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2. Sensory disturbances in Creutzfeldt-Jakob disease.

Author

Appel, Shmuel, Cohen, Yael, Appel, Shira, Cohen, Oren S., Chapman, Joab, Rosenmann, Hanna, Nitsan, Zeev, and Kahana, Esther

Subjects
CREUTZFELDT-Jakob disease, PERIPHERAL nervous system, TAU proteins, SYMPTOMS, CENTRAL nervous system
Abstract

Background: Creutzfeldt-Jakob disease (CJD) is a fatal neurodegenerative disease characterized by rapidly progressive dementia, motor impairments, and psychiatric symptoms. Sensory disturbances were occasionally reported as well. The study aims to describe the sensory symptoms of the disease. Methods: The CJD Israeli National Database was screened for patients who presented sensory symptoms throughout the disease course. Symptoms, characteristics, and distribution were reviewed and the demographic and clinical data (sex, etiologies of the disease, age of onset, disease duration, neurological exam finding, tau protein level, EEG and MRI findings) were compared with the demographics and clinical data of CJD without sensory symptoms. Then, the patients with sensory symptoms were divided into patients with symptom distribution consistent with peripheral nervous system (PNS) involvement and central nervous system (CNS) involvement. The demographics and clinical data of the 2 groups were compared. Results: Eighty-four CJD patients with sensory symptoms and 645 CJD patients without sensory symptoms were included in the study. Sensory symptoms were more common in genetic E200K CJD patients (14.6% vs. 5.6% respectively, p = 0.0005) (chi-squared test). Numbness and neuropathic pain were the most common symptoms and distribution of symptoms of "stocking gloves" with decreased deep tendon reflexes suggesting peripheral neuropathy in 44% of the patients. In these patients, the classical EEG findings of Periodic Sharp Wave Complexes were less often found (58% vs. 22%, p = 0.02) (chi-squared test). Conclusions: Sensory symptoms are more common in E200K patients and often follow peripheral neuropathy distribution that suggests PNS involvement. [ABSTRACT FROM AUTHOR]

Published
2024
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5. The epidemiological and clinical characteristics of patients with young-onset genetic Creutzfeldt-Jakob disease.

Author

Safadi, Daniel, Cohen, Oren S, Chapman, Joab, Rosenmann, Hanna, Nitsan, Zeev, Kahan, Esther, Appel, Shmuel, and Alkrenawi, Marwan

Subjects
CREUTZFELDT-Jakob disease, YOUNG adults, GENETIC disorders, OLDER patients, DYSARTHRIA, PRION diseases
Abstract

The onset of Creutzfeldt-Jakob disease (CJD) is usually around the age of 60, but younger patients have been described as well. Our study characterizes the demographic and clinical features of young-onset CJD patients. The CJD Israeli National Database was reviewed, and the patients were divided into groups of young (<40-year-old) (Y|) and older disease onset (>40-year-old) (O). Each group was further divided into sporadic (sCJD) and genetic (gCJD) patients. Clinical and demographic parameters were compared between the groups The study included 731 patients (Y- 18 patients, O- 713 patients). MRI showed classical features more often in the older population (O-76.9%, Y-36%, p = 0.006). Rapidly progressive dementia as a presenting feature was more common in the older group (O = 58%, Y = 27.7%, p = 0.019) whereas cerebellar onset (gait instability, dysarthria) was more common in the younger group (O = 6.7%, Y = 27.7%, p = 0.036)). Among gCJD patients, rapidly progressive dementia was commonly seen in older patients (O = 54%, Y = 21% p = 0.008) whereas cerebellar symptoms were seen in young patients (O = 7%, Y = 30% p = 0.01) Typical MRI findings were seen in 37% of young people compared to 87% of older patients (p = 0.002). No significant differences were between young and older patients in the sCJD group. Young-onset gCJD patients have unique disease features including less typical brain MRI changes, a lower prevalence of dementia, and a higher prevalence of cerebellar signs at disease onset. [ABSTRACT FROM AUTHOR]

Published
2023
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9. Genetic Creutzfeldt‐Jakob disease in Turkish Jews—demographic and clinical features.

Author

Menendez, Leslie, Milo, Ron, Cohen, Oren S., Chapman, Joab, Rosenmann, Hanna, Nitsan, Zeev, Kahana, Esther, and Appel, Shmuel

Subjects
CREUTZFELDT-Jakob disease, TURKS, GENETIC disorders, TAU proteins, JEWS
Abstract

Background: The largest cluster of genetic Creutzfeldt‐ Jakob Disease (CJD) exists in Libyan Jews carrying the E200K mutation in the PRNP gene. However, there is another cluster of genetic CJD with E200K mutation in families of Turkish–Jewish origin. Aims: In this retrospective study, we aim to describe the demographic and clinical features of this population of patients. Material and Methods: The Israeli National CJD database was searched for demographic, clinical, imaging, and laboratory data of genetic CJD patients of Libyan and Turkish ancestry with the E200K mutation. The data of Libyan and Turkish patients were compared with notice similar or different demographic or clinical courses. Results: Four hundred and twenty‐three patients with CJD of Libyan (L) ancestry and 27 patients with CJD of Turkish (T) ancestry were identified. There were no significant differences in demographic and clinical data between the two populations (age of onset: T = 62 ± 8.8, L = 60 ± 9.7; age of death: T = 63 ± 8.6, L = 61 ± 9.7; and disease duration: T = 7.8 ± 8.4 months, L = 9.6 ± 13.6 months). Rapidly progressive dementia was the most common presentation in both groups, followed by pure cerebellar onset. The levels of tau protein in CSF did not differ between groups (T = 1290 ± 397.6 pg/ml, L = 1276 ± 594.2 pg/ml). MRI and EEG showed classical CJD features in most patients in both groups. Discussion: The E200K mutation is the most common mutation among gCJD patients and was reported in different ethnical populations, suggesting several independent haplotypes of the mutation. The Turkish‐Jew cluster, first described in this study, shares similar demographic and clinical features with the bigger cluster of Libyan‐Jews CJD patients. Conclusion: E200K gCJD patients of Turkish ancestry share similar demographic and clinical features to patients of Libyan descent, suggesting a common origin of both populations. [ABSTRACT FROM AUTHOR]

Published
2022
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14. The association of quantitative EEG and MRI in Creutzfeldt‐Jakob Disease.

Author

Appel, Shmuel, Cohen, Oren S., Chapman, Joab, Gilat, Shlomo, Rosenmann, Hanna, Nitsan, Zeev, Kahan, Ester, and Blatt, Ilan

Subjects
CREUTZFELDT-Jakob disease, ELECTROENCEPHALOGRAPHY
Abstract

Introduction: Previous studies showed concordance between the typical Periodic Sharp Wave Complex (PSWC) activity in EEG of Creutzfeldt‐Jakob Disease (CJD) patients and the MRI findings, while the concordance with slow activity in EEG is less established. The aim of this study was to better characterize the association between MRI findings and EEG changes using quantitative EEG (qEEG) analysis. Methods: The demographics, clinical features, and the MRI findings of 12 familial E200K patients with CJD were gathered. EEG test was done and reviewed for the typical PSWC and for the non‐specific slow activity. A possible association between the MRI findings and the EEG activity was examined. Then, EEG was analyzed using qEEG tool, and the association between the qEEG finding and the MRI was examined. Results: Twelve patients were included in the study (67% women). Cortical MRI lesions finding were seen in 6/12 (50%) of the patients, and deep gray mater lesions were seen in 8/12 patients (67%). EEG showed the classic PSWC in 6/12 (50%) of the patients where slow activity was seen in 10/12 (83%). Slow activity and cortical MRI findings were associated in only 2/6 (33%) where deep gray matter findings and the slow activity had concordance of 4/8 (50%). qEEG analysis improved this concordance between slow activity and cortical findings to 3/6 (50%) and with the deep gray matter findings to 5/8 (63%). Conclusions: Quantitative EEG analysis modesty but not significantly, improves the association of EEG slow activity in familial E200K CJD patients with MRI findings. [ABSTRACT FROM AUTHOR]

Published
2019
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15. Early pathology in sleep studies of patients with familial Creutzfeldt-Jakob disease.

Author

Givaty, Gili, Maggio, Nicola, Cohen, Oren S., Blatt, Ilan, and Chapman, Joab

Subjects
SLEEP disorders, CREUTZFELDT-Jakob disease, MAGNETIC resonance imaging, CEREBROSPINAL fluid, SLEEP-wake cycle, PATIENTS
Abstract

In this study, we aimed to assess sleep function in patients with recent-onset familial Creutzfeldt-Jakob disease ( fCJD). The largest cluster of fCJD patients is found in Jews of Libyan origin, linked to the prion protein gene ( PRNP) E200K mutation. The high index of suspicion in these patients often leads to early diagnosis, with complaints of insomnia being a very common presenting symptom of the disease. The study included 10 fCJD patients diagnosed by clinical manifestations, magnetic resonance imaging ( MRI) scan of the brain, elevated tau protein in the cerebrospinal fluid ( CSF) and positive PRNP E200K mutation. Standard polysomnography was performed after a brief interview confirming the presence of sleep disturbances. All patients showed a pathological sleep pattern according to all scoring evaluation settings. The sleep stages were characterized by (i) disappearance of sleep spindles; (ii) outbursts of periodic sharp waves and shallowing of sleep consisting in increased Stage 2 and wake periods during the night, as well as decrease of slow-wave sleep and rapid eye movement ( REM) sleep. Recordings of respiratory functions reported irregular breathing with central and obstructive apnea and hypopnea. The typical hypotonia occurring during the night and atonia during REM sleep were replaced by hyperactive sleep consisting of multiple jerks, movements and parasomnia (mainly talking) throughout the night. In conclusion, we report unique pathological sleep patterns in early fCJD associated with the E200K mutation. Specific respiratory disturbances and lack of atonia could possibly serve as new, early diagnostic tools in the disease. [ABSTRACT FROM AUTHOR]

Published
2016
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16. CSF tau correlates with the degree of cortical involvement in E200K familial Creutzfeldt-Jakob disease.

Author

Cohen, Oren S., Chapman, Joab, Korczyn, Amos D., Siaw, Oliver L., Warman-Alaluf, Naama, Nitsan, Zeev, Appel, Shmuel, Kahana, Esther, Rosenmann, Hanna, and Hoffmann, Chen

Subjects
*CREUTZFELDT-Jakob disease, *CREUTZFELDT-Jakob disease diagnosis, *BIOMARKERS, *CEREBROSPINAL fluid, *TAU proteins, *PATIENTS
Abstract

Cerebrospinal fluid (CSF) tau was found to correlate with disease severity and cognitive status in E200K familial Creutzfeldt-Jakob disease (fCJD) patients. The objective of the present study was to test whether tau levels in the CSF also correlate with the disease burden as reflected by the degree of cortical involvement in DWI MRI. Forty-four consecutive E200K fCJD patients (25 males, mean age 58.6 ± 7.5, range 48–75 years) were recruited to the study and had a CSF tau examination as well as measurements of the extent of the cortical involvement in the DWI axial MRI. Correlation was tested using Pearson test. A significant correlation ( r = 0.617 p < 0.0001) was found between CSF tau levels and the extent of cortical involvement. This correlation between tau levels and the disease burden reinforce the notion that tau can be used as a biomarker reflecting the extent of disease in patients with E200K fCJD. [ABSTRACT FROM AUTHOR]

Published
2016
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17. Pros and cons of a prion-like pathogenesis in Parkinson's disease.

Author

Hilker, Ruediger, Brotchie, Jonathan M., and Chapman, Joab

Subjects
PARKINSON'S disease, NEURODEGENERATION, CREUTZFELDT-Jakob disease, COMMUNICABLE diseases, PATHOLOGICAL physiology
Abstract

Background: Parkinson's disease (PD) is a slowly progressive neurodegenerative disorder which affects widespread areas of the brainstem, basal ganglia and cerebral cortex. A number of proteins are known to accumulate in parkinsonian brains including ubiquitin and a-synuclein. Prion diseases are sporadic, genetic or infectious disorders with various clinical and histopathological features caused by prion proteins as infectious proteinaceous particles transmitting a misfolded protein configuration through brain tissue. The most important form is Creutzfeldt-Jakob disease which is associated with a self-propagating pathological precursor form of the prion protein that is physiologically widely distributed in the central nervous system. Discussion: It has recently been found that α-synuclein may behave similarly to the prion precursor and propagate between cells. The post-mortem proof of α-synuclein containing Lewy bodies in embryonic dopamine cells transplants in PD patient suggests that the misfolded protein might be transmitted from the diseased host to donor neurons reminiscent of prion behavior. The involvement of the basal ganglia and brainstem in the degenerative process are other congruencies between Parkinson's and Creutzfeldt-Jakob disease. However, a number of issues advise caution before categorizing Parkinson's disease as a prion disorder, because clinical appearance, brain imaging, cerebrospinal fluid and neuropathological findings exhibit fundamental differences between both disease entities. Most of all, infectiousness, a crucial hallmark of prion diseases, has never been observed in PD so far. Moreover, the cellular propagation of the prion protein has not been clearly defined and it is, therefore, difficult to assess the molecular similarities between the two disease entities. Summary: At the current state of knowledge, the molecular pathways of transmissible pathogenic proteins are not yet fully understood. Their exact involvement in the pathophysiology of prion disorders and neurodegenerative diseases has to be further investigated in order to elucidate a possible overlap between both disease categories that are currently regarded as distinct entities. [ABSTRACT FROM AUTHOR]

Published
2011
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18. Thalamo-striatal diffusion reductions precede disease onset in prion mutation carriers.

Author

Lee, Hedok, Rosenmann, Hanna, Chapman, Joab, Kingsley, Peter B., Hoffmann, Chen, Cohen, Oren S., Kahana, Esther, Korczyn, Amos D., and Prohovnik, Isak

Subjects
PRION diseases, PRIONS, NUCLEIC acids, GENETIC mutation, PATHOGENIC microorganisms, PATHOLOGICAL physiology
Abstract

Human prion diseases present substantial scientific and public health challenges. They are unique in being sporadic, infectious and inherited, and their pathogen is distinct from all other pathogens in lacking nucleic acids. Despite progress in understanding the molecular structure of prions, their initial cerebral pathophysiology and the loci of cerebral injury are poorly understood. As part of a large prospective study, we analysed early diffusion MRI scans of 14 patients with the E200K genetic form of Creutzfeldt–Jakob Disease, 20 healthy carriers of this mutation that causes the disease and 20 controls without the mutation from the same families. Cerebral diffusion was quantified by the Apparent Diffusion Coefficient, and analysed by voxel-wise statistical parametric mapping technique. Compared to the mutation-negative controls, diffusion was significantly reduced in a thalamic-striatal network, comprising the putamen and mediodorsal, ventrolateral and pulvinar thalamic nuclei, in both the patients and the healthy mutation carriers. With disease onset, these diffusion reductions intensified, but did not spread to other areas. The caudate nucleus was reduced only after symptomatic onset. These findings indicate that cerebral diffusion reductions can be detected early in the course of Creutzfeldt–Jakob Disease, and years before symptomatic onset in mutation carriers, in a distinct subcortical network. We suggest that this network is centrally involved in the pathogenesis of Creutzfeldt–Jakob Disease, and its anatomical connections are sufficient to account for the common symptoms of this disease. Further, we suggest that the abnormalities in healthy mutation-carrying subjects may reflect the accumulation of abnormal prion protein and/or associated vacuolation at this time, temporally close to disease onset. [ABSTRACT FROM PUBLISHER]

Published
2009
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19. Spatial distribution of abnormal EEG activity in Creutzfeldt-Jakob disease.

Author

Appel, Shmuel, Cohen, Oren S., Chapman, Joab, Gilat, Shlomo, Rosenmann, Hanna, Nitsan, Zeev, Kahana, Esther, and Blatt, Ilan

Subjects
*CREUTZFELDT-Jakob disease, *ELECTROENCEPHALOGRAPHY, *DISEASE duration, *PARTIAL epilepsy, *DISEASE progression
Abstract

Electroencephalogram (EEG) pattern in Creutzfeldt-Jakob disease (CJD) is characterized by diffuse abnormal activity, although lateralization to one hemisphere has been described in the first stages of the disease. This study aimed to determine whether abnormal EEG activity predominantly occurs in anterior versus posterior brain regions. As part of a prospective study, the demographics, clinical features and MRI findings of genetic E200K CJD patients were collected. EEG was performed and the recordings reviewed for the typical periodic sharp wave complex (PSWC) and non-specific slow activity. Data were analyzed using the qEEG tool, and the activity in anterior and posterior regions of the brain compared. Eleven genetic E200K CJD patients were included in the study (67% women). The average age was 59.1 ± 8.4 SD years and the average disease duration was 2.4 ± 2.1 months. EEG showed the classic PSWC pattern in 5/11 (45%) of the patients, and slow activity was seen in 9/11 (82%). EEG was normal in 2 patients. PSWC activity was diffuse in 2/5 patients and unilateral in 3/5 patients; slow activity was diffuse in 9 patients. Quantitative analysis of PSWC and slow activity showed no significant difference between anterior and posterior distribution. The abnormal EEG activity in CJD is diffuse with no clear spatial predominance in anterior or posterior brain regions. [ABSTRACT FROM AUTHOR]

Published
2021
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20. The imaging appearance of Creutzfeldt–Jakob disease caused by the E200K mutation

Author

Fulbright, Robert K., Kingsley, Peter B., Guo, Xiaodong, Hoffmann, Chen, Kahana, Esther, Chapman, Joab C., and Prohovnik, Isak

Subjects
*CREUTZFELDT-Jakob disease, *NEURODEGENERATION, *DIFFUSION magnetic resonance imaging, *MAGNETIC resonance imaging
Abstract

Abstract: The E200K mutation on chromosome 20 can cause familial Creutzfeldt–Jakob disease (CJD). Patients with this mutation are clinically similar to those with sporadic CJD, but their imaging features are not well documented. We report here the quantitative and qualitative evaluation of the magnetic resonance (MR) imaging characteristics of this unique group of patients using three-dimensional spoiled gradient recalled (SPGR) echo images, diffusion-weighted imaging (DWI) with apparent diffusion coefficient (ADC) measurements, MR spectroscopy and a fluid-attenuated inversion recovery (FLAIR) sequence. The SPGR and ADC data were analyzed with SPM99. ANCOVA and regression models were used for a region-of-interest (ROI) analysis of ADC and metabolic ratios. CJD patients had a decreased fraction of gray matter and an increased fraction of cerebrospinal fluid (P=.001) in the cortex and cerebellum and increased ADC values in the cortex (P<.001). Focal decreases of ADC were found in the putamen via ROI analysis (548±83 vs. 709±9 μm2/s, P=.02). N-acetyl aspartate (NAA) was generally reduced, with the NAA/Cho ratio lowest in the cingulate gyrus. Qualitative assessment revealed hyperintensities on FLAIR, DWI or both in the putamen (three out of four patients), caudate (three out of four patients) and thalamus. These results provide a framework for future study of patients with genetically defined familial CJD. [Copyright &y& Elsevier]

Published
2006
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21. Ancestral Origins and Worldwide Distribution of the PRNP 200K Mutation Causing Familial Creutzfeldt-Jakob Disease.

Author

Hee Suk Lee, Sambuughin, Nyamkhishig, Cervenakova, Larisa, Chapman, Joab, Pocchiari, Maurizio, Litvak, Svetlana, Hai Yan Qi, Budka, Herbert, del Ser, Teodoro, Furukawa, Hisako, Brown, Paul, Gajdusek, D. Carleton, Long, Jeffrey C., Korczyn, Amos D., and Goldfarb, Lev G.

Subjects
*GENETIC mutation, *CREUTZFELDT-Jakob disease, *GENES, *CHROMOSOMES
Abstract

Studies the ancestral origins and worldwide distribution of the PRNP 200K mutation causing familial Creutzfeldt-Jakob disease (CDJ). Selection of microsatellite markers on the PRNP gene on chromosome 20p12-pter and an intragenic single-nucleotide polymorphism at the PRNP codon 129; Role of founder effect and independent mutational events for the geographic distribution of heridatary CJD associated with the 200K mutation.

Published
1999
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