CCNF基因突变引起的行为变异性额颞叶痴呆:一例报告。

Feng-Ling You, Gao-Fu Xia, Jing Cai
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引用次数: 0

摘要

背景:额叶、颞叶痴呆(FTD)和肌萎缩侧索硬化症(ALS)是致命的神经退行性疾病。研究发现,在家族性和散发性ALS和FTD患者中发现了CCNF突变。行为变异性额颞叶痴呆(bvFTD)是一种以人格、社会行为和认知功能逐渐恶化为特征的临床综合征,与遗传因素关系最为密切。由于bvFTD的早期症状高度异质,这种情况经常被误诊为阿尔茨海默病或精神障碍。在这项研究中,一名bvFTD患者的CCNF基因发生突变,导致泛素化蛋白积累,最终导致神经退行性疾病。bvFTD患者及其家属的基因检测亟待改进,为额颞叶痴呆的早期诊断提供临床参考。病例介绍:本例患者65岁,发病隐匿,早发性记忆丧失,情节记忆显著下降,早期诊断为AD,口服盐酸多奈哌齐3年疗效不佳,随后改为口服盐酸美金刚片,病情控制数月。他的药物被换成了低聚甘露糖钠胶囊,他的病情逐渐得到控制,但没有观察到明显的改善。自发停药后,患者病情进展迅速;因此,他访问了我们的医院,并接受了中度至重度认知障碍的神经心理测试。AD脑脊液标志物无明显异常,颅骨MRI显示额颞叶萎缩和海马体积减少。对CCNF基因存在的遗传测试显示了c.1532C>a(p.T511N)杂合变体,这可能是bvFTD的诊断标准。因此,患者的症状在多奈哌齐、盐酸美金刚口服片和低聚甘露糖钠联合治疗后短暂好转后复发,但其总体情况与之前相比有所改善,并且在随访期间继续观察该治疗方案的变化。结论:bvFTD的早期临床表现复杂多变,而且这种情况很容易被误诊,从而延误治疗。因此,对于临床上高度怀疑FTD的患者,除了详细了解他们的病史和家族史并改进相关检查外,还应尽早进行基因检测,以帮助确认诊断。对于与基因密切相关的疾病,应尽可能优化其他家庭成员的基因检测,以便进行早期诊断和干预,并指导下一代的生育能力。
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Behavioural Variant Frontotemporal Dementia due to CCNF Gene Mutation: A Case Report.

Background: Frontal, temporal lobe dementia (FTD) and amyotrophic lateral sclerosis (ALS) are fatal neurodegenerative diseases. Studies have found that CCNF mutations have been found in patients with familial and sporadic ALS and FTD. Behavioural variant frontotemporal dementia (bvFTD) is a clinical syndrome characterized by progressive deterioration of personality, social behaviour, and cognitive function, which is most closely related to genetic factors. As the early symptoms of bvFTD are highly heterogeneous, the condition is often misdiagnosed as Alzheimer's disease or psychiatric disorders. In this study, a bvFTD patient had a CCNF gene mutation, which led to ubiquitinated protein accumulation and ultimately caused neurodegenerative disease. Genetic detection should be improved urgently for bvFTD patients and family members to provide a clinical reference for early diagnosis of frontotemporal dementia.

Case presentation: In this case, the patient was 65 years old with an insidious onset, early-onset memory loss, a significant decline in the episodic memory, an early AD diagnosis, and oral treatment with donepezil hydrochloride for 3 years with poor efficacy, followed by a change to oral memantine hydrochloride tablets, which controlled the condition for several months. His medication was switched to sodium oligomannate capsules, and his condition was gradually controlled, but no significant improvement was observed. After spontaneous drug withdrawal, the patient's condition progressed rapidly; therefore, he visited our hospital and underwent neuropsychological tests for moderate to severe cognitive impairment. AD cerebrospinal fluid markers showed no significant abnormalities, and cranial MRI revealed frontotemporal lobe atrophy and decreased hippocampal volume. Genetic testing for the presence of the CCNF gene revealed a c.1532C > A (p. T511N) heterozygous variant, which might be a diagnostic criterion for bvFTD. Therefore, the patient's symptoms recurred after transient improvement with the combination of donepezil, oral memantine hydrochloride tablets, and sodium oligomannate, but his overall condition was improved compared to that before, and this treatment regimen was continued to observe changes during the follow-up.

Conclusion: The early clinical manifestations of bvFTD are complex and variable, and the condition is easily misdiagnosed, thus delaying treatment. Therefore, for patients with a high clinical suspicion of FTD, in addition to a detailed understanding of their medical history and family history and improvement of relevant examinations, genetic testing should be performed as early as possible to help confirm the diagnosis. For diseases closely related to genes, genetic testing of other family members should be optimised as much as possible to allow early diagnosis and intervention and guide fertility in the next generation.

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