A novel splice‐site mutation in <scp>CHMP2B</scp> associated with frontotemporal dementia: The first report from China and literature review

Li, Chang; Wen, Ya; Zhao, Ming; Wang, Yaye; Li, Ping; Wang, L.; Wang, S.H.

doi:10.1002/mgg3.2222

Molec Gen & Gen Med

2023

DOI: 10.1002/mgg3.2222

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A novel splice‐site mutation in CHMP2B associated with frontotemporal dementia: The first report from China and literature review

Chang Li

Ya Wen

Ming Zhao³

et al.

Abstract: BackgroundFrontotemporal dementia (FTD) has genetic heterogeneity, and the endosomal ESCRTIII‐complex subunit CHMP2B variant is a rare cause of FTD. The mutations in CHMP2B were first identified in a large Danish pedigree with autosomal dominant FTD, and have also been found in several individuals from Belgium, France, the United States, and Türkiye. In the Chinese population, cases of CHMP2B variant‐associated FTD have never been reported.MethodsThe spectrum of clinical symptoms and the genetic analysis of th… Show more

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Cited by 2 publications

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A novel splice‐site mutation in CHMP2B associated with frontotemporal dementia: The first report from China and literature review

Wen

Zhao³

et al. 2023

Molec Gen & Gen Med

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BackgroundFrontotemporal dementia (FTD) has genetic heterogeneity, and the endosomal ESCRTIII‐complex subunit CHMP2B variant is a rare cause of FTD. The mutations in CHMP2B were first identified in a large Danish pedigree with autosomal dominant FTD, and have also been found in several individuals from Belgium, France, the United States, and Türkiye. In the Chinese population, cases of CHMP2B variant‐associated FTD have never been reported.MethodsThe spectrum of clinical symptoms and the genetic analysis of the presented patient were identified and investigated. Besides this case, we assessed previously reported cases with CHMP2B gene mutations.ResultsThis study presents a Chinese patient harboring a novel heterozygous A‐to‐T variant (NM_014043:c.532‐2A>T) in CHMP2B with a phenotype compatible with FTD. Although previous reports suggested cases of CHMP2B variant‐associated FTD initially presented with personality changes and stereotypical movements at the age of 50, this case was characterized by psychosis involving delusion of persecution, auditory hallucination, and suspiciousness at the earlier onset age of 44. Minigene splicing assay revealed that the splice‐site variant could result in the retention of intron 5.ConclusionThis is the first case of CHMP2B variant‐associated FTD reported in the Chinese population. The novel c.532‐2A>T variant in the acceptor splice site of exon 6 retaining intron 5 was predicted to cause truncated protein and protein conformation changes. This discovery may expand the genetic and phenotypic spectrum of CHMP2B variant‐associated FTD.

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A novel splice‐site mutation in CHMP2B associated with frontotemporal dementia: The first report from China and literature review

Wen

Zhao³

et al. 2023

Molec Gen & Gen Med

Self Cite

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Frontotemporal-TDP and LATE Neurocognitive Disorders: A Pathophysiological and Genetic Approach

Ortiz,

Ramírez-Jirano,

Arizaga

et al. 2023

Brain Sciences

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Frontotemporal lobar degeneration (FTLD) belongs to a heterogeneous group of highly complex neurodegenerative diseases and represents the second cause of presenile dementia in individuals under 65. Frontotemporal-TDP is a subgroup of frontotemporal dementia characterized by the aggregation of abnormal protein deposits, predominantly transactive response DNA-binding protein 43 (TDP-43), in the frontal and temporal brain regions. These deposits lead to progressive degeneration of neurons resulting in cognitive and behavioral impairments. Limbic age-related encephalopathy (LATE) pertains to age-related cognitive decline primarily affecting the limbic system, which is crucial for memory, emotions, and learning. However, distinct, emerging research suggests a potential overlap in pathogenic processes, with some cases of limbic encephalopathy displaying TDP-43 pathology. Genetic factors play a pivotal role in both disorders. Mutations in various genes, such as progranulin (GRN) and chromosome 9 open reading frame 72 (C9orf72), have been identified as causative in frontotemporal-TDP. Similarly, specific genetic variants have been associated with an increased risk of developing LATE. Understanding these genetic links provides crucial insights into disease mechanisms and the potential for targeted therapies.

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A novel splice‐site mutation in CHMP2B associated with frontotemporal dementia: The first report from China and literature review

Cited by 2 publications

References 26 publications

A novel splice‐site mutation in CHMP2B associated with frontotemporal dementia: The first report from China and literature review

A novel splice‐site mutation in CHMP2B associated with frontotemporal dementia: The first report from China and literature review

Frontotemporal-TDP and LATE Neurocognitive Disorders: A Pathophysiological and Genetic Approach

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