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神经元蜡样脂褐质沉积症相关疾病:儿童期痴呆的常见病因

NCL Disorders: Frequent Causes of Childhood Dementia.

作者信息

Schulz Angela, Kohlschütter Alfried

机构信息

Professor of Pediatrics Department of Pediatrics, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.

出版信息

Iran J Child Neurol. 2013 Winter;7(1):1-8.

Abstract

Dementia in children or young adults is most frequently caused by neuronal ceroidlipofuscinoses (NCL), a group of incurable lysosomal storage disorders linked by the accumulation of a characteristic intracellular storage material and progressive clinical deterioration, usually in combination with visual loss, epilepsy, and motor decline. The clinical characteristics can vary and the age at disease onset ranges from birth to over 30 years. Diagnosis of an NCL is difficult because of genetic heterogeneity with14 NCL forms (CLN1-CLN14) identified and a high phenotype variability. A new classification of the disorders is based on the affected gene and the age at disease onset and allows a precise and practicable delineation of every NCL disease. We present a clear diagnostic algorithm to identify each NCL form. A precise diagnosis is essential for genetic counseling of affected families and for optimizing palliative care. As patient management profits from recognizing characteristic complications, care supported by a specialized team of NCL clinicians is recommended. The development of curative therapies remains difficult as the underlying pathophysiological mechanism remains unclear for all NCL forms.

摘要

儿童或青年期的痴呆最常见于神经元蜡样脂褐质沉积症(NCL),这是一组无法治愈的溶酶体贮积症,其特征在于细胞内蓄积一种特殊的贮积物质,并伴有进行性临床恶化,通常还伴有视力丧失、癫痫和运动功能减退。临床特征各不相同,发病年龄从出生到30多岁不等。由于存在遗传异质性(已鉴定出14种NCL类型,即CLN1-CLN14)且表型高度可变,NCL的诊断颇具难度。该疾病的新分类基于受影响的基因和发病年龄,能够对每种NCL疾病进行精确且实用的界定。我们提出了一种清晰的诊断算法以识别每种NCL类型。精确诊断对于为受影响家庭提供遗传咨询以及优化姑息治疗至关重要。鉴于识别特征性并发症有助于患者管理,建议由专业的NCL临床医生团队提供护理支持。由于所有NCL类型的潜在病理生理机制仍不清楚,治愈性疗法的研发依然困难重重。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ce43/3943077/79df0a9a0197/ijcn-7-001-g001.jpg

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