Your search keyword '"Tian-Xinyu Xia"' showing total 3 results

1. Clinical profile of fatal familial insomnia: phenotypic variation in 129 polymorphisms and geographical regions

Author

Min Chu, Yue Cui, Liyong Wu, Jiali Meng, Zhuyi Jiang, Junjie Li, Hong Ye, Yang-Mingyue Ji, Wang Xin, Li Liu, Dong-Xin Wang, Jing Zhang, Haihan Yan, Lin Wang, Tian-Xinyu Xia, Kexin Xie, ZiChen Tian, and Ye Zhao

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Genotype, Population, Insomnia, Fatal Familial, Polymorphism, Single Nucleotide, Prion Proteins, Young Adult, Internal medicine, Humans, Medicine, Risk factor, education, Allele frequency, Aged, Genetic testing, Fatal familial insomnia, education.field_of_study, medicine.diagnostic_test, business.industry, Middle Aged, medicine.disease, Genotype frequency, Psychiatry and Mental health, Phenotype, Mutation, Female, Surgery, Neurology (clinical), Age of onset, business

Abstract

ObjectiveElucidate the core clinical and genetic characteristics and identify the phenotypic variation between different regions and genotypes of fatal familial insomnia (FFI).MethodsA worldwide large sample of FFI patients from our case series and literature review diagnosed by genetic testing were collected. The prevalence of clinical symptoms and genetic profile were obtained, and then the phenotypic comparison between Asians versus non-Asians and 129Met/Met versus 129Met/Val were conducted.ResultsIn total, 131 cases were identified. The age of onset was 47.51±12.53 (range 17–76) years, 106 patients died and disease duration was 13.20±9.04 (range 2–48) months. Insomnia (87.0%) and rapidly progressive dementia (RPD; 83.2%) occurred with the highest frequency. Hypertension (33.6%) was considered to be an objective indicator of autonomic dysfunction. Genotype frequency at codon 129 was Met/Met (84.7%) and Met/Val (15.3%), and allele frequency was Met (92.4%) and Val (7.6%).129 Met was a risk factor (OR: 3.728, 95% CI: 2.194 to 6.333, p=0.000) for FFI in the non-Asian population. Comparison of Asians and non-Asians revealed clinical symptoms and genetic background to show some differences (pConclusionsInsomnia, RPD and hypertension are representative key clinical presentations of FFI. Phenotypic variations in genotypes and geographic regions were documented. Prion protein gene 129 Met was considered to be a risk factor for FFI in the non-Asian population, and 129 polymorphisms could modify survival duration.

Published

2021

2. Clinical profile of fatal familial insomnia: phenotypic variation in 129 polymorphisms and geographical regions.

Author

Jing Zhang, Min Chu, ZiChen Tian, KeXin Xie, Yue Cui, Li Liu, JiaLi Meng, HaiHan Yan, Yang-Mingyue Ji, Zhuyi Jiang, Tian-Xinyu Xia, Dongxin Wang, Xin Wan, Ye Zhao, Hong Ye, Junjie Li, Lin Wang, Liyong Wu, Zhang, Jing, and Chu, Min

Subjects

PHENOTYPIC plasticity, GENETIC profile, GENETIC testing, INSOMNIA, SYMPTOMS, DYSAUTONOMIA, DISEASE duration, RESEARCH, GENETIC mutation, GENETIC polymorphisms, EVALUATION research, COMPARATIVE studies, GENOTYPES, PHENOTYPES

Abstract

Objective: Elucidate the core clinical and genetic characteristics and identify the phenotypic variation between different regions and genotypes of fatal familial insomnia (FFI).Methods: A worldwide large sample of FFI patients from our case series and literature review diagnosed by genetic testing were collected. The prevalence of clinical symptoms and genetic profile were obtained, and then the phenotypic comparison between Asians versus non-Asians and 129Met/Met versus 129Met/Val were conducted.Results: In total, 131 cases were identified. The age of onset was 47.51±12.53 (range 17-76) years, 106 patients died and disease duration was 13.20±9.04 (range 2-48) months. Insomnia (87.0%) and rapidly progressive dementia (RPD; 83.2%) occurred with the highest frequency. Hypertension (33.6%) was considered to be an objective indicator of autonomic dysfunction. Genotype frequency at codon 129 was Met/Met (84.7%) and Met/Val (15.3%), and allele frequency was Met (92.4%) and Val (7.6%).129 Met was a risk factor (OR: 3.728, 95% CI: 2.194 to 6.333, p=0.000) for FFI in the non-Asian population. Comparison of Asians and non-Asians revealed clinical symptoms and genetic background to show some differences (p<0.05). In the comparison of 129 polymorphisms, a longer disease duration was found in the 129 MV group, with alleviation of some clinical symptoms (p<0.05). After considering survival probability, significant differences in survival time between genotypes remained (p<0.0001).Conclusions: Insomnia, RPD and hypertension are representative key clinical presentations of FFI. Phenotypic variations in genotypes and geographic regions were documented. Prion protein gene 129 Met was considered to be a risk factor for FFI in the non-Asian population, and 129 polymorphisms could modify survival duration. [ABSTRACT FROM AUTHOR]

Published

2022

3. Three novel mutations in Chinese patients with CSF1R-related leukoencephalopathy

Author

Min Chu, Chaodong Wang, Tian-Xinyu Xia, Jing Zhang, Aihong Zhou, Kexin Xie, Yue Cui, Yu Kong, Ran Gao, Dong-Xin Wang, Li Liu, and Liyong Wu

Subjects

medicine.medical_specialty, Molecular pathology, business.industry, Leukodystrophy, Encephalopathy, General Medicine, Disease, medicine.disease, Leukoencephalopathy, Internal medicine, medicine, Medical genetics, Hereditary diffuse leukoencephalopathy with spheroids, Original Article, Family history, business

Abstract

Background CSF1R-related encephalopathy refers to adult-onset leukodystrophy with neuroaxonal spheroids and pigmented glia (ALSP) due to CSF1R mutations, which is a rare autosomal dominant white matter disease including two pathological entities, hereditary diffuse leukoencephalopathy with spheroids (HDLS) and pigmentary orthochromatic leukodystrophy (POLD). The aim of this study was to identify additional causative mutations in the CSF1R gene and clarify their pathogenic effects. Methods Whole-exome sequencing was conducted for nine Chinese patients diagnosed with possible ALSP based on clinical and neuroimaging findings from March 2014 to June 2020 at Xuanwu Hospital (Beijing, China). Variant pathogenicity was assessed according to the American College of Medical Genetics and Genomics and Association for Molecular Pathology (ACMG/AMP) Standards and Guidelines. Results Mean ± standard deviation (range) age of disease onset in the nine patients was 39.22±9.63 [25-54] years. Four of the nine patients were male, and four out of nine had a remarkable family history. Seven CSF1R mutations were identified in the nine patients; four (p.G17C, p.R579Q, p.I794T and c.2909_2910insATCA) have been previously reported, while three (p.V613L, p.W821R and c.2442+2_2442+3dupT) were novel. Of the latter, two (p.V613L and p.W821R) were likely pathogenic and 1 (c.2442+2_2442+3dupT) was of uncertain significance according to ACMG/AMP criteria. Conclusions These findings expand the mutational spectrum of ALSP and provide a basis for future investigations on etiologic factors and potential management strategies for this disease.

Published

2021