angiogenin and Cognition-Disorders

angiogenin has been researched along with Cognition-Disorders* in 2 studies

Other Studies

2 other study(ies) available for angiogenin and Cognition-Disorders

Article	Year
Comparison of the clinical and cognitive features of genetically positive ALS patients from the largest tertiary center in Serbia. Journal of neurology, 2017, Volume: 264, Issue:6 Discovering novel mutations in C9orf72, FUS, ANG, and TDP-43 genes in ALS patients arises necessities for better clinical characterizations of these subjects. The aim is to determine clinical and cognitive profile of genetically positive Serbian ALS patients. 241 ALS patients were included in the study (17 familiar and 224 apparently sporadic). The following genes were analyzed: SOD1, C9orf72, ANG, FUS, and TDP-43. An extensive battery of classic neuropsychological tests was used in 27 ALS patients (22 SOD1 positive and 5 SOD1 negative) and 82 healthy controls (HCs). Overall 37 (15.4%) of 241 ALS patients carried mutations in tested genes-among 17 familiar ALS patients 16 (94.1%) were positive and among 224 apparently sporadic 21 (9.4%) had causative mutation. Mutations in SOD1 gene were the most common, representing 27 (73.0%) of all genetically positive ALS patients. The main clinical characteristics of SOD1 positive patients were: spinal onset in lower extremities, common sphincter and sensitive disturbances, and dysexecutive syndrome. Within SOD1 positive patients, we noticed somewhat earlier onset in patients with A145G, sensory and sphincter disturbances were dominant in patients with L144F, while D90A patients had significant sensory involvement. SOD1 negative group consisted of ten (27.0%) patients (six C9orf72, two ANG, one TDP-43, and one patient baring triple FUS, C9orf72 expansion, and ANG variants). Bulbar involvement and more extensive neuropsychological impairment (including executive, visuospatial, and memory difficulties) were the main features of SOD1 negative cohort. Our results suggest that meaningful clinical suspicion of certain ALS genotype might be made based on thorough clinical evaluation of patients. Topics: Amyotrophic Lateral Sclerosis; C9orf72 Protein; Cognition Disorders; Cohort Studies; Disability Evaluation; DNA-Binding Proteins; Female; Genetic Association Studies; Genetic Testing; Humans; Male; Mutation; Neuropsychological Tests; Ribonuclease, Pancreatic; RNA-Binding Protein FUS; Serbia; Superoxide Dismutase-1; Tertiary Care Centers	2017
FUS mutations in amyotrophic lateral sclerosis: clinical, pathological, neurophysiological and genetic analysis. Journal of neurology, neurosurgery, and psychiatry, 2010, Volume: 81, Issue:6 FUS gene mutations were recently identified in familial amyotrophic lateral sclerosis (ALS). The present studies sought to define the clinical, post-mortem and neurophysiological phenotypes in ALS families with FUS mutations and to determine the frequency of FUS mutations in familial and sporadic ALS.. FUS was screened for mutations in familial and sporadic ALS cases. Clinical, post-mortem and neurophysiological features of large families with FUS mutations are described.. FUS mutations were evident in 3.2% (4/124) of familial ALS, representing the second most common gene abnormality to be described in familial ALS after SOD1. No mutations were present in 247 sporadic ALS cases. The clinical presentation in 49 affected patients was consistent with a predominantly lower motor neuron disorder, supported by post-mortem findings. Upper motor neuron involvement varied, with Wallerian degeneration of corticospinal tracts present in one post-mortem case but absent in a second case from the same family. Features of cortical hyperexcitability demonstrated upper motor neuron involvement consistent with other forms of familial and sporadic ALS. One case presented with frontotemporal dementia (FTD) indicating that this may be a rare presenting feature in families with FUS mutation. Ubiquitin-positive cytoplasmic skein-like inclusions were present in lower motor neurons, but in contrast to sporadic ALS, no TDP-43 pathology was evident. Mutation-specific clinical features were identified. Patients with a R521C mutation were significantly more likely to develop disease at a younger age, and dropped-head syndrome was a frequent feature. Reduced disease penetrance was evident among most affected families. Topics: Adult; Aged; Amyotrophic Lateral Sclerosis; Brain; Cognition Disorders; DNA Mutational Analysis; DNA-Binding Proteins; Dynactin Complex; Endosomal Sorting Complexes Required for Transport; Female; Genetic Testing; Humans; Male; Microtubule-Associated Proteins; Middle Aged; Nerve Tissue Proteins; Neuropsychological Tests; Point Mutation; Ribonuclease, Pancreatic; RNA-Binding Protein FUS; RNA, Messenger; Severity of Illness Index; Superoxide Dismutase; Superoxide Dismutase-1; Vesicular Transport Proteins; Young Adult	2010

Article

Year

Comparison of the clinical and cognitive features of genetically positive ALS patients from the largest tertiary center in Serbia.

Journal of neurology, 2017, Volume: 264, Issue:6

Discovering novel mutations in C9orf72, FUS, ANG, and TDP-43 genes in ALS patients arises necessities for better clinical characterizations of these subjects. The aim is to determine clinical and cognitive profile of genetically positive Serbian ALS patients. 241 ALS patients were included in the study (17 familiar and 224 apparently sporadic). The following genes were analyzed: SOD1, C9orf72, ANG, FUS, and TDP-43. An extensive battery of classic neuropsychological tests was used in 27 ALS patients (22 SOD1 positive and 5 SOD1 negative) and 82 healthy controls (HCs). Overall 37 (15.4%) of 241 ALS patients carried mutations in tested genes-among 17 familiar ALS patients 16 (94.1%) were positive and among 224 apparently sporadic 21 (9.4%) had causative mutation. Mutations in SOD1 gene were the most common, representing 27 (73.0%) of all genetically positive ALS patients. The main clinical characteristics of SOD1 positive patients were: spinal onset in lower extremities, common sphincter and sensitive disturbances, and dysexecutive syndrome. Within SOD1 positive patients, we noticed somewhat earlier onset in patients with A145G, sensory and sphincter disturbances were dominant in patients with L144F, while D90A patients had significant sensory involvement. SOD1 negative group consisted of ten (27.0%) patients (six C9orf72, two ANG, one TDP-43, and one patient baring triple FUS, C9orf72 expansion, and ANG variants). Bulbar involvement and more extensive neuropsychological impairment (including executive, visuospatial, and memory difficulties) were the main features of SOD1 negative cohort. Our results suggest that meaningful clinical suspicion of certain ALS genotype might be made based on thorough clinical evaluation of patients.

Topics: Amyotrophic Lateral Sclerosis; C9orf72 Protein; Cognition Disorders; Cohort Studies; Disability Evaluation; DNA-Binding Proteins; Female; Genetic Association Studies; Genetic Testing; Humans; Male; Mutation; Neuropsychological Tests; Ribonuclease, Pancreatic; RNA-Binding Protein FUS; Serbia; Superoxide Dismutase-1; Tertiary Care Centers

2017

FUS mutations in amyotrophic lateral sclerosis: clinical, pathological, neurophysiological and genetic analysis.

Journal of neurology, neurosurgery, and psychiatry, 2010, Volume: 81, Issue:6

FUS gene mutations were recently identified in familial amyotrophic lateral sclerosis (ALS). The present studies sought to define the clinical, post-mortem and neurophysiological phenotypes in ALS families with FUS mutations and to determine the frequency of FUS mutations in familial and sporadic ALS.. FUS was screened for mutations in familial and sporadic ALS cases. Clinical, post-mortem and neurophysiological features of large families with FUS mutations are described.. FUS mutations were evident in 3.2% (4/124) of familial ALS, representing the second most common gene abnormality to be described in familial ALS after SOD1. No mutations were present in 247 sporadic ALS cases. The clinical presentation in 49 affected patients was consistent with a predominantly lower motor neuron disorder, supported by post-mortem findings. Upper motor neuron involvement varied, with Wallerian degeneration of corticospinal tracts present in one post-mortem case but absent in a second case from the same family. Features of cortical hyperexcitability demonstrated upper motor neuron involvement consistent with other forms of familial and sporadic ALS. One case presented with frontotemporal dementia (FTD) indicating that this may be a rare presenting feature in families with FUS mutation. Ubiquitin-positive cytoplasmic skein-like inclusions were present in lower motor neurons, but in contrast to sporadic ALS, no TDP-43 pathology was evident. Mutation-specific clinical features were identified. Patients with a R521C mutation were significantly more likely to develop disease at a younger age, and dropped-head syndrome was a frequent feature. Reduced disease penetrance was evident among most affected families.

Topics: Adult; Aged; Amyotrophic Lateral Sclerosis; Brain; Cognition Disorders; DNA Mutational Analysis; DNA-Binding Proteins; Dynactin Complex; Endosomal Sorting Complexes Required for Transport; Female; Genetic Testing; Humans; Male; Microtubule-Associated Proteins; Middle Aged; Nerve Tissue Proteins; Neuropsychological Tests; Point Mutation; Ribonuclease, Pancreatic; RNA-Binding Protein FUS; RNA, Messenger; Severity of Illness Index; Superoxide Dismutase; Superoxide Dismutase-1; Vesicular Transport Proteins; Young Adult

2010