Gene mutations in a Han Chinese Alzheimer's disease cohort

Ma, Limin; Zhang, Jiewen; Shi, Yingying; Wang, Wan; Ren, Zhixia; Xia, Mingrong; Zhang, Yuanxing; Yang, Miaomiao

doi:10.1002/brb3.1180

Cited by 10 publications

(14 citation statements)

References 37 publications

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“…The mutation frequency is lower in our cohort than reported in Caucasians; 17 of 129 (13.2%) young‐onset AD patients had PSEN1 mutations in a previous study (Lanoiselee et al, 2017). However, the mutation frequency in our cohort is higher than those conducted in a previous Chinese study with 1 of 108 young‐onset and familial AD patients (0.9%) had PSEN1 mutations (Ma et al, 2019). The variant c.G438A (p.M146I) in PSEN1 is potentially a mutation hot spot, as it contributes to three‐fourths of young‐onset AD patients having a PSEN1 mutation.…”

Section: Discussioncontrasting

confidence: 79%

Genetic study ofyoung‐onsetdementia using targeted gene panel sequencing in Taiwan

Hsu

Lin

Chen

et al. 2021

American J of Med Genetics Pt B

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Recent genetic progress allows the molecular diagnosis of young‐onset dementia, including Alzheimer's disease (AD) and frontotemporal dementia (FTD). We aimed to identify the mutational and clinical spectra of causal genes in a Taiwanese cohort of young‐onset dementia. Ninety‐one patients with young‐onset dementia and 22 age/gender‐matched controls were recruited. Genetic causes were identified by a targeted panel containing 90 causative genes for AD, FTD, and related neurodegenerative disorders. Plasma biomarkers, including total tau, Aβ42, and Aβ40, were assayed. Molecular amyloid and tau PET scans were performed in some patients carrying mutations. Nine of 52 patients (17.3%) with young‐onset AD had mutations: 2 (22.2%), 4 (44.5%), 2 (22.2%), and 1 (11.1%) in APP, PSEN1, PSEN2, and TREM2, respectively. Two of 33 patients (6.1%) with young‐onset FTD had mutations in MAPT and LRRK2. Three of the 6 patients (50.0%) with possible FTD combined with other neurodegenerative disorders had individual mutations in APP, PSEN2, or MAPT. Patients with PSEN1 mutations had earlier onset of disease than those without mutations (p = .02). Plasma level of total tau was increased and Aβ42 and Aβ40 levels decreased in all groups of dementia patients compared to controls. Our findings provide a genetic spectrum of young‐onset dementia in our population.

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Section: Discussioncontrasting

confidence: 79%

Genetic study ofyoung‐onsetdementia using targeted gene panel sequencing in Taiwan

Hsu

Lin

Chen

et al. 2021

American J of Med Genetics Pt B

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“…The patient showed symptoms of cognitive decline and memory impairment, as well as atypical neurological symptoms [64]. The p.H169N mutation of PSEN2 reported by Ma et al has also been detected in both AD and FTD patients, in support of the previous finding by Shi et al [58,63]. A known PSEN2 mutation (p.V139M) which was first reported in an Italian LOAD patient, was observed in a Chinese patient with early-onset disease phenotypes [39,73].…”

Section: Psen2supporting

confidence: 76%

“…Structural analyses indicated that these mutations might induce structural alterations in γ-secretases due to the change in interaction patterns, thereby participating in the pathogenesis of FAD [40]. The p.L226R mutation of PSEN1, which is located at the transmembrane domain of the protein, was reported in an EOAD family characterized by language impairment at disease onset [58]. In a whole-exome sequencing study on 15 Chinese FAD patients, Jiang et al identified six previously reported PSEN1 mutations in all subjects, including p.M139I, p.T147I, p.L173W, p.F177S, p.R269H, and p.R157S [39].…”

Section: Psen1mentioning

confidence: 99%

“…The p.V391G mutation in PSEN1 was found to be responsible for EOAD with extrapyramidal symptoms according to a study on a very early-onset AD proband in China [63]. Li and colleagues performed Sanger sequencing on PSEN1 in three Chinese EOAD families and discovered two novel mutations (p.Y256N and p.H214R) in AD families and a de novo mutation (p.G206V) in a patient with very early-onset sporadic AD [58]. The three mutations might contribute to the pathogenesis of EOAD [58,62,63].…”

Section: Psen1mentioning

confidence: 99%

“…Li and colleagues performed Sanger sequencing on PSEN1 in three Chinese EOAD families and discovered two novel mutations (p.Y256N and p.H214R) in AD families and a de novo mutation (p.G206V) in a patient with very early-onset sporadic AD [58]. The three mutations might contribute to the pathogenesis of EOAD [58,62,63]. A study on an FAD patient cohort in China was conducted by Gao et al recently, which showed that PSEN1 mutations account for the largest proportion of FAD patients, and three novel mutations in PSEN1, namely p.M139L, p.V103G, and p.F177V, were identified in the study [40].…”

Section: Psen1mentioning

confidence: 99%

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The Genetics of Alzheimer’s Disease in the Chinese Population

Gan

Zhang

Lee

2020

IJMS

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Alzheimer’s disease (AD) is a neurodegenerative disease characterized by progressive cognitive dysfunction and behavioral impairment. In China, the number of AD patients is growing rapidly, which poses a considerable burden on society and families. In recent years, through the advancement of genome-wide association studies, second-generation gene sequencing technology, and their application in AD genetic research, more genetic loci associated with the risk for AD have been discovered, including KCNJ15, TREM2, and GCH1, which provides new ideas for the etiology and treatment of AD. This review summarizes three early-onset AD causative genes (APP, PSEN1, and PSEN2) and some late-onset AD susceptibility genes and their mutation sites newly discovered in China, and briefly introduces the potential mechanisms of these genetic susceptibilities in the pathogenesis of AD, which would help in understanding the genetic mechanisms underlying this devastating disease.

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