Early trigeminal and sensory impairment and lysosomal dysfunction in accurate models of Wolfram syndrome Article Swipe
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· 2024
· Open Access
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· DOI: https://doi.org/10.1016/j.expneurol.2024.115099
Wolfram syndrome (WS) is a rare condition caused by homozygous or compound heterozygous mutations in the WFS1 gene primarily. It is diagnosed on the basis of early-onset diabetes mellitus and optic nerve atrophy. Patients complain of trigeminal-like migraines and show deficits in vibration sensation, but the underlying cause is unknown. Using accurate cell models and two separate, accurate rodent models of WS that show excellent face and construct validity, here we have examined trigeminus, sensation and sensory neuronal function in WS. Analysis of ex vivo and in vivo MRI sequences revealed profound trigeminal atrophy in each rodent model, a novel finding in WS. Optic nerve atrophy is a diagnostic sign in WS, and trigeminal atrophy occurred at the time of earliest loss of optic nerve volume. We also observed deficits in mechanical sensation in our mouse WS model, and pathological analysis revealed extensive inflammation in trigeminal sensory nucleus, both of which are novel findings in WS. Sensory neurons (dorsal root ganglia) showed impaired calcium handling upon depolarisation and reduced mitochondrial membrane potential. Finally, lysosomes were smaller, soma lysosome content was decreased and importantly, lysosome acidity was impaired in sensory neurons, all of which are novel findings in WS. We validated these findings using two separate publicly available datasets, both from WS patient fibroblast-derived neural stem cells. We observed a highly significant functional enrichment of GO cellular component lysosome-related terms among the differentially expressed proteins and genes, with the majority of lysosome-related proteins being downregulated. These data reveal extensive impairments in the trigeminal pathway and nociceptive neurons in WS that may contribute to trigeminal and sensory symptoms observed in patients. Moreover, we note that mutations in WFS1 are relatively common and, given the importance of WFS1 for sensory function, our data may also shed light on sensory impairments in general.
Related Topics
- Type
- article
- Language
- en
- Landing Page
- https://doi.org/10.1016/j.expneurol.2024.115099
- OA Status
- hybrid
- References
- 72
- Related Works
- 10
- OpenAlex ID
- https://openalex.org/W4405185559
Raw OpenAlex JSON
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https://openalex.org/W4405185559Canonical identifier for this work in OpenAlex
- DOI
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https://doi.org/10.1016/j.expneurol.2024.115099Digital Object Identifier
- Title
-
Early trigeminal and sensory impairment and lysosomal dysfunction in accurate models of Wolfram syndromeWork title
- Type
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articleOpenAlex work type
- Language
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enPrimary language
- Publication year
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2024Year of publication
- Publication date
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2024-12-09Full publication date if available
- Authors
-
Kerli Tulva, Aleksander Pirajev, Akbar Zeb, Asya Esin Aksoy, Ajediran Bello, Benjamin Lee, Baldvin F Guðjónsson, Sigridur B Helgadottir, Toomas Jagomäe, Andrea García‐Llorca, Þór Eysteinsson, Monika Jürgenson, Mario Plaas, Eero Vasar, Allen Kaasik, Miriam A. HickeyList of authors in order
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https://doi.org/10.1016/j.expneurol.2024.115099Publisher landing page
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YesWhether a free full text is available
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hybridOpen access status per OpenAlex
- OA URL
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https://doi.org/10.1016/j.expneurol.2024.115099Direct OA link when available
- Concepts
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Neuroscience, Sensory system, Medicine, Wolfram syndrome, Physical medicine and rehabilitation, Audiology, Psychology, Internal medicine, AtrophyTop concepts (fields/topics) attached by OpenAlex
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0Total citation count in OpenAlex
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72Number of works referenced by this work
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10Other works algorithmically related by OpenAlex
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| referenced_works_count | 72 |
| abstract_inverted_index.a | 4, 98, 107, 218 |
| abstract_inverted_index.GO | 224 |
| abstract_inverted_index.It | 19 |
| abstract_inverted_index.WS | 61, 136, 210, 257 |
| abstract_inverted_index.We | 126, 198, 216 |
| abstract_inverted_index.at | 116 |
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| abstract_inverted_index.we | 70, 270 |
| abstract_inverted_index.MRI | 88 |
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| abstract_inverted_index.WS. | 80, 102, 155, 197 |
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| abstract_inverted_index.sensory | 76, 146, 188, 264, 286, 295 |
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| abstract_inverted_index.fibroblast-derived | 212 |
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