Your search keyword '"Jeon, Beomseok"' showing total 20 results

1. Opicapone for the treatment of early wearing-off in levodopa-treated Parkinson's disease: pooled analysis of patient level data from two randomized open-label studies.

Author

Ferreira, Joaquim J., Lee, Jee-Young, Ma, Hyeo-il, Jeon, Beomseok, Poewe, Werner, Antonini, Angelo, Stocchi, Fabrizio, Rodrigues, Daniela M., Fonseca, Miguel M., Castilla-Fernández, Guillermo, Holenz, Joerg, Rocha, José-Francisco, and Rascol, Olivier

Subjects

PARKINSON'S disease, DOPA, MOVEMENT disorders, CATECHOL-O-methyltransferase

Abstract

Background: The wearing-off phenomenon is a key driver of medication change for patients with Parkinson's disease (PD) treated with levodopa. Common first-line options include increasing the levodopa dose or adding a catechol-O-methyltransferase (COMT) inhibitor, but there are no trials comparing the efficacy of these approaches. We evaluated the effectiveness of adjunct opicapone versus an additional 100 mg levodopa dose in PD patients with early wearing-off using pooled data from 2 randomized studies. Methods: The ADOPTION study program included two similarly designed 4-week, open-label studies conducted in South Korea (NCT04821687) and Europe (NCT04990284). Patients with PD, treated with 3–4 daily doses of levodopa therapy and with signs of early wearing-off were randomized (1:1) to adjunct opicapone 50 mg or an additional dose of levodopa 100 mg. Patient-level data from the two studies were pooled. Results: The adjusted mean [SE] change from baseline to week 4 in absolute OFF time (key endpoint) was − 62.8 min [8.8] in the opicapone group and − 33.8 min [9.0] in the levodopa 100 mg group, the difference significantly favoring opicapone (− 29.0 [− 53.8, − 4.2] min, p = 0.02). Significant differences in the Movement Disorder Society—Unified Parkinson's Disease Rating Scale Part III subscore (− 4.1 with opicapone vs − 2.5 with levodopa 100 mg), also favored opicapone (− 1.7 [− 3.3, − 0.04], p < 0.05). Dyskinesia was the most frequently reported adverse event (opicapone 7.2% vs. levodopa 100 mg 4.2%). Conclusions: In these short-term trials, introducing adjunct opicapone was more effective at reducing OFF time than adding another 100 mg levodopa dose in PD patients with early signs of wearing-off. [ABSTRACT FROM AUTHOR]

Published

2024

2. Parkinson's disease is associated with clonal hematopoiesis with TET2 mutation.

Author

Woo, Kyung Ah, Kim, Han-Joon, Lee, Chan Young, Shin, Jung Hwan, Sun, Choonghyun, Im, Hogune, An, Hongyul, Lim, Jiwoo, Choi, Su-Yeon, Koh, Youngil, and Jeon, Beomseok

Published

2024

3. Diagnostic accuracy and predictors of alpha-synuclein accumulation in the gastrointestinal tract of Parkinson's disease.

Author

Shin, Chaewon, Kim, Seong-Ik, Park, Sung-Hye, Kim, Jong-Min, Lee, Jee-Young, Chung, Sun Ju, Kim, Jae Woo, Ahn, Tae-Beom, Park, Kye Won, Shin, Jung Hwan, Lee, Chan Young, Lee, Hyuk-Joon, Kong, Seong-Ho, Suh, Yun-Suhk, Kim, Han-Joon, Yang, Han-Kwang, and Jeon, Beomseok

Published

2024

4. Clinical comparison of the 2008 and 2022 diagnostic criteria for early multiple system atrophy-cerebellar type.

Author

Kim, Seoyeon, Woo, Kyung Ah, Shin, Jung Hwan, Kim, Han-Joon, and Jeon, Beomseok

Subjects

CEREBELLAR ataxia, MAGNETIC resonance imaging, SYMPTOMS, INSTITUTIONAL review boards, MOVEMENT disorders, MULTIPLE system atrophy

Abstract

The article discusses the clinical comparison of the 2008 and 2022 diagnostic criteria for early multiple system atrophy-cerebellar type (MSA-C). The 2022 Movement Disorders Society criteria for MSA aimed to enhance specificity and balance sensitivity, introducing new terms and requirements for diagnosis. The study found discrepancies between the two criteria in diagnosing MSA in patients with early MSA-C, highlighting challenges in early detection and the need for additional biomarkers to improve sensitivity. The article concludes by suggesting that future revisions of diagnostic criteria should consider these challenges to enhance early detection of MSA-C. [Extracted from the article]

Published

2024

5. Clinical correlates of pareidolias and color discrimination deficits in idiopathic REM sleep behavior disorder and Parkinson's disease.

Author

Kim, Seoyeon, Choi, Ji-Hyun, Woo, Kyung Ah, Joo, Jae Young, Jeon, Beomseok, and Lee, Jee-Young

Subjects

COLOR vision, PARKINSON'S disease, RAPID eye movement sleep, SLEEP disorders, OPTICAL illusions, MOVEMENT disorders

Abstract

Visuoperceptual dysfunction is common in Parkinson's disease (PD) and is also reported in its prodromal phase, isolated REM sleep behavior disorder (iRBD). We aimed to investigate color discrimination ability and complex visual illusions known as pareidolias in patients with iRBD and PD compared to healthy controls, and their associating clinical factors. 46 iRBD, 43 PD, and 64 healthy controls performed the Farnsworth–Munsell 100 hue test and noise pareidolia tests. Any relationship between those two visual functions and associations with prodromal motor and non-motor manifestations were evaluated, including MDS-UPDRS part I to III, Cross-Cultural Smell Identification Test, sleep questionnaires, and comprehensive neuropsychological assessment. iRBD and PD patients both performed worse on the Farnsworth–Munsell 100 hue test and had greater number of pareidolias compared to healthy controls. No correlations were found between the extent of impaired color discrimination and pareidolia scores in either group. In iRBD patients, pareidolias were associated with frontal executive dysfunction, while impaired color discrimination was associated with visuospatial dysfunction, hyposmia, and higher MDS-UPDRS-III scores. Pareidolias in PD patients correlated with worse global cognition, whereas color discrimination deficits were associated with frontal executive dysfunction. Color discrimination deficits and pareidolias are frequent but does not correlate with each other from prodromal to clinically established stage of PD. The different pattern of clinical associates with the two visual symptoms suggests that evaluation of both color and pareidolias may aid in revealing the course of neurodegeneration in iRBD and PD patients. [ABSTRACT FROM AUTHOR]

Published

2024

6. Multimodal brain and retinal imaging of dopaminergic degeneration in Parkinson disease

Author

Universidad de Alicante. Departamento de Fisiología, Genética y Microbiología, Lee, Jee-Young, Martin-Bastida, Antonio, Murueta-Goyena Larrañaga, Ane, Gabilondo, Iñigo, Cuenca, Nicolás, Piccini, Paola, Jeon, Beomseok, Universidad de Alicante. Departamento de Fisiología, Genética y Microbiología, Lee, Jee-Young, Martin-Bastida, Antonio, Murueta-Goyena Larrañaga, Ane, Gabilondo, Iñigo, Cuenca, Nicolás, Piccini, Paola, and Jeon, Beomseok

Abstract

Parkinson disease (PD) is a progressive disorder characterized by dopaminergic neurodegeneration in the brain. The development of parkinsonism is preceded by a long prodromal phase, and >50% of dopaminergic neurons can be lost from the substantia nigra by the time of the initial diagnosis. Therefore, validation of in vivo imaging biomarkers for early diagnosis and monitoring of disease progression is essential for future therapeutic developments. PET and single-photon emission CT targeting the presynaptic terminals of dopaminergic neurons can be used for early diagnosis by detecting axonal degeneration in the striatum. However, these techniques poorly differentiate atypical parkinsonian syndromes from PD, and their availability is limited in clinical settings. Advanced MRI in which pathological changes in the substantia nigra are visualized with diffusion, iron-sensitive susceptibility and neuromelanin-sensitive sequences potentially represents a more accessible imaging tool. Although these techniques can visualize the classic degenerative changes in PD, they might be insufficient for phenotyping or prognostication of heterogeneous aspects of PD resulting from extranigral pathologies. The retina is an emerging imaging target owing to its pathological involvement early in PD, which correlates with brain pathology. Retinal optical coherence tomography (OCT) is a non-invasive technique to visualize structural changes in the retina. Progressive parafoveal thinning and fovea avascular zone remodelling, as revealed by OCT, provide potential biomarkers for early diagnosis and prognostication in PD. As we discuss in this Review, multimodal imaging of the substantia nigra and retina is a promising tool to aid diagnosis and management of PD.

Published

2022

7. Laboratory prognostic factors for the long-term survival of multiple system atrophy.

Author

Shin, Jung Hwan, Kim, Han-Joon, Lee, Chan Young, Chang, Hee Jin, Woo, Kyung Ah, and Jeon, Beomseok

Published

2022

8. Peripapillary retinal nerve fiber layer thinning in patients with progressive supranuclear palsy.

Author

Woo, Kyung Ah, Shin, Joo Young, Kim, Heejung, Ahn, Jeeyun, Jeon, Beomseok, and Lee, Jee-Young

Subjects

PROGRESSIVE supranuclear palsy, PEARSON correlation (Statistics), OPTICAL coherence tomography, SLEEP interruptions, GENERALIZED estimating equations, CEREBRAL atrophy, OPTIC disc, NERVE fibers

Abstract

Objectives: To investigate peripapillary retinal nerve fiber layer (pRNFL) changes in patients with progressive supranuclear palsy (PSP). Methods: We included 21 PSP patients (36 eyes) who underwent peripapillary optical coherence tomography (OCT) scans at 2.5 ± 1.3 years of disease, without ophthalmologic co-morbidities. We compared pRNFL thicknesses in PSP eyes with age-matched 22 controls (22 eyes) using generalized estimating equation model adjusting for intra-subject inter-eye correlations, age and sex. We also analyzed the correlation between the pRNFL thickness and clinical severity using Spearman's correlation. In twelve PSP patients with 3 T brain MRI volumetric scan within 1 year of OCT exam, we investigated the correlation between the pRNFL thickness and brain atrophy using Pearson's correlation. Results: PSP patients had global pRNFL thinning compared to controls (beta = − 6.436, p = 0.025). Global pRNFL thickness correlated with Hoehn & Yahr stages (r = − 0.487, p = 0.025), and nasal pRNFL thinning showed a trend of correlation (uncorrected p < 0.05). Exploratory correlation analysis between global pRNFL thickness and nonmotor items in the PSP rating scale showed a trend toward association with sleep disturbances (uncorrected p = 0.008) and urinary incontinence (uncorrected p = 0.031), although not significant after Bonferroni correction (all 28 items). The patients had significant atrophy in the posterior cingulate cortex, third ventricle, pallidum, and midbrain with reduced midbrain-to-pons ratio, but no correlation was found between pRNFL thickness and brain volumes. Conclusion: The pRNFL seems to be affected in PSP, which is more severe with advanced disease stages. Retinal investigation in a larger longitudinal cohort would help elucidate the pathophysiological role of retinal thinning in PSP. [ABSTRACT FROM AUTHOR]

Published

2022

9. Placebo response in degenerative cerebellar ataxias: a descriptive review of randomized, placebo-controlled trials.

Author

Choi, Ji-Hyun, Shin, Chaewon, Kim, Han-Joon, and Jeon, Beomseok

Subjects

PLACEBOS, RANDOMIZED controlled trials, CLINICAL trials, TRIAL practice

Abstract

Placebo response in degenerative cerebellar ataxias (CAs) has never been studied despite the large number of randomized controlled trials (RCTs) that have been conducted. In this descriptive review, we aimed to examine the placebo response in patients with CAs. We performed a literature search on PubMed for RCTs on CAs that were published from 1977 to January 2020 and collected data on the changes from the baseline to the endpoint on various objective ataxia-associated clinical rating scales. We reviewed 56 clinical trials, finally including 35 parallel-group studies and excluding 21 cross-over studies. The included studies were categorized as follows: (1) studies showing significant improvements in one or more ataxia scales in the placebo groups (n = 3); (2) studies reporting individual placebo responders with improvements in one or more ataxia scales in the placebo groups (n = 5)—the overall proportion of placebo responders was 31.9%; (3) studies showing mean changes in the direction of improvement in at least one ataxia scale in the placebo groups, though not statistically significant (n = 19); (4) studies showing no placebo response in any of the ataxia scales in the placebo groups (n = 4); (5) studies where data on the placebo groups were unavailable (n = 9). This review demonstrated the placebo response in patients with CAs on various objective ataxia scales. Our study emphasizes that the placebo response should be considered when designing, analyzing, and interpreting clinical trials and in clinical practice in CA patients. [ABSTRACT FROM AUTHOR]

Published

2022

10. SLC20A2 mutation manifesting as very late-onset orofacial dyskinesia.

Author

Woo, Kyung Ah, Yoo, Dallah, Lee, Jee-Young, Kim, Man Jin, Seong, Moon-Woo, Park, Sung Sup, and Jeon, Beomseok

Subjects

DYSKINESIAS, COMPUTED tomography, GENETIC variation, GENETIC mutation, MOVEMENT disorders, CARRIER proteins

Abstract

Brain computed tomography (CT) scans revealed prominent calcifications in bilateral basal ganglia and dentate nuclei in both patients 1 and 2 and in the occipital cortex in patient 2. There was also a focal calcification in the right frontal lobe in patient 2 We performed mutational analyses of the I HTT i gene and the four causative genes of PFBC: I SLC20A2 i , I PDGFB i , I PDGFRB i , and I XPR1 i . [Extracted from the article]

Published

2021

11. Arching deep brain stimulation in dystonia types.

Author

Kim, Han-Joon and Jeon, Beomseok

Subjects

*DEEP brain stimulation, *DYSTONIA, *BRAIN stimulation, *FOCAL dystonia

Abstract

Although medical treatment including botulinum toxic injection is the first-line treatment for dystonia, response is insufficient in many patients. In these patients, deep brain stimulation (DBS) can provide significant clinical improvement. Mounting evidence indicates that DBS is an effective and safe treatment for dystonia, especially for idiopathic and inherited isolated generalized/segmental dystonia, including DYT-TOR1A. Other inherited dystonia and acquired dystonia also respond to DBS to varying degrees. For Meige syndrome (craniofacial dystonia), other focal dystonia, and some rare inherited dystonia, further evidences are still needed to evaluate the role of DBS. Because short disease duration at DBS surgery and absence of fixed musculoskeletal deformity are associated with better outcome, DBS should be considered as early as possible when indicated after careful evaluation including genetic work-up. This review will focus on the factors to be considered in DBS for patients with dystonia and the outcome of DBS in the different types of dystonia. [ABSTRACT FROM AUTHOR]

Published

2021

12. Eye movements and association with regional brain atrophy in clinical subtypes of progressive supranuclear palsy.

Author

Choi, Ji-Hyun, Kim, Heejung, Shin, Jung Hwan, Lee, Jee-Young, Kim, Han-Joon, Kim, Jong-Min, and Jeon, Beomseok

Subjects

PROGRESSIVE supranuclear palsy, CEREBRAL atrophy, EYE movements, PARKINSON'S disease, MAGNETIC resonance imaging

Abstract

Objective: To investigate oculomotor impairment in subtypes of progressive supranuclear palsy (PSP) and its associations with clinical features and regional brain volumes in PSP. Methods: We compared the video-oculography (VOG) findings of 123 PSP patients, consisting of 66 PSP-Richardson syndrome (PSP-RS), 28 PSP-parkinsonism (PSP-P), and 29 PSP-progressive gait freezing (PSP-PGF), along with 80 Parkinson's disease (PD) patients. We also investigated the associations of the VOG results with clinical features (disease duration, PSP rating scales [PSPRS] scores for dysphagia and postural stability) in the subtypes of PSP patients and with regional volumes in the brainstem, including the midbrain, pons, medulla, and the superior cerebellar peduncle (SCP), among the patients who had MRI images at the time of VOG (30 PSP). Results: All of the three subtypes of PSP patients showed slower vertical saccades and smooth pursuit than that of the PD patients (adjusted p < 0.05). Among the PSP subtypes, saccadic peak velocity, saccadic accuracy, and pursuit gain were significantly decreased in patients with the PSP-RS compared to those with the PSP-PGF (adjusted p < 0.05). In multiple linear regression model, vertical saccadic velocity, latency, accuracy, and pursuit gain were associated with the PSPRS score for dysphagia (adjusted p < 0.05), and a decrease in vertical saccadic speed and accuracy was associated with SCP atrophy (corrected p < 0.05). Conclusions: This study demonstrated the severity of oculomotor dysfunction in differentiating the subtypes of PSP and its significant relationships with the dysphagia symptom and SCP volume in PSP. [ABSTRACT FROM AUTHOR]

Published

2021

13. Consensus guidelines for botulinum toxin therapy: general algorithms and dosing tables for dystonia and spasticity.

Author

Dressler, Dirk, Altavista, Maria Concetta, Altenmueller, Eckart, Bhidayasiri, Roongroj, Bohlega, Saeed, Chana, Pedro, Chung, Tae Mo, Colosimo, Carlo, Fheodoroff, Klemens, Garcia-Ruiz, Pedro J., Jeon, Beomseok, Jin, Lingjing, Kanovsky, Petr, Milanov, Ivan, Micheli, Federico, Orlova, Olga, Pandey, Sanjay, Pirtosek, Zvezdan, Relja, Maja, and Rosales, Raymond

Subjects

BOTULINUM toxin, BOTULINUM A toxins, SPASTICITY, DYSTONIA, INJECTIONS

Abstract

Botulinum toxin (BT) therapy is a complex and highly individualised therapy defined by treatment algorithms and injection schemes describing its target muscles and their dosing. Various consensus guidelines have tried to standardise and to improve BT therapy. We wanted to update and improve consensus guidelines by: (1) Acknowledging recent advances of treatment algorithms. (2) Basing dosing tables on statistical analyses of real-life treatment data of 1831 BT injections in 36 different target muscles in 420 dystonia patients and 1593 BT injections in 31 different target muscles in 240 spasticity patients. (3) Providing more detailed dosing data including typical doses, dose variabilities, and dosing limits. (4) Including total doses and target muscle selections for typical clinical entities thus adapting dosing to different aetiologies and pathophysiologies. (5) In addition, providing a brief and concise review of the clinical entity treated together with general principles of its BT therapy. For this, we collaborated with IAB—Interdisciplinary Working Group for Movement Disorders which invited an international panel of experts for the support. [ABSTRACT FROM AUTHOR]

Published

2021

14. Urinary Symptoms and Urodynamic Findings in Patients with Spinocerebellar Ataxia.

Author

Jang, Mihee, Kim, Han-Joon, Kim, Aryun, and Jeon, Beomseok

Subjects

SYMPTOMS, CEREBELLAR ataxia, MEDICAL records, SPINOCEREBELLAR ataxia, NEUROGENIC bladder, DISEASE duration, FAMILY history (Medicine)

Abstract

Urinary dysfunctions are not considered symptoms of spinocerebellar ataxias (SCAs). However, given that a patient with SCAs without a family history might be misdiagnosed as MSA-C when having urinary dysfunctions, characterization of urinary dysfunctions in SCAs is needed not only to understand SCAs but also to correctly diagnosis patients with ataxia. We retrospectively reviewed medical records of 143 patients with genetically confirmed SCA1, 2, 3, 6, 7, 17, and DRPLA. Twenty-two patients (men n = 9; age 62.1 ± 10.9; disease duration 8.2 ± 2.9 years) who had lower urinary track symptoms (LUTS) were included in this study. Six patients underwent urodynamic study (UDS), and 2 underwent uroflowmetry. LUTS was present in 1 of 11 patients with SCA1, in 4 of 51 with SCA2, in 2 of 26 with SCA3, in 3 of 20 with SCA6, in 2 of 4 with SCA7, in 8 of 26 with SCA17, and in 2 of 5 with DRPLA. Overall, urinary frequency was the most common symptom (16 patients, 72.7%) followed by voiding difficulty. In three of the 6 patients with UDS, post-micturition residuals were > 100 ml. Detrusor overactivity was noted in three patients. Detrusor areflexia was observed in one. Four patients were diagnosed with a neurogenic bladder, 3 with a storage problem, and 1 with both storage and voiding problems. Fifteen percent of the patients with SCAs had LUTS, and LUTS occurred in various types of SCAs. Our results indicate that SCAs should be considered in patients with progressive cerebellar ataxia and urinary dysfunctions. [ABSTRACT FROM AUTHOR]

Published

2020

15. GCH-1 genetic variant may cause Parkinsonism by unmasking the subclinical nigral pathology.

Author

Shin, Jung Hwan, Lee, Woong-Woo, Lee, Jee-Young, Kim, Han-Joon, and Jeon, Beomseok

Subjects

PARKINSONIAN disorders, PATHOLOGY, DISEASE progression, PARKINSON'S disease, NEURODEGENERATION

Abstract

Background: Recent studies suggest that GTP cyclohydrolase 1 (GCH-1) variant may be a risk factor for nigral degeneration causing PD. Methods: A 49-year-old Korean woman visited our movement disorder clinic with the initial presentation of Parkinsonism starting at age 47. We monitored the degree of nigral degeneration with serial FP-CIT PET throughout the course of her disease (2, 8 and 11 years from disease onset). Results: The initial clinical presentation was consistent with intrinsic dopamine deficiency caused by GCH-1 variant. However, her follow-up disease course was consistent with Parkinsonism caused by nigral neurodegeneration. We found a novel GCH-1 variant in the current case. The disease course of the patient was overall benign in motor and non-motor aspects, corresponding to previously reported GCH-1 cases with PD. Serial FP-CIT PET scans showed normal initial FP-CIT binding followed by a continuous decline of the putaminal binding ratio. However, the decreased binding ratio could not sufficiently explain the corresponding clinical duration of the patient. Therefore, dopamine deficiency by GCH-1 genetic variant contributed to Parkinsonism in the current case with subclinical nigral degeneration. Conclusion: Our case suggests that GCH-1 variant causes Parkinsonism by unmasking the subclinical nigral pathology, not by causing the nigral neurodegeneration. [ABSTRACT FROM AUTHOR]

Published

2020

16. Contrast sensitivity impairment in drug-naïve Parkinson's disease patients associates with early cognitive decline.

Author

Hong, Sang Bin, Ahn, Jeeyun, Yoo, Dalla, Shin, Joo Young, Jeon, Beomseok, and Lee, Jee-Young

Subjects

CONTRAST sensitivity (Vision), PARKINSON'S disease, COGNITION disorders, ODDS ratio

Abstract

Objectives: To investigate the contrast sensitivity function in drug-naïve Parkinson's disease (PD) patients and its predictive value with longitudinal follow-up data. Methods: We included newly diagnosed non-demented PD patients who performed contrast sensitivity test between 2013 and 2014. Contrast sensitivity function at drug-naïve state in PD patients was compared with age-matched normal control data of our center. Correlation between contrast sensitivity function and parkinsonian motor and non-motor features including the Mini-Mental State Exam (MMSE) score at the time of diagnosis were analyzed by linear regression. With longitudinal follow-up data after initiating anti-parkinsonian therapy, the risk conferred on subsequent visual hallucinations and cognitive impairment requiring anti-dementia drugs was analyzed by dichotomizing PD group based on the initial contrast sensitivity function. Results: Forty-eight patients were finally included, and mean follow-up periods were 43 months. Contrast sensitivity function in drug-naïve PD patients was significantly worse than controls. Contrast sensitivity function correlated with sleep disturbance (p = 0.001) and global cognitive status reflected by the MMSE score (p = 0.020). It also associated with further decline in the MMSE during the follow-ups (p = 0.029). Patients with below average contrast sensitivity function at the time of diagnosis showed higher risk of cognitive decline requiring anti-dementia drugs (adjusted odds ratio = 4.68, p = 0.04) and of visual hallucinations (adjusted odds ratio = 12.54, p = 0.04) than those above average function during the follow-up. Conclusion: Contrast sensitivity impairment in drug-naïve PD patients associates with clinical demand for therapeutic intervention of cognitive decline as well as development of visual hallucinations in the early course of the disease. [ABSTRACT FROM AUTHOR]

Published

2020

17. Progression of Oropharyngeal Dysphagia in Patients with Multiple System Atrophy.

Author

Do, Hui Jae, Seo, Han Gil, Lee, Hyun Haeng, Oh, Byung-Mo, Kim, Yoon, Kim, Aryun, Kim, Han-Joon, Jeon, Beomseok, and Han, Tai Ryoon

Abstract

We investigated the progression of oropharyngeal dysphagia in patients with multiple system atrophy (MSA), with particular emphasis on MSA subtype variation. Fifty-nine MSA patients (31 MSA-P, 21 MSA-C, and 7 MSA-PC) who had undergone at least one videofluoroscopic swallowing study (VFSS) to evaluate dysphagia symptoms were included. Clinical data and VFSS findings were retrospectively evaluated using the videofluoroscopic dysphagia scale (VDS), and the results of each MSA subtype group were compared. The median latency to onset of diet modification from onset of MSA symptoms was 5.995 (95% CI 4.890-7.099) years in all MSA patients, 5.036 (95% CI 3.605-6.467) years in MSA-P, and 6.800 (95% CI 6.078-7.522) years in MSA-C (P = 0.035). The latency to onset of diet modification from onset of dysphagia symptoms was 2.715 (95% CI 2.132-3.298) years in all MSA patients, 2.299 (95% CI 1.194-3.403) years in MSA-P, and 5.074 (95% CI 2.565-7.583) years in MSA-C (P = 0.039). The latencies to onset of tube feeding from onset of MSA symptoms and dysphagia symptoms were 7.003 (95% CI 6.738-7.268) years and 3.515 (95% CI 2.123-4.907) years, respectively, in all MSA patients, without significant difference between subtypes. In the patients who underwent VFSS follow-up for ≥ 1 year, 6 oral VDS items significantly worsened; only two pharyngeal items exhibited significant changes. Patients with MSA-P commenced diet modification earlier than patients with MSA-C, despite no significant difference in the latency to onset of tube feeding. Deterioration of dysphagia may be more pronounced in the oral function of MSA patients. [ABSTRACT FROM AUTHOR]

Published

2020

18. Macular ganglion-cell-complex layer thinning and optic nerve integrity in drug-naïve Parkinson's disease.

Author

Lee, Jee-Young, Ahn, Jeeyun, Yoon, Eun Jin, Oh, Sohee, Kim, Yu Kyeong, and Jeon, Beomseok

Subjects

OPTIC nerve, PARKINSON'S disease, MACULA lutea, DIFFUSION tensor imaging, CHOROID, OPTICAL coherence tomography, INTEGRITY

Abstract

To reveal the macular inner retinal change linked to axonal degeneration in Parkinson's disease (PD), we performed macular optical coherence tomography scan and diffusion tensor imaging of the retrobulbar optic nerve on both eyes of 36 drug-naïve PD patients. Thicknesses of inner retinal layers were automatically measured, and correlation analysis was conducted between the retinal thickness and diffusion parameters of the optic nerve. PD patients showed thinning of the inner retinal layers compared to control data. Thicknesses of the ganglion cell and inner plexiform layers were both correlated positively with fractional anisotropy and negatively with diffusivity indices of ipsilateral optic nerve (FDR-adjusted p < 0.05). This study revealed a novel in vivo connection between macular parafoveal ganglion cell change and integrity in the retrobulbar optic nerve in drug-naïve PD. [ABSTRACT FROM AUTHOR]

Published

2019

19. Increased Diagnostic Yield of Spastic Paraplegia with or Without Cerebellar Ataxia Through Whole-Genome Sequencing.

Author

Kim, Aryun, Kumar, Kishore R., Davis, Ryan L., Mallawaarachchi, Amali C., Gayevskiy, Velimir, Minoche, Andre E., Walls, Zachary, Kim, Han-Joon, Jang, Mihee, Cowley, Mark J., Choi, Ji-Hyun, Shin, Chaewon, Sue, Carolyn M., and Jeon, Beomseok

Subjects

CEREBELLAR ataxia, FAMILIAL spastic paraplegia, FRIEDREICH'S ataxia, DNA copy number variations, PARAPLEGIA, ATAXIA

Abstract

Inherited disorders of spasticity or ataxia exist on a spectrum with overlapping causative genes and phenotypes. We investigated the use of whole-genome sequencing (WGS) to detect a genetic cause when considering this spectrum of disorders as a single group. We recruited 18 Korean individuals with spastic paraplegia with or without cerebellar ataxia in whom common causes of hereditary cerebellar ataxia and hereditary spastic paraplegia had been excluded. We performed WGS with analysis for single nucleotide variants, small insertions and deletions, copy number variants (CNVs), structural variants (SVs) and intronic variants. Disease-relevant variants were identified in ABCD1 (n = 3), CAPN1 (n = 2), NIPA1 (n = 1) and PLA2G6 (n = 1) for 7/18 patients (38.9%). A 'reverse phenotyping' approach was used to clarify the diagnosis in individuals with PLA2G6 and ABCD1 variants. One of the ABCD1 disease-relevant variants was detected on analysis for intronic variants. No CNV or SV causes were found. The two males with ABCD1 variants were initiated on monitoring for adrenal dysfunction. This is one of only a few studies to analyse spastic-ataxias as a continuous spectrum using a single approach. The outcome was improved diagnosis of unresolved cases for which common genetic causes had been excluded. This includes the detection of ABCD1 variants which had management implications. Therefore, WGS may be particularly relevant to diagnosing spastic ataxias given the large number of genes associated with this condition and the relatively high diagnostic yield. [ABSTRACT FROM AUTHOR]

Published

2019

20. Multimodal brain and retinal imaging of dopaminergic degeneration in Parkinson disease.

Author

Lee, Jee-Young, Martin-Bastida, Antonio, Murueta-Goyena, Ane, Gabilondo, Iñigo, Cuenca, Nicolás, Piccini, Paola, and Jeon, Beomseok

Abstract

Parkinson disease (PD) is a progressive disorder characterized by dopaminergic neurodegeneration in the brain. The development of parkinsonism is preceded by a long prodromal phase, and >50% of dopaminergic neurons can be lost from the substantia nigra by the time of the initial diagnosis. Therefore, validation of in vivo imaging biomarkers for early diagnosis and monitoring of disease progression is essential for future therapeutic developments. PET and single-photon emission CT targeting the presynaptic terminals of dopaminergic neurons can be used for early diagnosis by detecting axonal degeneration in the striatum. However, these techniques poorly differentiate atypical parkinsonian syndromes from PD, and their availability is limited in clinical settings. Advanced MRI in which pathological changes in the substantia nigra are visualized with diffusion, iron-sensitive susceptibility and neuromelanin-sensitive sequences potentially represents a more accessible imaging tool. Although these techniques can visualize the classic degenerative changes in PD, they might be insufficient for phenotyping or prognostication of heterogeneous aspects of PD resulting from extranigral pathologies. The retina is an emerging imaging target owing to its pathological involvement early in PD, which correlates with brain pathology. Retinal optical coherence tomography (OCT) is a non-invasive technique to visualize structural changes in the retina. Progressive parafoveal thinning and fovea avascular zone remodelling, as revealed by OCT, provide potential biomarkers for early diagnosis and prognostication in PD. As we discuss in this Review, multimodal imaging of the substantia nigra and retina is a promising tool to aid diagnosis and management of PD. [ABSTRACT FROM AUTHOR]

Published

2022