S mice. The proteome screen identified a dramatic alteration of serine protease inhibitor (serpin) proteins in the mutant P497S animals. Double immunofluorescent staining of brain and spinal cord tissues of the mutant and control mice revealed an age‐dependent change in accumulation of Serpin A1, C1, and I1 in puncta whose staining colocalized with UBQLN2 puncta in the mutant P497S mice. Serpin A1 aggregation in P497S animals was confirmed by biochemical extraction and filter retardation assays. A similar phenomenon of serpin protein aggregation was found in HeLa and NSC34 motor neuron cells with inactivated UBQLN2 expression. We found aberrant aggregation of serpin proteins, particularly Serpin A1, in the brain and spinal cord of the P497S UBQLN2 mouse model of ALS/FTD. Similar aggregation of serpin proteins was found in UBQLN2 knockout cells suggesting that serpin aggregation in the mutant P497S animals may stem from loss of UBQLN2 function. Because serpin aggregation is known to cause disease through both loss‐ and gain‐of‐function mechanisms, we speculate that their accumulation in the P497S mouse model of ALS/FTD may contribute to disease pathogenesis through similar mechanism(s).
format Online
Article
Text
id pubmed-8387369
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher John Wiley and Sons Inc.
record_format MEDLINE/PubMed
spelling pubmed-83873692021-09-01 Serpin neuropathology in the P497S UBQLN2 mouse model of ALS/FTD Higgins, Nicole R. Greenslade, Jessie E. Wu, Josephine J. Miranda, Elena Galliciotti, Giovanna Monteiro, Mervyn J. Brain Pathol Research Articles Accumulating evidence suggests X‐linked dominant mutations in UBQLN2 cause amyotrophic lateral sclerosis (ALS) with frontotemporal dementia (FTD) through both loss‐ and gain‐of‐function mechanisms. However, the mechanisms by which the mutations cause disease are still unclear. The goal of the study was to uncover the possible pathomechanism(s) by which UBQLN2 mutations cause ALS/FTD. An analysis of proteomic changes in neuronal tissue was used to identify proteins with altered accumulation in the P497S UBQLN2 transgenic mouse model of ALS/FTD. We then used immunocytochemistry and biochemical techniques to confirm protein changes in the mutant P497S mice. Additionally, we used cell lines inactivated of UBQLN2 expression to determine whether its loss underlies the alteration in the proteins seen in P497S mice. The proteome screen identified a dramatic alteration of serine protease inhibitor (serpin) proteins in the mutant P497S animals. Double immunofluorescent staining of brain and spinal cord tissues of the mutant and control mice revealed an age‐dependent change in accumulation of Serpin A1, C1, and I1 in puncta whose staining colocalized with UBQLN2 puncta in the mutant P497S mice. Serpin A1 aggregation in P497S animals was confirmed by biochemical extraction and filter retardation assays. A similar phenomenon of serpin protein aggregation was found in HeLa and NSC34 motor neuron cells with inactivated UBQLN2 expression. We found aberrant aggregation of serpin proteins, particularly Serpin A1, in the brain and spinal cord of the P497S UBQLN2 mouse model of ALS/FTD. Similar aggregation of serpin proteins was found in UBQLN2 knockout cells suggesting that serpin aggregation in the mutant P497S animals may stem from loss of UBQLN2 function. Because serpin aggregation is known to cause disease through both loss‐ and gain‐of‐function mechanisms, we speculate that their accumulation in the P497S mouse model of ALS/FTD may contribute to disease pathogenesis through similar mechanism(s). John Wiley and Sons Inc. 2021-03-29 /pmc/articles/PMC8387369/ /pubmed/33780087 http://dx.doi.org/10.1111/bpa.12948 Text en © 2021 The Authors. Brain Pathology published by John Wiley & Sons Ltd on behalf of International Society of Neuropathology https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ (https://creativecommons.org/licenses/by-nc-nd/4.0/) License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Research Articles
Higgins, Nicole R.
Greenslade, Jessie E.
Wu, Josephine J.
Miranda, Elena
Galliciotti, Giovanna
Monteiro, Mervyn J.
Serpin neuropathology in the P497S UBQLN2 mouse model of ALS/FTD
title Serpin neuropathology in the P497S UBQLN2 mouse model of ALS/FTD
title_full Serpin neuropathology in the P497S UBQLN2 mouse model of ALS/FTD
title_fullStr Serpin neuropathology in the P497S UBQLN2 mouse model of ALS/FTD
title_full_unstemmed Serpin neuropathology in the P497S UBQLN2 mouse model of ALS/FTD
title_short Serpin neuropathology in the P497S UBQLN2 mouse model of ALS/FTD
title_sort serpin neuropathology in the p497s ubqln2 mouse model of als/ftd
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8387369/
https://www.ncbi.nlm.nih.gov/pubmed/33780087
http://dx.doi.org/10.1111/bpa.12948
work_keys_str_mv AT higginsnicoler serpinneuropathologyinthep497subqln2mousemodelofalsftd
AT greensladejessiee serpinneuropathologyinthep497subqln2mousemodelofalsftd
AT wujosephinej serpinneuropathologyinthep497subqln2mousemodelofalsftd
AT mirandaelena serpinneuropathologyinthep497subqln2mousemodelofalsftd
AT galliciottigiovanna serpinneuropathologyinthep497subqln2mousemodelofalsftd
AT monteiromervynj serpinneuropathologyinthep497subqln2mousemodelofalsftd

Ejemplares similares