Cognitive Decline and Other Late-Stage Neurologic Complications in Cockayne Syndrome.

IF 2.3 Q3 CLINICAL NEUROLOGY Neurology. Clinical practice Pub Date : 2024-08-01 Epub Date: 2024-05-16 DOI:10.1212/CPJ.0000000000200309

Geetanjali Rajamani, Seth A Stafki, Audrey L Daugherty, William G Mantyh, Hannah R Littel, Christine C Bruels, Christina A Pacak, Paul D Robbins, Laura J Niedernhofer, Adesoji Abiona, Paola Giunti, Shehla Mohammed, Vincent Laugel, Peter B Kang

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Abstract

Background and objectives: Cockayne syndrome (CS) is an ultra-rare, autosomal recessive, premature aging disorder characterized by impaired growth, neurodevelopmental delays, neurodegeneration, polyneuropathy, and other multiorgan system complications. The anatomic aspects of CS neurodegeneration have long been known from postmortem examinations and MRI studies, but the clinical features of this neurodegeneration are not well characterized, especially at later stages of the disease.

Methods: This was a retrospective observational study in which individuals with CS who survived beyond 18 years were ascertained at 3 centers in the United States, France, and the United Kingdom. Medical records were examined to determine the frequencies and features of the following neurologic complications: neurocognitive/neuropsychiatric decline (8 symptoms), tremors, neuropathy, seizures, and strokes.

Results: Among 18 individuals who met inclusion criteria, all but one (94.4%) experienced at least one symptom of neurocognitive/neuropsychiatric decline, with most individuals experiencing at least half of those symptoms. Most participants experienced tremors and peripheral neuropathy, with a few experiencing seizures and strokes. For individuals with available data, 100.0% were reported to have gait ataxia and neuroimaging showed that 85.7% had generalized cerebral atrophy on MRI while 78.6% had white matter changes.

Discussion: Symptoms of neurocognitive/neuropsychiatric decline are nearly universal in our cohort of adults with CS, suggesting that these individuals are at risk of developing neurocognitive/neuropsychiatric decline, with symptoms related to but not specific to dementia. Considering the prominent role of DNA repair defects in CS disease mechanisms and emerging evidence for increased DNA damage in neurodegenerative disease, impaired genome maintenance may be a shared pathway underlying multiple forms of neurocognitive/neuropsychiatric decline. Components of the DNA damage response mechanism may bear further study as potential therapeutic targets that could alleviate neurocognitive/neuropsychiatric symptoms in CS and other neurodegenerative disorders.

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科凯恩综合征的认知功能衰退及其他晚期神经并发症。

背景和目的：科凯恩综合征（Cockayne Syndrome，CS）是一种超罕见的常染色体隐性早衰性疾病，其特征是生长发育障碍、神经发育迟缓、神经变性、多发性神经病和其他多器官系统并发症。人们很早就从尸检和核磁共振成像研究中了解到 CS 神经变性的解剖学特征，但这种神经变性的临床特征并不十分明确，尤其是在疾病的晚期：这是一项回顾性观察研究，在美国、法国和英国的 3 个中心对存活超过 18 年的 CS 患者进行了调查。研究人员检查了病历，以确定以下神经系统并发症的发生频率和特征：神经认知/神经精神衰退（8 种症状）、震颤、神经病变、癫痫发作和中风：在符合纳入标准的 18 人中，除一人（94.4%）外，其他人都出现了至少一种神经认知/神经精神衰退症状，其中大多数人至少出现了一半的症状。大多数参与者出现震颤和周围神经病变，少数人出现癫痫发作和中风。有数据显示，100.0%的患者有步态共济失调，神经影像学检查显示，85.7%的患者有全身性脑萎缩，78.6%的患者有白质改变：讨论：在我们的成人 CS 患者队列中，神经认知/神经精神衰退的症状几乎普遍存在，这表明这些人面临着神经认知/神经精神衰退的风险，其症状与痴呆有关，但并非痴呆的特异性症状。考虑到DNA修复缺陷在CS疾病机制中的突出作用，以及神经退行性疾病中DNA损伤增加的新证据，基因组维护受损可能是多种形式的神经认知/神经精神衰退的共同途径。DNA 损伤反应机制的组成部分可能值得进一步研究，因为这些潜在的治疗靶点可以减轻 CS 和其他神经退行性疾病的神经认知/神经精神症状。

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来源期刊

Neurology. Clinical practice CLINICAL NEUROLOGY-

CiteScore

4.00

自引率

0.00%

发文量

期刊介绍： Neurology® Genetics is an online open access journal publishing peer-reviewed reports in the field of neurogenetics. The journal publishes original articles in all areas of neurogenetics including rare and common genetic variations, genotype-phenotype correlations, outlier phenotypes as a result of mutations in known disease genes, and genetic variations with a putative link to diseases. Articles include studies reporting on genetic disease risk, pharmacogenomics, and results of gene-based clinical trials (viral, ASO, etc.). Genetically engineered model systems are not a primary focus of Neurology® Genetics, but studies using model systems for treatment trials, including well-powered studies reporting negative results, are welcome.