| Literature DB >> 32602554 |
Zhiyong Chen1, Zheyu Xu1, Qianhui Cheng2, Yi Jayne Tan1, Helen L Ong3, Yi Zhao3, Weng Khong Lim4,5, Jing Xian Teo4, Jia Nee Foo6,7, Hwei Yee Lee8, Jeanne M M Tan1, Liting Hang7, Wai-Yung Yu2, Simon K S Ting9, Eng-King Tan10,9, Tchoyoson C C Lim2, Adeline S L Ng1,10.
Abstract
Neuronal intranuclear inclusion disease (NIID) is a neurodegenerative disorder associated with GGC repeats of >60 to 500 copies in the 5'-untranslated region of NOTCH2NLC. The clinical and genetic characterization of NIID outside of East Asia remains unknown. We identified twelve patients who underwent genetic testing using long-read sequencing or repeat primed polymerase chain reaction. All were positive for a GGC repeat expansion; the median repeat length was 107 (range 92-138). Ten were Chinese and two of Malay ethnicity. Age at onset ranged from 50 to 69 years. Eight (66.7%) patients had dementia, while four (33.3%) patients were oligosymptomatic, without typical NIID symptoms of dementia, Parkinsonism, or muscle weakness. GGA interruptions within the GGC expansion were present in four patients; the number of GGA interruptions was highest (6.71%) in the patient with the earliest age at onset (50 years). Median plasma neurofilament light level was 47.3 pg/mL in seven patients (range 26-380 pg/mL). The highest level (380 pg/mL) was found in one patient who experienced an encephalitic episode. Overall, we describe a cohort of genetically confirmed NIID patients from Southeast Asia and provide further information that the presence of GGA interruptions within GGC repeat expansions may serve as a potential genetic modifier in NIID.Entities:
Keywords: GGC repeat expansion; NOTCH2NLC; diffusion-weighted imaging; neurofilament light; neuronal intranuclear inclusion disease
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Year: 2020 PMID: 32602554 DOI: 10.1111/cge.13802
Source DB: PubMed Journal: Clin Genet ISSN: 0009-9163 Impact factor: 4.438