Your search keyword '"Stamelou, Maria"' showing total 170 results

1. Correction: Whole-genome sequencing analysis reveals new susceptibility loci and structural variants associated with progressive supranuclear palsy

Author

Wang, Hui, Chang, Timothy S., Dombroski, Beth A., Cheng, Po-Liang, Patil, Vishakha, Valiente-Banuet, Leopoldo, Farrell, Kurt, Mclean, Catriona, Molina-Porcel, Laura, Rajput, Alex, De Deyn, Peter Paul, Le Bastard, Nathalie, Gearing, Marla, Kaat, Laura Donker, Van Swieten, John C., Dopper, Elise, Ghetti, Bernardino F., Newell, Kathy L., Troakes, Claire, de Yébenes, Justo G., Rábano-Gutierrez, Alberto, Meller, Tina, Oertel, Wolfgang H., Respondek, Gesine, Stamelou, Maria, Arzberger, Thomas, Roeber, Sigrun, Müller, Ulrich, Hopfner, Franziska, Pastor, Pau, Brice, Alexis, Durr, Alexandra, Le Ber, Isabelle, Beach, Thomas G., Serrano, Geidy E., Hazrati, Lili-Naz, Litvan, Irene, Rademakers, Rosa, Ross, Owen A., Galasko, Douglas, Boxer, Adam L., Miller, Bruce L., Seeley, Willian W., Van Deerlin, Vivanna M., Lee, Edward B., White, III, Charles L., Morris, Huw, de Silva, Rohan, Crary, John F., Goate, Alison M., Friedman, Jeffrey S., Leung, Yuk Yee, Coppola, Giovanni, Naj, Adam C., Wang, Li-San, Dalgard, Clifton, Dickson, Dennis W., Höglinger, Günter U., Schellenberg, Gerard D., Geschwind, Daniel H., and Lee, Wan-Ping

Published

2024

2. Whole-genome sequencing analysis reveals new susceptibility loci and structural variants associated with progressive supranuclear palsy

Author

Wang, Hui, Chang, Timothy S., Dombroski, Beth A., Cheng, Po-Liang, Patil, Vishakha, Valiente-Banuet, Leopoldo, Farrell, Kurt, Mclean, Catriona, Molina-Porcel, Laura, Rajput, Alex, De Deyn, Peter Paul, Le Bastard, Nathalie, Gearing, Marla, Kaat, Laura Donker, Van Swieten, John C., Dopper, Elise, Ghetti, Bernardino F., Newell, Kathy L., Troakes, Claire, de Yébenes, Justo G., Rábano-Gutierrez, Alberto, Meller, Tina, Oertel, Wolfgang H., Respondek, Gesine, Stamelou, Maria, Arzberger, Thomas, Roeber, Sigrun, Müller, Ulrich, Hopfner, Franziska, Pastor, Pau, Brice, Alexis, Durr, Alexandra, Le Ber, Isabelle, Beach, Thomas G., Serrano, Geidy E., Hazrati, Lili-Naz, Litvan, Irene, Rademakers, Rosa, Ross, Owen A., Galasko, Douglas, Boxer, Adam L., Miller, Bruce L., Seeley, Willian W., Van Deerlin, Vivanna M., Lee, Edward B., White, III, Charles L., Morris, Huw, de Silva, Rohan, Crary, John F., Goate, Alison M., Friedman, Jeffrey S., Leung, Yuk Yee, Coppola, Giovanni, Naj, Adam C., Wang, Li-San, Dalgard, Clifton, Dickson, Dennis W., Höglinger, Günter U., Schellenberg, Gerard D., Geschwind, Daniel H., and Lee, Wan-Ping

Published

2024

3. The Movement Disorder Society Criteria for the Diagnosis of Multiple System Atrophy

Author

Wenning, Gregor K, Stankovic, Iva, Vignatelli, Luca, Fanciulli, Alessandra, Calandra‐Buonaura, Giovanna, Seppi, Klaus, Palma, Jose‐Alberto, Meissner, Wassilios G, Krismer, Florian, Berg, Daniela, Cortelli, Pietro, Freeman, Roy, Halliday, Glenda, Höglinger, Günter, Lang, Anthony, Ling, Helen, Litvan, Irene, Low, Phillip, Miki, Yasuo, Panicker, Jalesh, Pellecchia, Maria Teresa, Quinn, Niall, Sakakibara, Ryuji, Stamelou, Maria, Tolosa, Eduardo, Tsuji, Shoji, Warner, Tom, Poewe, Werner, and Kaufmann, Horacio

Subjects

Neurosciences, Rare Diseases, Prevention, Brain Disorders, 4.1 Discovery and preclinical testing of markers and technologies, Detection, screening and diagnosis, 4.2 Evaluation of markers and technologies, Brain, Consensus, Humans, Magnetic Resonance Imaging, Multiple System Atrophy, Prospective Studies, multiple system atrophy, diagnostic criteria, diagnosis, Clinical Sciences, Human Movement and Sports Sciences, Neurology & Neurosurgery

Abstract

BackgroundThe second consensus criteria for the diagnosis of multiple system atrophy (MSA) are widely recognized as the reference standard for clinical research, but lack sensitivity to diagnose the disease at early stages.ObjectiveTo develop novel Movement Disorder Society (MDS) criteria for MSA diagnosis using an evidence-based and consensus-based methodology.MethodsWe identified shortcomings of the second consensus criteria for MSA diagnosis and conducted a systematic literature review to answer predefined questions on clinical presentation and diagnostic tools relevant for MSA diagnosis. The criteria were developed and later optimized using two Delphi rounds within the MSA Criteria Revision Task Force, a survey for MDS membership, and a virtual Consensus Conference.ResultsThe criteria for neuropathologically established MSA remain unchanged. For a clinical MSA diagnosis a new category of clinically established MSA is introduced, aiming for maximum specificity with acceptable sensitivity. A category of clinically probable MSA is defined to enhance sensitivity while maintaining specificity. A research category of possible prodromal MSA is designed to capture patients in the earliest stages when symptoms and signs are present, but do not meet the threshold for clinically established or clinically probable MSA. Brain magnetic resonance imaging markers suggestive of MSA are required for the diagnosis of clinically established MSA. The number of research biomarkers that support all clinical diagnostic categories will likely grow.ConclusionsThis set of MDS MSA diagnostic criteria aims at improving the diagnostic accuracy, particularly in early disease stages. It requires validation in a prospective clinical and a clinicopathological study. © 2022 The Authors. Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society.

Published

2022

4. Worldwide barriers to genetic testing for movement disorders

Author

Gatto, Emilia M, Walker, Ruth H, Gonzalez, Claudio, Cesarini, Martin, Cossu, Giovanni, Stephen, Christopher D, Balint, Bettina, Rodríguez‐Violante, Mayela, Jankovic, Joseph, Morgante, Francesca, Jinnah, Hyder A, Albanese, Alberto, Amorin, Ignacio, Bhatia, Kailash, Brandabur, Melanie, Canals, Francisca, Cardoso, Francisco, Cardozo, Adriana, Carvalho, Vanessa, Chade, Anabel, Chana, Pedro, Darling, Alejandra, Correia Guedes, Leonor, De la Cerda, Andrés, de Koning‐Tijssen, Marina, Della Coletta, Marcus V, Duquette, Antoine, Espay, Alberto, Etcheverry, Jose, Ferreira, Joaquim, Friedman, Jennifer, Fung, Victor, Ganos, Christos, Ruiz, Pedro Garcia, Gershanik, Oscar, Gross, Kenneth BV, Han‐Joon, Kim, Kaji, Ruyji, Kotschet, Katya, Rosa, Andres Lescano Da, Litvan, Irene, Lubarr, Naomi, Marano, Massimo, Josep Martí, Maria, Martinez Ramirez, Daniel, Miyasaki, Janis, Münchau, Alexander, Chesta, Daniela Muñoz, Pal, Pramod, Peralta, María Cecilia, Phielipp, Nicolás, Maria Riboldi, Giulietta, Oroz, María Cruz Rodríguez, Rodriguez‐Porcel, Federico, Sarva, Harini, Schoels, Ludger, Stamelou, Maria, and Uribe Roca, Claudia

Subjects

Neurodegenerative, Genetic Testing, Clinical Research, Neurosciences, Genetics, Neurological, Asia, Europe, Humans, Middle East, Movement Disorders, Rare Movement Disorders Study Group of the International Parkinson Disease, Movement Disorders Society, Parkinson's disease, chorea, dystonia, genetic and inherited disorders, genetic diagnosis, genetic testing, movement disorders, whole exome sequencing, Clinical Sciences, Neurology & Neurosurgery

Abstract

Background and purposeDespite enormous advances in identifying genetic variants responsible for many neurological diseases, access to genetic testing may be limited in clinical practice. The objective of this study was to assess worldwide access to genetic tests for movement disorders and factors impacting their utilization.MethodsThe Rare Movement Disorders Study Group of the International Parkinson and Movement Disorder Society designed an online survey electronically mailed to all 7815 members.ResultsSurvey data completed by 1269 participants from 109 countries were analysed. Limited access to geneticists and genetic counsellors was reported in many world regions compared to Europe and North America. Availability of genetic testing was limited, with rates of access lower than 50%. Genetic testing for chorea was the most commonly available. For parkinsonism, dystonia, ataxia, hereditary spastic paraplegias and metabolic disorders, there was limited access to genetic testing in all countries compared to Europe and North America, with significant differences found for Africa, Central/South America, Asia. In many regions, genetic testing was supported by either private or public funding. Genetic testing was free of charge in Europe according to 63.5% of respondents. In North America, Africa, Central/South America, Asia and the Middle East access to free of charge genetic testing was by far significantly lower compared to Europe.ConclusionsThis survey highlights difficulties in accessing genetic testing and individuals with expertise in genetics at the worldwide level. In addition, major disparities in genetic testing amongst world regions are highlighted, probably due to a variety of factors including financial barriers.

Published

2021

5. The Progressive Supranuclear Palsy Clinical Deficits Scale

Author

Piot, Ines, Schweyer, Kerstin, Respondek, Gesine, Stamelou, Maria, Sckopke, Philipp, Schenk, Thomas, Goetz, Christopher G, Stebbins, Glenn T, Höglinger, Günter U, Gasser, Thomas, Hermann, Andreas, Höglinger, Günter, Höllerhage, Matthias, Kimmich, Okka, Klockgether, Thomas, Levin, Johannes, Machetanz, Gerrit, Osterrath, Antje, Palleis, Carla, Prudlo, Johannes, Spottke, Annika, Berg, Daniela, Bürk, Katrin, Claßen, Joseph, Eggers, Carsten, Greuel, Andrea, Grimm, Max‐Joseph, Hermann, Lennard, Iankova, Vassilena, Jahn, Klaus, Jost, Wolfgang, Klietz, Martin, Kühn, Andrea, Marxreiter, Franz, Paschen, Steffen, Poetter‐Nerger, Monika, Preisl, Marie‐Therese, Prilop, Lisa, Tönges, Lars, Trenkwalder, Claudia, Warnecke, Tobias, Wegner, Florian, Winkler, Jürgen, Antonini, Angelo, P, Kailash P, L, Adam L, Colosimo, Carlo, Compta, Yaroslau, Corvol, Jean‐Christophe, I, Lawrence I, E, Anthony E, Litvan, Irene, R, Huw R, Nilsson, Christer, and Pantelyat, Alexander

Subjects

Pediatric, Clinical Research, Perinatal Period - Conditions Originating in Perinatal Period, Neurosciences, Brain Disorders, 4.2 Evaluation of markers and technologies, Detection, screening and diagnosis, Neurological, Disease Progression, Female, Fingers, Humans, Male, Motor Skills, Reproducibility of Results, Supranuclear Palsy, Progressive, progressive supranuclear palsy, clinical rating scales, outcome measures, power calculation, DescribePSP study group, ProPSP study group, MDS-endorsed PSP study group, Clinical Sciences, Human Movement and Sports Sciences, Neurology & Neurosurgery

Abstract

BackgroundThere is currently no undisputed, validated, clinically meaningful measure for deficits in the broad spectrum of PSP phenotypes.ObjectiveTo develop a scale to monitor clinical deficits in patients with PSP across its broad phenotypes.MethodsThe Progressive Supranuclear Palsy Clinical Deficits Scale was conceptualized to cover seven clinical domains (Akinesia-rigidity, Bradyphrenia, Communication, Dysphagia, Eye movements, Finger dexterity, and Gait & balance), each scored from 0 to 3 (no, mild, moderate, or severe deficits). User guidelines were developed to standardize its application. Progressive Supranuclear Palsy Clinical Deficits Scale scores were collected in patients fulfilling the MDS-PSP diagnostic criteria in two independent, multicenter, observational studies, both cross-sectionally (exploratory DescribePSP cohort; confirmatory ProPSP cohort) and longitudinally (12-months' follow-up, both cohorts).ResultsCognitive pretesting demonstrated easy scale utility. In total, 164 patients were scored (70.4 ± 7.6 years; 62% males, 35% variant phenotypes). Mean Progressive Supranuclear Palsy Clinical Deficits Scale completion time was 4 minutes. The Progressive Supranuclear Palsy Clinical Deficits Scale total score correlated with existing scales (e.g., Progressive Supranuclear Palsy Rating Scale: R = 0.88; P

Published

2020

6. How to apply the movement disorder society criteria for diagnosis of progressive supranuclear palsy.

Author

Grimm, Max-Joseph, Respondek, Gesine, Stamelou, Maria, Arzberger, Thomas, Ferguson, Leslie, Gelpi, Ellen, Giese, Armin, Grossman, Murray, Irwin, David J, Pantelyat, Alexander, Rajput, Alex, Roeber, Sigrun, van Swieten, John C, Troakes, Claire, Antonini, Angelo, Bhatia, Kailash P, Colosimo, Carlo, van Eimeren, Thilo, Kassubek, Jan, Levin, Johannes, Meissner, Wassilios G, Nilsson, Christer, Oertel, Wolfgang H, Piot, Ines, Poewe, Werner, Wenning, Gregor K, Boxer, Adam, Golbe, Lawrence I, Josephs, Keith A, Litvan, Irene, Morris, Huw R, Whitwell, Jennifer L, Compta, Yaroslau, Corvol, Jean-Christophe, Lang, Anthony E, Rowe, James B, Höglinger, Günter U, and Movement Disorder Society-endorsed PSP Study Group

Subjects

Movement Disorder Society-endorsed PSP Study Group, Brain, Humans, Parkinsonian Disorders, Supranuclear Palsy, Progressive, Ocular Motility Disorders, Sensation Disorders, Autopsy, Retrospective Studies, Cohort Studies, Adult, Aged, Aged, 80 and over, Middle Aged, Societies, Medical, Female, Male, Postural Balance, Cognitive Dysfunction, autopsy, diversity, phenotype, progressive supranuclear palsy, Brain Disorders, Pediatric, Neurosciences, Rare Diseases, Clinical Research, Perinatal Period - Conditions Originating in Perinatal Period, 4.2 Evaluation of markers and technologies, Neurology & Neurosurgery, Clinical Sciences, Human Movement and Sports Sciences

Abstract

BackgroundThe Movement Disorder Society criteria for progressive supranuclear palsy define diagnostic allocations, stratified by certainty levels and clinical predominance types. We aimed to study the frequency of ambiguous multiple allocations and to develop rules to eliminate them.MethodsWe retrospectively collected standardized clinical data by chart review in a multicenter cohort of autopsy-confirmed patients with progressive supranuclear palsy, to classify them by diagnostic certainty level and predominance type and to identify multiple allocations.ResultsComprehensive data were available from 195 patients. More than one diagnostic allocation occurred in 157 patients (80.5%). On average, 5.4 allocations were possible per patient. We developed four rules for Multiple Allocations eXtinction (MAX). They reduced the number of patients with multiple allocations to 22 (11.3%), and the allocations per patient to 1.1.ConclusionsThe proposed MAX rules help to standardize the application of the Movement Disorder Society criteria for progressive supranuclear palsy. © 2019 International Parkinson and Movement Disorder Society.

Published

2019

7. Radiological biomarkers for diagnosis in PSP: Where are we and where do we need to be?

Author

Whitwell, Jennifer L, Höglinger, Günter U, Antonini, Angelo, Bordelon, Yvette, Boxer, Adam L, Colosimo, Carlo, van Eimeren, Thilo, Golbe, Lawrence I, Kassubek, Jan, Kurz, Carolin, Litvan, Irene, Pantelyat, Alexander, Rabinovici, Gil, Respondek, Gesine, Rominger, Axel, Rowe, James B, Stamelou, Maria, Josephs, Keith A, and Group, for the Movement Disorder Society‐endorsed PSP Study

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Aging, Neurosciences, Neurodegenerative, Alzheimer's Disease Related Dementias (ADRD), Acquired Cognitive Impairment, Frontotemporal Dementia (FTD), Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Biomedical Imaging, Brain Disorders, Rare Diseases, Dementia, 4.2 Evaluation of markers and technologies, 4.1 Discovery and preclinical testing of markers and technologies, 2.1 Biological and endogenous factors, Neurological, Biomarkers, Humans, Neuroimaging, Supranuclear Palsy, Progressive, progressive supranuclear palsy, diagnosis, magnetic resonance imaging, positron emission tomography, single-photon emission computed tomography, Movement Disorder Society-endorsed PSP Study Group, Human Movement and Sports Sciences, Neurology & Neurosurgery, Clinical sciences

Abstract

PSP is a pathologically defined neurodegenerative tauopathy with a variety of clinical presentations including typical Richardson's syndrome and other variant PSP syndromes. A large body of neuroimaging research has been conducted over the past two decades, with many studies proposing different structural MRI and molecular PET/SPECT biomarkers for PSP. These include measures of brainstem, cortical and striatal atrophy, diffusion weighted and diffusion tensor imaging abnormalities, [18F] fluorodeoxyglucose PET hypometabolism, reductions in striatal dopamine imaging and, most recently, PET imaging with ligands that bind to tau. Our aim was to critically evaluate the degree to which structural and molecular neuroimaging metrics fulfill criteria for diagnostic biomarkers of PSP. We queried the PubMed, Cochrane, Medline, and PSYCInfo databases for original research articles published in English over the past 20 years using postmortem diagnosis or the NINDS-SPSP criteria as the diagnostic standard from 1996 to 2016. We define a five-level theoretical construct for the utility of neuroimaging biomarkers in PSP, with level 1 representing group-level findings, level 2 representing biomarkers with demonstrable individual-level diagnostic utility, level 3 representing biomarkers for early disease, level 4 representing surrogate biomarkers of PSP pathology, and level 5 representing definitive PSP biomarkers of PSP pathology. We discuss the degree to which each of the currently available biomarkers fit into this theoretical construct, consider the role of biomarkers in the diagnosis of Richardson's syndrome, variant PSP syndromes and autopsy confirmed PSP, and emphasize current shortfalls in the field. © 2017 The Authors. Movement Disorders published by Wiley Periodicals, Inc. on behalf of International Parkinson and Movement Disorder Society.

Published

2017

8. Which ante mortem clinical features predict progressive supranuclear palsy pathology?

Author

Respondek, Gesine, Kurz, Carolin, Arzberger, Thomas, Compta, Yaroslau, Englund, Elisabet, Ferguson, Leslie W, Gelpi, Ellen, Giese, Armin, Irwin, David J, Meissner, Wassilios G, Nilsson, Christer, Pantelyat, Alexander, Rajput, Alex, van Swieten, John C, Troakes, Claire, Josephs, Keith A, Lang, Anthony E, Mollenhauer, Brit, Müller, Ulrich, Whitwell, Jennifer L, Antonini, Angelo, Bhatia, Kailash P, Bordelon, Yvette, Corvol, Jean‐Christophe, Colosimo, Carlo, Dodel, Richard, Grossman, Murray, Kassubek, Jan, Krismer, Florian, Levin, Johannes, Lorenzl, Stefan, Morris, Huw, Nestor, Peter, Oertel, Wolfgang H, Rabinovici, Gil D, Rowe, James B, van Eimeren, Thilo, Wenning, Gregor K, Boxer, Adam, Golbe, Lawrence I, Litvan, Irene, Stamelou, Maria, Höglinger, Günter U, and Group, for the Movement Disorder Society‐Endorsed PSP Study

Subjects

Biomedical and Clinical Sciences, Ophthalmology and Optometry, Frontotemporal Dementia (FTD), Neurodegenerative, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Rare Diseases, Aging, Parkinson's Disease, Dementia, Brain Disorders, Neurosciences, Pick's Disease, Alzheimer's Disease Related Dementias (ADRD), Acquired Cognitive Impairment, 4.2 Evaluation of markers and technologies, 2.1 Biological and endogenous factors, Neurological, Humans, Supranuclear Palsy, Progressive, Progressive supranuclear palsy, clinical features, diagnosis, clinico-pathological series, systematic review, Movement Disorder Society-Endorsed PSP Study Group, Clinical Sciences, Human Movement and Sports Sciences, Neurology & Neurosurgery, Clinical sciences

Abstract

BackgroundProgressive supranuclear palsy (PSP) is a neuropathologically defined disease presenting with a broad spectrum of clinical phenotypes.ObjectiveTo identify clinical features and investigations that predict or exclude PSP pathology during life, aiming at an optimization of the clinical diagnostic criteria for PSP.MethodsWe performed a systematic review of the literature published since 1996 to identify clinical features and investigations that may predict or exclude PSP pathology. We then extracted standardized data from clinical charts of patients with pathologically diagnosed PSP and relevant disease controls and calculated the sensitivity, specificity, and positive predictive value of key clinical features for PSP in this cohort.ResultsOf 4166 articles identified by the database inquiry, 269 met predefined standards. The literature review identified clinical features predictive of PSP, including features of the following 4 functional domains: ocular motor dysfunction, postural instability, akinesia, and cognitive dysfunction. No biomarker or genetic feature was found reliably validated to predict definite PSP. High-quality original natural history data were available from 206 patients with pathologically diagnosed PSP and from 231 pathologically diagnosed disease controls (54 corticobasal degeneration, 51 multiple system atrophy with predominant parkinsonism, 53 Parkinson's disease, 73 behavioral variant frontotemporal dementia). We identified clinical features that predicted PSP pathology, including phenotypes other than Richardson's syndrome, with varying sensitivity and specificity.ConclusionsOur results highlight the clinical variability of PSP and the high prevalence of phenotypes other than Richardson's syndrome. The features of variant phenotypes with high specificity and sensitivity should serve to optimize clinical diagnosis of PSP. © 2017 International Parkinson and Movement Disorder Society.

Published

2017

9. Longitudinal magnetic resonance imaging in progressive supranuclear palsy: A new combined score for clinical trials

Author

Höglinger, Günter U, Schöpe, Jakob, Stamelou, Maria, Kassubek, Jan, del Ser, Teodoro, Boxer, Adam L, Wagenpfeil, Stefan, Huppertz, Hans‐Jürgen, Investigators, for the AL‐108‐231, Investigators, the Tauros MRI, and Group, the Movement Disorder Society‐Endorsed PSP Study

Subjects

Biomedical and Clinical Sciences, Neurosciences, Clinical Sciences, Clinical Research, Clinical Trials and Supportive Activities, Biomedical Imaging, Brain Disorders, Neurodegenerative, Neurological, Aged, Clinical Trials as Topic, Disease Progression, Female, Frontal Lobe, Humans, Longitudinal Studies, Magnetic Resonance Imaging, Male, Mesencephalon, Middle Aged, Supranuclear Palsy, Progressive, Third Ventricle, progressive supranuclear palsy, magnetic resonance imaging, volumetry, power calculation, clinical trials, AL-108-231 Investigators, Tauros MRI Investigators, Movement Disorder Society-Endorsed PSP Study Group, Human Movement and Sports Sciences, Neurology & Neurosurgery, Clinical sciences

Abstract

BackgroundTwo recent, randomized, placebo-controlled phase II/III trials (clinicaltrials.gov: NCT01110720, NCT01049399) of davunetide and tideglusib in progressive supranuclear palsy (PSP) generated prospective, 1-year longitudinal datasets of high-resolution T1-weighted three-dimensional MRI.ObjectiveThe objective of this study was to develop a quantitative MRI disease progression measurement for clinical trials.MethodsThe authors performed a fully automated quantitative MRI analysis employing atlas-based volumetry and provide sample size calculations based on data collected in 99 PSP patients assigned to placebo in these trials. Based on individual volumes of 44 brain compartments and structures at baseline and 52 weeks of follow-up, means and standard deviations of annualized percentage volume changes were used to estimate standardized effect sizes and the required sample sizes per group for future 2-armed, placebo-controlled therapeutic trials.ResultsThe highest standardized effect sizes were found for midbrain, frontal lobes, and the third ventricle. Using the annualized percentage volume change of these structures to detect a 50% change in the 1-year progression (80% power, significance level 5%) required lower numbers of patients per group (third ventricle, n = 32; midbrain, n = 37; frontal lobe, n = 43) than the best clinical scale (PSP rating scale total score, n = 58). A combination of volume changes in these 3 structures reduced the number of required patients to only 20 and correlated best with the progression in the clinical scales.ConclusionsWe propose the 1-year change in the volumes of third ventricle, midbrain, and frontal lobe as combined imaging read-out for clinical trials in PSP that require the least number of patients for detecting efficacy to reduce brain atrophy. © 2017 International Parkinson and Movement Disorder Society.

Published

2017

10. Clinical diagnosis of progressive supranuclear palsy: The movement disorder society criteria.

Author

Höglinger, Günter U, Respondek, Gesine, Stamelou, Maria, Kurz, Carolin, Josephs, Keith A, Lang, Anthony E, Mollenhauer, Brit, Müller, Ulrich, Nilsson, Christer, Whitwell, Jennifer L, Arzberger, Thomas, Englund, Elisabet, Gelpi, Ellen, Giese, Armin, Irwin, David J, Meissner, Wassilios G, Pantelyat, Alexander, Rajput, Alex, van Swieten, John C, Troakes, Claire, Antonini, Angelo, Bhatia, Kailash P, Bordelon, Yvette, Compta, Yaroslau, Corvol, Jean-Christophe, Colosimo, Carlo, Dickson, Dennis W, Dodel, Richard, Ferguson, Leslie, Grossman, Murray, Kassubek, Jan, Krismer, Florian, Levin, Johannes, Lorenzl, Stefan, Morris, Huw R, Nestor, Peter, Oertel, Wolfgang H, Poewe, Werner, Rabinovici, Gil, Rowe, James B, Schellenberg, Gerard D, Seppi, Klaus, van Eimeren, Thilo, Wenning, Gregor K, Boxer, Adam L, Golbe, Lawrence I, Litvan, Irene, and Movement Disorder Society-endorsed PSP Study Group

Subjects

Movement Disorder Society-endorsed PSP Study Group, Humans, Supranuclear Palsy, Progressive, Societies, Medical, Practice Guidelines as Topic, clinical diagnostic criteria, consensus-based, evidence-based, progressive supranuclear palsy, Brain Disorders, Neurosciences, Neurological, Clinical Sciences, Human Movement and Sports Sciences, Neurology & Neurosurgery

Abstract

BackgroundPSP is a neuropathologically defined disease entity. Clinical diagnostic criteria, published in 1996 by the National Institute of Neurological Disorders and Stroke/Society for PSP, have excellent specificity, but their sensitivity is limited for variant PSP syndromes with presentations other than Richardson's syndrome.ObjectiveWe aimed to provide an evidence- and consensus-based revision of the clinical diagnostic criteria for PSP.MethodsWe searched the PubMed, Cochrane, Medline, and PSYCInfo databases for articles published in English since 1996, using postmortem diagnosis or highly specific clinical criteria as the diagnostic standard. Second, we generated retrospective standardized clinical data from patients with autopsy-confirmed PSP and control diseases. On this basis, diagnostic criteria were drafted, optimized in two modified Delphi evaluations, submitted to structured discussions with consensus procedures during a 2-day meeting, and refined in three further Delphi rounds.ResultsDefined clinical, imaging, laboratory, and genetic findings serve as mandatory basic features, mandatory exclusion criteria, or context-dependent exclusion criteria. We identified four functional domains (ocular motor dysfunction, postural instability, akinesia, and cognitive dysfunction) as clinical predictors of PSP. Within each of these domains, we propose three clinical features that contribute different levels of diagnostic certainty. Specific combinations of these features define the diagnostic criteria, stratified by three degrees of diagnostic certainty (probable PSP, possible PSP, and suggestive of PSP). Clinical clues and imaging findings represent supportive features.ConclusionsHere, we present new criteria aimed to optimize early, sensitive, and specific clinical diagnosis of PSP on the basis of currently available evidence. © 2017 International Parkinson and Movement Disorder Society.

Published

2017

11. Evolving concepts in progressive supranuclear palsy and other 4-repeat tauopathies

Author

Stamelou, Maria, Respondek, Gesine, Giagkou, Nikolaos, Whitwell, Jennifer L., Kovacs, Gabor G., and Höglinger, Günter U.

Published

2021

12. Precision Dopaminergic Treatment in a Cohort of Parkinson's Disease Patients Carrying Autosomal Recessive Gene Variants: Clinical Cohort Data and a Mini Review.

Author

Koros, Christos, Simitsi, Athina-Maria, Papagiannakis, Nikolaos, Bougea, Anastasia, Antonelou, Roubina, Pachi, Ioanna, Sfikas, Evangelos, Stanitsa, Evangelia, Angelopoulou, Efthalia, Constantinides, Vasilios C., Papageorgiou, Sokratis G., Potagas, Constantin, Stamelou, Maria, and Stefanis, Leonidas

Subjects

RECESSIVE genes, PARKINSON'S disease, GENETIC variation, DOPAMINE agonists, DOPA

Abstract

Introduction: Parkinson's disease (PD) patients harboring recessive gene variants exhibit a distinct clinical phenotype with an early disease onset and relatively mild symptoms. Data concerning individualized therapy for autosomal recessive PD forms are still scarce. Methods: Demographic and treatment data of a cohort of PD carriers of recessive genes (nine homozygous or compound heterozygous PRKN carriers, four heterozygous PRKN carriers, and three biallelic PINK1 carriers) were evaluated. Results: The average levodopa equivalent daily dose (LEDD) was 806.8 ± 453.5 (range 152–1810) in PRKN carriers and 765 ± 96.6 (range 660–850) in PINK1 carriers. The majority responded to low/moderate doses of levodopa. The response to dopamine agonists (DAs) was often favorable both as initial and longitudinal therapy. In total, 8/13 PRKN and 1/3 PINK1 carriers were treated with amantadine successfully, and this also applied to patients who could not tolerate levodopa or DAs. Conclusions: In the era of personalized treatment, the therapeutic approach in recessive PD gene carriers might differ as compared to idiopathic PD. Lower LEDD doses were efficient even in patients with a very long disease duration, while a few patients were doing well without any levodopa treatment decades after disease initiation. DAs or amantadine could be used as a first and main line treatment regimen if well tolerated. Literature data on therapeutic strategies in carriers of pathogenic mutations in recessive PD genes, including device-aided treatments, will be further discussed. [ABSTRACT FROM AUTHOR]

Published

2024

13. Power calculations and placebo effect for future clinical trials in progressive supranuclear palsy.

Author

Stamelou, Maria, Schöpe, Jakob, Wagenpfeil, Stefan, Del Ser, Teodoro, Bang, Jee, Lobach, Iryna Y, Luong, Phi, Respondek, Gesine, Oertel, Wolfgang H, Boxer, AdamL, Höglinger, Günter U, and AL-108-231 Investigators, Tauros Investigators, and MDS-Endorsed PSP Study Group

Subjects

AL-108-231 Investigators, Tauros Investigators, and MDS-Endorsed PSP Study Group, Humans, Supranuclear Palsy, Progressive, Thiadiazoles, Oligopeptides, Activities of Daily Living, Severity of Illness Index, Sample Size, Placebo Effect, Research Design, Randomized Controlled Trials as Topic, Outcome Assessment, Health Care, clinical trials, placebo effect, power calculation, progressive supranuclear palsy, rate of progression, Clinical Trials and Supportive Activities, Neurosciences, Brain Disorders, Clinical Research, Neurodegenerative, Rare Diseases, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Neurological, Clinical Sciences, Human Movement and Sports Sciences, Neurology & Neurosurgery

Abstract

BackgroundTwo recent randomized, placebo-controlled trials of putative disease-modifying agents (davunetide, tideglusib) in progressive supranuclear palsy (PSP) failed to show efficacy, but generated data relevant for future trials.MethodsWe provide sample size calculations based on data collected in 187 PSP patients assigned to placebo in these trials. A placebo effect was calculated.ResultsThe total PSP-Rating Scale required the least number of patients per group (N = 51) to detect a 50% change in the 1-year progression and 39 when including patients with ≤ 5 years disease duration. The Schwab and England Activities of Daily Living required 70 patients per group and was highly correlated with the PSP-Rating Scale. A placebo effect was not detected in these scales.ConclusionsWe propose the 1-year PSP-Rating Scale score change as the single primary readout in clinical neuroprotective or disease-modifying trials. The Schwab and England Activities of Daily Living could be used as a secondary outcome. © 2016 International Parkinson and Movement Disorder Society.

Published

2016

14. The Landscape of Monogenic Parkinson’s Disease in Populations of Non-European Ancestry: A Narrative Review

Author

Koros, Christos, primary, Bougea, Anastasia, additional, Simitsi, Athina Maria, additional, Papagiannakis, Nikolaos, additional, Angelopoulou, Efthalia, additional, Pachi, Ioanna, additional, Antonelou, Roubina, additional, Bozi, Maria, additional, Stamelou, Maria, additional, and Stefanis, Leonidas, additional

Published

2023

15. Serum Uric Acid as a Putative Biomarker in Prodromal Parkinson’s Disease: Longitudinal Data from the PPMI Study

Author

Koros, Christos, primary, Simitsi, Athina-Maria, additional, Papagiannakis, Nikolaos, additional, Bougea, Anastasia, additional, Prentakis, Andreas, additional, Papadimitriou, Dimitra, additional, Pachi, Ioanna, additional, Beratis, Ion, additional, Stanitsa, Evangelia, additional, Angelopoulou, Efthalia, additional, Antonelou, Roubina, additional, Bregianni, Marianna, additional, Lourentzos, Konstantinos, additional, Papageorgiou, Sokratis G., additional, Bonakis, Anastasios, additional, Trapali, Xenia Geronicola, additional, Stamelou, Maria, additional, and Stefanis, Leonidas, additional

Published

2023

16. Reward Pays the Cost of Noise Reduction in Motor and Cognitive Control

Author

Manohar, Sanjay G., Chong, Trevor T.-J., Apps, Matthew A.J., Batla, Amit, Stamelou, Maria, Jarman, Paul R., Bhatia, Kailash P., and Husain, Masud

Published

2015

17. Author Correction: Safety and efficacy of anti-tau monoclonal antibody gosuranemab in progressive supranuclear palsy: a phase 2, randomized, placebo-controlled trial

Author

Dam, Tien, Boxer, Adam L, Yang, Lili, Shill, Holly, Shprecher, David, Stamelou, Maria, Steiger, Malcolm, Takahashi, Yuji, Takigawa, Hiroshi, Tartaglia, Carmela, Toenges, Lars, Truong, Daniel, Tse, Winona, Tidemann-Miller, Beth, Tuite, Paul, Volc, Dieter, Wills, Anne-Marie A, Woitalla, Dirk, Xie, Tao, Yuasa, Tatsuhiko, Zauber, Sarah Elizabeth, Zesiewicz, Theresa, Kupferman, Joseph, Harper, Kristine, Kamisoglu, Kubra, Wald, Michael J, Graham, Danielle L, Gedney, Liz, O'Gorman, John, Haeberlein, Samantha Budd, Golbe, Lawrence I, Group, PASSPORT Study, Aiba, Ikuko, Antonini, Angelo, Apetauerova, Diana, Azulay, Jean-Philippe, Martinez, Ernest Balaguer, Bang, Jee, Barone, Paolo, Barrett, Matthew, Bega, Danny, Höglinger, Günter, Berg, Daniela, Corrales, Koldo Berganzo, Bordelon, Yvette, Brandt, Moritz, Brueggemann, Norbert, Castelnovo, Giovanni, Ceravolo, Roberto, Chuang, Rosalind, Chung, Sun Ju, Morris, Huw R, Church, Alistair, Corvol, Jean-Christophe, Cudia, Paola, Dale, Marian, Defebvre, Luc, Drapier, Sophie, Driver-Dunckley, Erika D, Ebersbach, Georg, Eggert, Karla M, Ellenbogen, Aaron, Litvan, Irene, Eusebio, Alexandre, Evans, Andrew H, Fedorova, Natalia, Finger, Elizabeth, Foubert-Samier, Alexandra, Ghosh, Boyd, Golbe, Lawrence, Perez, Francisco Grandas, Grossman, Murray, Hall, Deborah, Lang, Anthony E, Hamada, Kyoko, Hasegawa, Kazuko, Hoeglinger, Guenter, Honig, Lawrence, Houghton, David, Huang, Xuemei, Isaacson, Stuart, Koh, SeongBeom, Bojarski, Jaime Kulisevsky, Leigh, Peter Nigel, Lozano, Juan Jose Lopez, Moreno, Jose Luis Lopez-Sendon, Ludolph, Albert Christian, Piudo, Ma Rosario Luquin, Torres, Irene Martinez, McFarland, Nikolaus, Meissner, Wassilios, Mestre, Tiago, Rivera, Pablo Mir, Molho, Eric, Mollenhauer, Britt, Murata, Miho, Obi, Tomokazu, Magne, Fabienne Ory, O'Suilleabhain, Padraig, Pahwa, Rajesh, Pantelyat, Alexander, Grundman, Michael, Pavese, Nicola, Pokhabov, Dmitry, Prudlo, Johannes, Rodriguez-Porcel, Federico, Rowe, James, Savitt, Joseph, Schnitzler, Alfons, Schulz, Joerg B, Seppi, Klaus, and Shah, Binit

Subjects

ddc:610, General Medicine, General Biochemistry, Genetics and Molecular Biology

Published

2022

18. Mutations in ANO3 Cause Dominant Craniocervical Dystonia: Ion Channel Implicated in Pathogenesis

Author

Charlesworth, Gavin, Plagnol, Vincent, Holmström, Kira M., Bras, Jose, Sheerin, Una-Marie, Preza, Elisavet, Rubio-Agusti, Ignacio, Ryten, Mina, Schneider, Susanne A., Stamelou, Maria, Trabzuni, Daniah, Abramov, Andrey Y., Bhatia, Kailash P., and Wood, Nicholas W.

Published

2012

19. Mediterranean diet adherence is related to reduced probability of prodromal Parkinson's disease

Author

Maraki, Maria I., Yannakoulia, Mary, Stamelou, Maria, Stefanis, Leonidas, Xiromerisiou, Georgia, Kosmidis, Mary H., Dardiotis, Efthimios, Hadjigeorgiou, Georgios M., Sakka, Paraskevi, Anastasiou, Costas A., Simopoulou, Eleni, Scarmeas, Nikolaos, Hadjigeorgiou, Georgios M. [0000-0001-5386-4273], Dardiotis, Efthimios [0000-0003-2957-641X], Anastasiou, Costas A. [0000-0002-3536-3034], Yannakoulia, Mary [0000-0003-2171-7337], Kosmidis, Mary H. [0000-0001-8790-1220], Scarmeas, Nikolaos [0000-0001-6453-8908], Stamelou, Maria [0000-0003-1668-9925], and Xiromerisiou, Georgia [0000-0001-7162-3588]

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Constipation, Parkinson's disease, Mediterranean diet, Population, Prodromal Symptoms, Diet, Mediterranean, Older population, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, education, Depression (differential diagnoses), Aged, education.field_of_study, Greece, Depression, business.industry, Incidence, Parkinson Disease, Middle Aged, medicine.disease, Treatment Adherence and Compliance, 030104 developmental biology, Neurology, Quartile, Female, Neurology (clinical), medicine.symptom, business, Biomarkers, 030217 neurology & neurosurgery, Cohort study

Abstract

Background The International Parkinson and Movement Disorder Society recently introduced a methodology for probability score calculation for prodromal PD. Objectives To assess the probability of prodromal PD in an older population and investigate its possible association with Mediterranean diet adherence. Methods Data from a population-based cohort study of older adults (HEllenic Longitudinal Investigation of Aging and Diet) in Greece were used. Probability of prodromal PD was calculated according to International Parkinson and Movement Disorder Society research criteria. A detailed food frequency questionnaire was used to evaluate dietary intake and calculate Mediterranean diet adherence score, ranging from 0 to 55, with higher scores indicating higher adherence. Results Median probability of prodromal PD was 1.9%, ranging from 0.2 to 96.7% in 1,731 PD-free individuals aged ≥ 65 (41% male). Lower probability for prodromal PD (P < 0.001) in the higher Mediterranean diet adherence groups was noted, driven mostly by nonmotor markers of prodromal PD, depression, constipation, urinary dysfunction, and daytime somnolence. Each unit increase in Mediterranean diet score was associated with a 2% decreased probability for prodromal PD (P < 0.001). Compared to participants in the lowest quartile of Mediterranean diet adherence, those in the highest quartile were associated with a ∼21% lower probability for prodromal PD. Conclusions Adherence to the Mediterranean diet is associated with lower probability of prodromal PD in older people. Further studies are needed to elucidate the potential causality of this association, potential relation of the Mediterranean diet to delayed onset or lower incidence of PD, as well as the underlying neurobiological mechanisms. © 2018 International Parkinson and Movement Disorder Society 34 1 48 57

Published

2018

20. Association of the Polygenic Risk Score With the Probability of Prodromal Parkinson’s Disease in Older Adults

Author

Maraki, Maria I., primary, Hatzimanolis, Alexandros, additional, Mourtzi, Niki, additional, Stefanis, Leonidas, additional, Yannakoulia, Mary, additional, Kosmidis, Mary H., additional, Dardiotis, Efthimios, additional, Hadjigeorgiou, Georgios M., additional, Sakka, Paraskevi, additional, Ramirez, Alfredo, additional, Grenier-Boley, Benjamin, additional, Lambert, Jean-Charles, additional, Heilmann-Heimbach, Stefanie, additional, Stamelou, Maria, additional, Scarmeas, Nikolaos, additional, and Xiromerisiou, Georgia, additional

Published

2021

21. Validation of the movement disorder society criteria for the diagnosis of 4-repeat tauopathies

Author

Respondek, Gesine, Grimm, Max‐Joseph, Piot, Ines, Arzberger, Thomas, Compta, Yaroslau, Englund, Elisabet, Ferguson, Leslie W., Gelpi, Ellen, Roeber, Sigrun, Giese, Armin, Grossman, Murray, Irwin, David J., Meissner, Wassilios G., Nilsson, Christer, Pantelyat, Alexander, Rajput, Alex, Swieten, John C., Troakes, Claire, Höglinger, Günter U., Aiba, Ikuko, Antonini, Angelo, Barone, Paolo, Bhatia, Kailash P., Boxer, Adam K., Colosimo, Carlo, Corvol, Jean Christophe, Dickson, Dennis W., Golbe, Lawrence I., Hopfner, Franziska, Josephs, Keith A., Kassubek, Jan, Kovacs, Gabor G., Lang, Anthony E., Levin, Johannes, Litvan, Irene, Höllerhage, Matthias, McFarland, Nikolaus, Morris, Huw R., Müller, Ulrich, Oertel, Wolfgang H., Rowe, James B., Sakakibara, Ruji, Schellenberg, Gerard, Stamelou, Maria, Eimeren, Thilo, Wenning, Gregor K., Whitwell, Jennifer L., and Neurology

Subjects

0301 basic medicine, Male, pathology [Tauopathies], Pediatrics, medicine.medical_specialty, pathology [Supranuclear Palsy, Progressive], Disease, pathology [Parkinsonian Disorders], Progressive supranuclear palsy, 03 medical and health sciences, 0302 clinical medicine, Atrophy, pathology [Brain], medicine, pathology [Multiple System Atrophy], Diagnostic biomarker, Corticobasal degeneration, Humans, ddc:610, Aged, corticobasal degeneration, diagnostic criteria, Four-repeat tauopathies, progressive supranuclear palsy, business.industry, Frontotemporal lobar degeneration, Middle Aged, medicine.disease, Therapeutic trial, pathology [Parkinson Disease], 030104 developmental biology, Neurology, Clinical diagnosis, Female, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

The Movement Disorder Society criteria for progressive supranuclear palsy introduced the category 'probable 4-repeat (4R)-tauopathy' for joint clinical diagnosis of progressive supranuclear palsy and corticobasal degeneration.To validate the accuracy of these clinical criteria for 'probable 4R-tauopathy' to predict underlying 4R-tauopathy pathology.Diagnostic accuracy for 4R-tauopathies according to the established criteria was estimated retrospectively in autopsy-confirmed patients with progressive supranuclear palsy and corticobasal degeneration (grouped as 4R-tauopathies), and Parkinson's disease, multiple system atrophy, and frontotemporal lobar degeneration (grouped as non-4R-tauopathies).We identified 250 cases with progressive supranuclear palsy (N = 195) and corticobasal degeneration (N = 55) and with and non-4R-tauopathies (N = 161). Sensitivity and specificity of 'probable 4R-tauopathy' was 10% and 99% in the first year and 59% and 88% at final record.The new diagnostic category 'probable 4R-tauopathy' showed high specificity and may be suitable for the recruitment of patients with progressive supranuclear palsy and corticobasal degeneration into therapeutic trials targeting 4R-tauopathy. The low sensitivity underpins the need for diagnostic biomarkers. © 2019 International Parkinson and Movement Disorder Society.

Published

2020

22. The clinical and genetic heterogeneity of paroxysmal dyskinesias

Author

Gardiner, Alice R., Jaffer, Fatima, Dale, Russell C., Labrum, Robyn, Erro, Roberto, Meyer, Esther, Xiromerisiou, Georgia, Stamelou, Maria, Walker, Matthew, Kullmann, Dimitri, Warner, Tom, Jarman, Paul, Hanna, Mike, Kurian, Manju A., Bhatia, Kailash P., and Houlden, Henry

Published

2015

23. Commentary: Insulinoma‐Induced Hypoglycemia with Generalized Chorea, Dystonia, and Ataxia: A Neurological Kaleidoscope

Author

Stamelou, Maria, primary, Mishra, Anumeha, additional, Bhattad, Sonali, additional, Pandey, Sanjay, additional, and Fung, Victor S.C., additional

Published

2021

24. Parkinson’s disease in GTP cyclohydrolase 1 mutation carriers

Author

Mencacci, Niccolò E., Isaias, Ioannis U., Reich, Martin M., Ganos, Christos, Plagnol, Vincent, Polke, James M., Bras, Jose, Hersheson, Joshua, Stamelou, Maria, Pittman, Alan M., Noyce, Alastair J., Mok, Kin Y., Opladen, Thomas, Kunstmann, Erdmute, Hodecker, Sybille, Münchau, Alexander, Volkmann, Jens, Samnick, Samuel, Sidle, Katie, Nanji, Tina, Sweeney, Mary G., Houlden, Henry, Batla, Amit, Zecchinelli, Anna L., Pezzoli, Gianni, Marotta, Giorgio, Lees, Andrew, Alegria, Paulo, Krack, Paul, Cormier-Dequaire, Florence, Lesage, Suzanne, Brice, Alexis, Heutink, Peter, Gasser, Thomas, Lubbe, Steven J., Morris, Huw R., Taba, Pille, Koks, Sulev, Majounie, Elisa, Raphael Gibbs, J., Singleton, Andrew, Hardy, John, Klebe, Stephan, Bhatia, Kailash P., and Wood, Nicholas W.

Published

2014

25. Evaluation of the 2020 EAN Virtual Congress: transition from a face-to-face to a virtual meeting

Author

Stamelou, Maria, Struhal, Walter, Ten Cate, Olle, Matczak, Magdalena, Çalışkan, S Ayhan, Soffietti, Riccardo, Marson, Anthony, Zis, Panagiotis, di Lorenzo, Francesco, Sander, Anja, Deuschl, Günther, de Visser, Marianne, and Bassetti, Claudio L.A.

Subjects

evaluation, international congress, quality, transition, virtual congress, 610 Medicine & health

Abstract

BACKGROUND Due to the COVID-19 pandemic, scientific congresses are increasingly being organised as virtual congresses. In May 2020, the European Academy of Neurology (EAN) held a VC, free-of-charge. In the absence of systematic studies on this topic, the aim of this study is to evaluate the attendance and perceived quality of the 2020 EAN virtual congress (VC) compared to the 2019 EAN face-to-face congress (FFC). METHODS Analysis of demographic data of participants obtained from the online registration collected. Comparison of the two congresses based on a survey with questions on the perception of speakers' performance, quality of networking, and other aspects. RESULTS Of 43,596 registered participants, 20,694 active participants attended the VC. Compared to 2019, the number of participants tripled (6916 in 2019) and the cumulated number of participants attending the sessions was five times higher (169,334 in 2020 vs 33,024 in 2019). Out of active participants 55% were from outside Europe, 42% were board-certified neurologists (FFC: 80%), and 21% were students (FFC: 0.6%). The content of the congress was evaluated as 'above expectation' by 56% of the attendees (FFC: 41%). Out of the respondents who had been exposed to earlier EAN congresses 73% preferred the FFC congress compared to the VC (17%). CONCLUSION The VC fulfilled the main mission of organizing high quality EAN congresses despite the restrictions of the impersonal format. The geographical distribution of the participants prove the expected higher inclusivity of a VC. The large participation of students and neurologists in training opens new educational potentials for the EAN.

Published

2021

26. Genotype-Phenotype Relations for the Atypical Parkinsonism Genes: MDSGene Systematic Review

Author

Wittke, Christina, Petkovic, Sonja, Kuhnke, Neele, Lohmann, Katja, Dulovic Mahlow, Marija, Marras, Connie, König, Inke R, Stamelou, Maria, Bonifati, Vincenzo, Lill, Christina M, Kasten, Meike, Huppertz, Hans-Jürgen, Dobricic, Valerija, Höglinger, Günter, Klein, Christine, Arzberger, Thomas, Compta, Yaroslau, Englund, Elisabet, Ferguson, Leslie W, Gelpi, Ellen, Roeber, Sigrun, Giese, Armin, Grossman, Murray, Schaake, Susen, Irwin, David J, Meissner, Wassilios G, Nilsson, Christer, Pantelyat, Alexander, Rajput, Alex, van Swieten, John C, Troakes, Claire, Group, MDS-endorsed PSP Study, Respondek, Gesine, Weissbach, Anne, Madoev, Harutyun, Trinh, Joanne, and Vollstedt, Eva-Juliane

Subjects

Pediatrics, medicine.medical_specialty, Parkinson's disease, Genotype, Levodopa, 03 medical and health sciences, red flags, 0302 clinical medicine, Atrophy, systematic review, Parkinsonian Disorders, medicine, Corticobasal degeneration, Humans, genetics, ddc:610, Cognitive decline, 030304 developmental biology, Genetic testing, 0303 health sciences, medicine.diagnostic_test, business.industry, Parkinsonism, MDSGene, Parkinson Disease, Frontotemporal lobar degeneration, medicine.disease, Supranuclear gaze palsy, ddc, 3. Good health, nervous system diseases, atypical parkinsonism, Phenotype, Neurology, genetics [Parkinsonian Disorders], Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

This Movement Disorder Society Genetic mutation database Systematic Review focuses on monogenic atypical parkinsonism with mutations in the ATP13A2, DCTN1, DNAJC6, FBXO7, SYNJ1, and VPS13C genes. We screened 673 citations and extracted genotypic and phenotypic data for 140 patients (73 families) from 77 publications. In an exploratory fashion, we applied an automated classification procedure via an ensemble of bootstrap-aggregated ('bagged') decision trees to distinguish these 6 forms of monogenic atypical parkinsonism and found a high accuracy of 86.5% (95%CI, 86.3%-86.7%) based on the following 10 clinical variables: age at onset, spasticity and pyramidal signs, hypoventilation, decreased body weight, minimyoclonus, vertical gaze palsy, autonomic symptoms, other nonmotor symptoms, levodopa response quantification, and cognitive decline. Comparing monogenic atypical with monogenic typical parkinsonism using 2063 data sets from Movement Disorder Society Genetic mutation database on patients with SNCA, LRRK2, VPS35, Parkin, PINK1, and DJ-1 mutations, the age at onset was earlier in monogenic atypical parkinsonism (24 vs 40 years; P = 1.2647 × 10-12) and levodopa response less favorable than in patients with monogenic typical presentations (49% vs 93%). In addition, we compared monogenic to nonmonogenic atypical parkinsonism using data from 362 patients with progressive supranuclear gaze palsy, corticobasal degeneration, multiple system atrophy, or frontotemporal lobar degeneration. Although these conditions share many clinical features with the monogenic atypical forms, they can typically be distinguished based on their later median age at onset (64 years; IQR, 57-70 years). In conclusion, age at onset, presence of specific signs, and degree of levodopa response inform differential diagnostic considerations and genetic testing indications in atypical forms of parkinsonism. © 2021 International Parkinson and Movement Disorder Society.

Published

2020

27. Association of the Polygenic Risk Score With the Probability of Prodromal Parkinson's Disease in Older Adults

Author

Maraki, Maria I., Hatzimanolis, Alexandros, Mourtzi, Niki, Stefanis, Leonidas, Yannakoulia, Mary, Kosmidis, Mary H., Dardiotis, Efthimios, Hadjigeorgiou, Georgios M., Sakka, Paraskevi, Ramirez, Alfredo, Grenier-Boley, Benjamin, Lambert, Jean-Charles, Heilmann-Heimbach, Stefanie, Stamelou, Maria, Scarmeas, Nikolaos, Xiromerisiou, Georgia, Maraki, Maria I., Hatzimanolis, Alexandros, Mourtzi, Niki, Stefanis, Leonidas, Yannakoulia, Mary, Kosmidis, Mary H., Dardiotis, Efthimios, Hadjigeorgiou, Georgios M., Sakka, Paraskevi, Ramirez, Alfredo, Grenier-Boley, Benjamin, Lambert, Jean-Charles, Heilmann-Heimbach, Stefanie, Stamelou, Maria, Scarmeas, Nikolaos, and Xiromerisiou, Georgia

Abstract

Several studies have investigated the association of the Parkinson's disease (PD) polygenic risk score (PRS) with several aspects of well-established PD. We sought to evaluate the association of PRS with the prodromal stage of PD. We calculated PRS in a longitudinal sample (n = 1120) of community dwelling individuals >= 65 years from the HELIAD (The Hellenic Longitudinal Investigation of Aging and Diet) study in order to evaluate the association of this score with the probability of prodromal PD or any of the established risk and prodromal markers in MDS research criteria, using regression multi-adjusted models. Increases in PRS estimated from GWAS summary statistics' ninety top SNPS with p < 5 x 10(-8) was associated with increased odds of having probable/possible prodromal PD (i.e., >= 30% probability, OR = 1.033, 95%CI: 1.009-1.057 p = 0.006). From the prodromal PD risk markers, significant association was found between PRS and global cognitive deficit exclusively (p = 0.003). To our knowledge, our study is the first population based study investigating the association between PRS scores and prodromal markers of Parkinson's disease. Our results suggest a strong relationship between the accumulation of many common genetic variants, as measured by PRS, and cognitive deficits.

Published

2021

28. A Modified Progressive Supranuclear Palsy Rating Scale

Author

Volkswagen Foundation, Munich Cluster for Systems Neurology, Ministry for Science and Culture of Lower Saxony, Petermax Müller Foundation, German Center for Neurodegenerative Diseases, International Parkinson and Movement Disorder Society, Grötsch, Marie-Therese, Respondek, Gesine, Colosimo, Carlo, Compta, Yaroslau, Corvol, Jean Christophe, Ferreira, Joaquim, Huber, Meret Koroni, Klietz, Martin, Krey, Lea F. M., Levin, Johannes, Jecmenica-Lukic, Milica, Macías García, Daniel, Meissner, Wassilios G., Mir, Pablo, Morris, Huw, Nilsson, Christer, Rowe, James B., Seppi, Klaus, Stamelou, Maria, van Swieten, John C., Wenning, Gregor, Ser, Teodoro Del, Golbe, Lawrence I., Höglinger, Günter U., Volkswagen Foundation, Munich Cluster for Systems Neurology, Ministry for Science and Culture of Lower Saxony, Petermax Müller Foundation, German Center for Neurodegenerative Diseases, International Parkinson and Movement Disorder Society, Grötsch, Marie-Therese, Respondek, Gesine, Colosimo, Carlo, Compta, Yaroslau, Corvol, Jean Christophe, Ferreira, Joaquim, Huber, Meret Koroni, Klietz, Martin, Krey, Lea F. M., Levin, Johannes, Jecmenica-Lukic, Milica, Macías García, Daniel, Meissner, Wassilios G., Mir, Pablo, Morris, Huw, Nilsson, Christer, Rowe, James B., Seppi, Klaus, Stamelou, Maria, van Swieten, John C., Wenning, Gregor, Ser, Teodoro Del, Golbe, Lawrence I., and Höglinger, Günter U.

Abstract

[Background] The Progressive Supranuclear Palsy Rating Scale is a prospectively validated physician-rated measure of disease severity for progressive supranuclear palsy. We hypothesized that, according to experts' opinion, individual scores of items would differ in relevance for patients' quality of life, functionality in daily living, and mortality. Thus, changes in the score may not equate to clinically meaningful changes in the patient's status., [Objective] The aim of this work was to establish a condensed modified version of the scale focusing on meaningful disease milestones., [Methods] Sixteen movement disorders experts evaluated each scale item for its capacity to capture disease milestones (0 = no, 1 = moderate, 2 = severe milestone). Items not capturing severe milestones were eliminated. Remaining items were recalibrated in proportion to milestone severity by collapsing across response categories that yielded identical milestone severity grades. Items with low sensitivity to change were eliminated, based on power calculations using longitudinal 12-month follow-up data from 86 patients with possible or probable progressive supranuclear palsy., [Results] The modified scale retained 14 items (yielding 0–2 points each). The items were rated as functionally relevant to disease milestones with comparable severity. The modified scale was sensitive to change over 6 and 12 months and of similar power for clinical trials of disease-modifying therapy as the original scale (achieving 80% power for two-sample t test to detect a 50% slowing with n = 41 and 25% slowing with n = 159 at 12 months)., [Conclusions] The modified Progressive Supranuclear Palsy Rating Scale may serve as a clinimetrically sound scale to monitor disease progression in clinical trials and routine. © 2021 International Parkinson and Movement Disorder Society.

Published

2021

29. Genotype–Phenotype Relations for the Atypical Parkinsonism Genes:MDSGene Systematic Review

Author

Wittke, Christina, Petkovic, Sonja, Dobricic, Valerija, Schaake, Susen, Respondek, Gesine, Weissbach, Anne, Madoev, Harutyun, Trinh, Joanne, Vollstedt, Eva Juliane, Kuhnke, Neele, Lohmann, Katja, Dulovic Mahlow, Marija, Marras, Connie, König, Inke R., Stamelou, Maria, Bonifati, Vincenzo, Lill, Christina M., Kasten, Meike, Huppertz, Hans Jürgen, Höglinger, Günter, Klein, Christine, Wittke, Christina, Petkovic, Sonja, Dobricic, Valerija, Schaake, Susen, Respondek, Gesine, Weissbach, Anne, Madoev, Harutyun, Trinh, Joanne, Vollstedt, Eva Juliane, Kuhnke, Neele, Lohmann, Katja, Dulovic Mahlow, Marija, Marras, Connie, König, Inke R., Stamelou, Maria, Bonifati, Vincenzo, Lill, Christina M., Kasten, Meike, Huppertz, Hans Jürgen, Höglinger, Günter, and Klein, Christine

Abstract

This Movement Disorder Society Genetic mutation database Systematic Review focuses on monogenic atypical parkinsonism with mutations in the ATP13A2, DCTN1, DNAJC6, FBXO7, SYNJ1, and VPS13C genes. We screened 673 citations and extracted genotypic and phenotypic data for 140 patients (73 families) from 77 publications. In an exploratory fashion, we applied an automated classification procedure via an ensemble of bootstrap-aggregated (“bagged”) decision trees to distinguish these 6 forms of monogenic atypical parkinsonism and found a high accuracy of 86.5% (95%CI, 86.3%–86.7%) based on the following 10 clinical variables: age at onset, spasticity and pyramidal signs, hypoventilation, decreased body weight, minimyoclonus, vertical gaze palsy, autonomic symptoms, other nonmotor symptoms, levodopa response quantification, and cognitive decline. Comparing monogenic atypical with monogenic typical parkinsonism using 2063 data sets from Movement Disorder Society Genetic mutation database on patients with SNCA, LRRK2, VPS35, Parkin, PINK1, and DJ-1 mutations, the age at onset was earlier in monogenic atypical parkinsonism (24 vs 40 years; P = 1.2647 × 10−12) and levodopa response less favorable than in patients with monogenic typical presentations (49% vs 93%). In addition, we compared monogenic to nonmonogenic atypical parkinsonism using data from 362 patients with progressive supranuclear gaze palsy, corticobasal degeneration, multiple system atrophy, or frontotemporal lobar degeneration. Although these conditions share many clinical features with the monogenic atypical forms, they can typically be distinguished based on their later median age at onset (64 years; IQR, 57–70 years). In conclusion, age at onset, presence of specific signs, and degree of levodopa response inform differential diagnostic considerations and genetic testing indications in atypical forms of parkinsonism.

Published

2021

30. Evaluation of the 2020 European Academy of Neurology virtual congress: transition from a face-to-face to a virtual meeting

Author

Onderwijscentrum Onderwijs, Stamelou, Maria, Struhal, Walter, Ten Cate, Olle, Matczak, Magdalena, Çalışkan, Süleyman Ayhan, Soffietti, Riccardo, Marson, Anthony, Zis, Panagiotis, di Lorenzo, Francesco, Sander, Anja, Deuschl, Günther, de Visser, Marianne, Bassetti, Claudio L A, Onderwijscentrum Onderwijs, Stamelou, Maria, Struhal, Walter, Ten Cate, Olle, Matczak, Magdalena, Çalışkan, Süleyman Ayhan, Soffietti, Riccardo, Marson, Anthony, Zis, Panagiotis, di Lorenzo, Francesco, Sander, Anja, Deuschl, Günther, de Visser, Marianne, and Bassetti, Claudio L A

Published

2021

31. Hormetic Responses of Photosystem II in Tomato to Botrytis cinerea

Author

Stamelou, Maria-Lavrentia, primary, Sperdouli, Ilektra, additional, Pyrri, Ioanna, additional, Adamakis, Ioannis-Dimosthenis S., additional, and Moustakas, Michael, additional

Published

2021

32. The non-motor syndrome of primary dystonia: clinical and pathophysiological implications

Author

Stamelou, Maria, Edwards, Mark J., Hallett, Mark, and Bhatia, Kailash P.

Published

2012

33. Rational therapeutic approaches to progressive supranuclear palsy

Author

Stamelou, Maria, de Silva, Rohan, Arias-Carrión, Oscar, Boura, Evangelia, Höllerhage, Matthias, Oertel, Wolfgang H., Müller, Ulrich, and Höglinger, Günter U.

Published

2010

34. Higher probability of prodromal Parkinson disease is related to lower cognitive performance

Author

Bougea, Anastasia, Maraki, Maria I., Yannakoulia, Mary, Stamelou, Maria, Xiromerisiou, Georgia, Kosmidis, Mary H., Ntanasi, Eva, Dardiotis, Efthimios, Hadjigeorgiou, Georgios M., Sakka, Paraskevi, Anastasiou, Costas A., Stefanis, Leonidas, Scarmeas, Nikolaos, Hadjigeorgiou, Georgios M. [0000-0001-5386-4273], Dardiotis, Efthimios [0000-0003-2957-641X], Anastasiou, Costas A. [0000-0002-3536-3034], Yannakoulia, Mary [0000-0003-2171-7337], Kosmidis, Mary H. [0000-0001-8790-1220], Scarmeas, Nikolaos [0000-0001-6453-8908], Stamelou, Maria [0000-0003-1668-9925], Xiromerisiou, Georgia [0000-0001-7162-3588], Ntanasi, Eva [0000-0001-9311-0994], and Bougea, Anastasia [0000-0003-3006-8711]

Subjects

0301 basic medicine, Male, Population, Prodromal Symptoms, Disease, Standard score, Neuropsychological Tests, 03 medical and health sciences, 0302 clinical medicine, Cognition, medicine, Dementia, Humans, Cognitive Dysfunction, Effects of sleep deprivation on cognitive performance, education, Aged, Aged, 80 and over, education.field_of_study, business.industry, Parkinson Disease, Middle Aged, medicine.disease, Causality, 030104 developmental biology, Cohort, Disease Progression, Female, Neurology (clinical), business, 030217 neurology & neurosurgery, Clinical psychology

Abstract

ObjectiveGiven the limited information on cognitive function before Parkinson disease (PD) clinical onset in the general population, we sought to assess prodromal PD (pPD) probability and relate it to detailed cognitive performance in a community cohort.MethodsIn a population-based cohort of 1,629 dementia-free and PD-free participants ≥65 years of age in Greece, we assessed probability of pPD according to the International Parkinson and Movement Disorder Society's criteria. Clinical cognitive diagnoses (cognitively unimpaired, mild cognitive impairment [MCI], dementia) considering neuropsychological testing and functional status were assigned in consensus conferences. Cognitive performance in 5 cognitive domains was assessed by a detailed neuropsychological battery and summarized in the form of z scores. We investigated associations between pPD probability (and its individual constituents) and cognitive outcomes.ResultsThe median probability of pPD was 1.81% (0.2%–96.7%). Participants with MCI had higher probability of pPD compared to those with normal cognition (p < 0.001). Higher probability of pPD was related to lower performance in all cognitive domains (memory, language, executive, attention, and visuospatial function) (p < 0.001). Lower cognitive performance was further associated with certain nonmotor markers of pPD, such as daytime somnolence, depression, urinary dysfunction, constipation, and subthreshold parkinsonism (p < 0.001).ConclusionsHigher probability of pPD was associated with lower cognitive performance in all domains and higher probability of MCI. This may reflect a widespread pathologic process although future studies are warranted to infer causality. These results suggest to clinicians that they should assess cognition early, and to researchers that they should further look into the possible mechanisms that may underlie this observation.

Published

2018

35. DaTSCAN (123I-FP-CIT SPECT) imaging in early versus mid and late onset Parkinson's disease: Longitudinal data from the PPMI study

Author

Koros, Christos Simitsi, Athina-Maria Prentakis, Andreas and Papagiannakis, Nikolaos Bougea, Anastasia Pachi, Ioanna and Papadimitriou, Dimitra Beratis, Ion Papageorgiou, Sokratis G. and Stamelou, Maria Trapali, Xenia Geronicola Stefanis, Leonidas

Abstract

Introduction: It has been reported that early onset Parkinson’s Disease (PD) patients have a less profound dopaminergic degeneration. The aim of the current study was to determine whether there are longitudinal differences in dopaminergic denervation [signal reduction in 123I-FP-CIT SPECT] in early versus mid and late onset PD. Methods: DaTSCAN (123I-FP-CIT SPECT) imaging was acquired at Parkinson’s Progression Markers Initiative (PPMI) imaging centers and sent to the imaging core for calculation of striatal binding ratios. Data from the PPMI database of 58 early de novo PD patients (age 50 years). Results: Although raw striatal binding ratios were higher in early onset versus mid/late onset PD, especially on the ipsilateral side, such differences were not observed, and were in fact reversed in the contralateral putamen, after age correction. The rate of signal decline was similar between the two groups. Interestingly, based on both raw and age-adjusted data, caudate nucleus and putamen asymmetry (contralateral/ipsilateral ratio) was more pronounced in early onset PD. Striatal asymmetry also significantly correlated with age at onset as a continuous variable. Conclusion: Early onset PD patients exhibited similar rates of decline of dopaminergic denervation compared to mid/late onset PD. These results are not supportive of a more benign disease in this subgroup. The more pronounced asymmetry in early onset PD may however signify a qualitatively different pattern of neurodegeneration compared to mid/late onset PD.

Published

2020

36. Extensive validation study of the Parkinson's Disease Composite Scale

Author

Martinez-Martin, P. Radicati, F. G. Rodriguez Blazquez, C. and Wetmore, J. Kovacs, N. Chaudhuri, K. Ray Stocchi, F. and Vuletic, Vladimira Falup-Pecurariu, Cristian Diaconu, Stefania and Johansson, Anders Sundgren, Mathias Simitsi, Athima and Stefanis, Leonidas Gurevich, Tanya Migirov-Sanderovich, Angel and Ezra, Adi Guekht, Alla Popov, Georgy Stamelou, Maria and Giagkou, Nikolaos Stefani, Alessandro Cerroni, Rocco Corbo, Massimo Grassi, Andrea Dellaporta, Dionysia Tsolaki, Magda and Ariadne, Vakirli Kefalopoulou, Zinovia Ellul, John Mir, Pablo Adarmes, Astrid D. Mendez-del-Barrio, Carlota and Skorvanek, Matej Necpal, Jan Bostantjopoulou, Sevasti Zoe, Katsarou Minar, Michal Simu, Mihaela Rosca, Cecilia and Popovici, Maria Kostic, Vladimir S. Marti, Maria J. and Planelles, Lluis Kovacs, Norbert Aschermann, Zsuzsanna and Juhasz, Annamaria Harmat, Mark PDCS European Study Grp

Subjects

hemic and immune systems

Abstract

Background and purpose A composite instrument able to rapidly and reliably assess the most relevant motor and non-motor afflictions suffered by Parkinson’s disease (PD) patients in a real world clinic setting is an unmet need. The recently validated PD Composite Scale (PDCS) was designed to fulfil this gap as a quick, comprehensive PD assessment. The objective of this study was extensive evaluation of the PDCS’s clinimetric properties using a large international sample. Methods This was a cross-sectional study in which the PDCS, the Movement Disorder Society Unified Parkinson’s Disease Rating Scale and the Clinical Impression of Severity Index for PD were applied. Basic clinimetric attributes of the PDCS were analysed. Results In total, 776 PD patients were included. The PDCS total score showed negligible floor and ceiling effects. Three factors (54.5% of the variance) were identified: factor 1 included motor impairment, fluctuations and disability; factor 2, non-motor symptoms; and factor 3, tremor and complications of therapy. Cronbach’s alpha was from 0.66 to 0.79. Inter-rater reliability showed weighted kappa values from 0.79 to 0.98 for items and intraclass correlation coefficient values from 0.95 (Disability) to 0.99 (Motor and total score). The Bland-Altmann method, however, showed irregular concordance. PDCS standard error of measurement and convergent validity with equivalent constructs of other measures were satisfactory (>= 0.70). PDCS scores significantly differed by Hoehn and Yahr stage. Conclusion Overall, in line with previous findings, the PDCS is a feasible, acceptable, valid, reliable and precise instrument for quickly and comprehensively assessing PD patients.

Published

2019

37. Treatable inherited rare movement disorders

Author

Jinnah, H. A., Albanese, Alberto, Jankovic, Joseph, Kaji, Ryuji, Kotschet, Katya, Marras, Connie, Miyasaki, Janis M, Morgante, Francesca, Munchau, Alexander, Pal, Pramod Kumar, Rodriguez Oroz, Maria C, Rodríguez-Violante, Mayela, Bhatia, Kailash P, Schöls, Ludger, Stamelou, Maria, Tijssen, Marina, Uribe Roca, Claudia, de la Cerda, Andres, Gatto, Emilia M, Disorders, International Parkinson's Disease Movement Disorders Society Task Force on Rare Movement, Cardoso, Francisco, Da Prat, Gustavo, de Koning, Tom J, Espay, Alberto J, Fung, Victor, Garcia-Ruiz, Pedro J, and Gershanik, Oscar

Subjects

experimental therapeutics, inherited disease, orphan disease, Rare disease, treatment, Neurology, Neurology (clinical), Clinical Trials as Topic, Movement Disorders, genetics [Rare Diseases], therapy [Movement Disorders], genetics [Movement Disorders], Article, therapy [Rare Diseases], Settore MED/26 - NEUROLOGIA, Rare Diseases, Treatment Outcome, Humans, methods [Clinical Trials as Topic], ddc:610

Abstract

There are many rare movement disorders, and new ones are described every year. Because they are not well recognized, they often go undiagnosed for long periods of time. However, early diagnosis is becoming increasingly important. Rapid advances in our understanding of the biological mechanisms responsible for many rare disorders have enabled the development of specific treatments for some of them. Well-known historical examples include Wilson disease and dopa-responsive dystonia, for which specific and highly effective treatments have life-altering effects. In recent years, similarly specific and effective treatments have been developed for more than 30 rare inherited movement disorders. These treatments include specific medications, dietary changes, avoidance or management of certain triggers, enzyme replacement therapy, and others. This list of treatable rare movement disorders is likely to grow during the next few years because a number of additional promising treatments are actively being developed or evaluated in clinical trials. © 2017 International Parkinson and Movement Disorder Society.

Published

2018

38. Selective cognitive impairment and hyposmia in p.A53T SNCA PD vs typical PD

Author

Koros, Christos Stamelou, Maria Simitsi, Athina Beratis, Ion and Papadimitriou, Dimitra Papagiannakis, Nikolaos Fragkiadaki, Stella Kontaxopoulou, Dionysia Papageorgiou, Sokratis G. and Stefanis, Leonidas

Abstract

ObjectiveTo evaluate nonmotor symptoms in early SNCA/p.A53T Parkinson disease (PD) (A53T PD) compared to typical PD (tPD).MethodsThe presence of hyposmia, neuropsychiatric, dysautonomic, and sleep disturbances was assessed by standardized questionnaires and validated scales in 18 patients with A53T PD and 18 patients with tPD, matched for age, sex, and disease duration. All patients were enrolled into the Parkinson's Progression Markers Initiative study.ResultsThe levodopa equivalent daily dose was higher in the A53T PD (p = 0.018) group vs the tPD group. Scores on the University of Pennsylvania Smell Identification Test (p = 0.001), Benton Judgement of Line Orientation test (p = 0.001), Letter Number Sequencing Test (p = 0.002), and phonemic verbal fluency (p = 0.002) were lower in the A53T PD group vs the tPD group. In contrast, overall cognition, verbal memory, and semantic fluency were similar between groups.ConclusionThe observed selective cognitive impairment reflecting frontal-parietal network dysfunction, together with impaired olfaction, define a set of nonmotor dysfunctions related to A53T PD. These results have implications for the prognosis of patients with A53T PD. Moreover, as the archetypal -synucleinopathy, such results may give insights into tPD.

Published

2018

39. 123I-FP-CIT SPECT [(123) I-2 beta-carbomethoxy-3 beta-(4-iodophenyl)-N-(3-fluoropropyl) nortropane single photon emission computed tomography] Imaging in a p.A53T alpha-synuclein Parkinson’s disease cohort versus Parkinson’s disease

Author

Koros, Christos Simitsi, Athina Prentakis, Andreas Beratis, Ion Papadimitriou, Dimitra Kontaxopoulou, Dionysia and Fragkiadaki, Stella Papagiannakis, Nikolaos Seibyl, John and Marek, Kenneth Papageorgiou, Sokratis G. Trapali, Xenia Geronicola Stamelou, Maria Stefanis, Leonidas

Abstract

Background: The p.A53T point mutation in the alpha-synuclein gene (SNCA) is a rare but highly relevant cause of autosomal dominant Parkinson’s disease (PD). Objectives: The objective of this study was to assess striatal dopaminergic denervation in a cohort of symptomatic carriers of the p.A53T SNCA mutation as compared to PD patients. Methods: Data from the Parkinson’s Progression Markers Initiative database of 11 symptomatic p.A53T SNCA mutation carriers who underwent 123I-FP-CIT SPECT [(123) I-2 beta-carbomethoxy-3 beta-(4-iodophenyl)-N-(3-fluoropropyl) nortropane single photon emission computed tomography] imaging at our site were compared with those of 33 age-, sex-, and disease duration-matched PD patients. Results: The p.A53T mutation carriers had significantly lower caudate nucleus binding ratio both contralaterally and ipsilaterally to the most affected side (P = .002 and P = .006) and a decreased contralateral caudate/putamen signal ratio (P = .007) as compared to PD. A similar degree of striatal asymmetry was observed in both subgroups. No correlation between scores in neuropsychological tests and caudate nucleus dopaminergic denervation could be demonstrated. Conclusions: PD patients harboring the p.A53T SNCA mutation show evidence of a more severe nigrostriatal denervation, especially evident in the caudate nucleus. The lack of significant differences in the putaminal binding ratios may reflect a floor effect or a true preferential targeting of the caudate terminals in p.A53T SNCA-associated PD. (c) 2018 International Parkinson and Movement Disorder Society

Published

2018

40. Genomewide association study in cervical dystonia demonstrates possible association with sodium leak channel

Author

Mok, Kin Y, Schneider, Susanne A, Trabzuni, Daniah, Stamelou, Maria, Edwards, Mark, Kasperaviciute, Dalia, Pickering-Brown, Stuart, Silverdale, Monty, Hardy, John, and Bhatia, Kailash P

Subjects

Male, cervical dystonia, NALCN, Genotype, Membrane Proteins, imputation, Exons, Middle Aged, Polymorphism, Single Nucleotide, Ion Channels, Sodium Channels, England, Gene Frequency, GWAS, Humans, sodium leaking channel, Female, Genetic Predisposition to Disease, Research Articles, Torticollis, Aged, Genome-Wide Association Study

Abstract

Dystonia is a common movement disorder. A number of monogenic causes have been identified. However, the majority of dystonia cases are not explained by single gene defects. Cervical dystonia is one of the commonest forms without genetic causes identified. This pilot study aimed to identify large effect-size risk loci in cervical dystonia. A genomewide association study (GWAS) was performed. British resident cervical dystonia patients of European descent were genotyped using the Illumina-610-Quad. Comparison was made with controls of European descent from the Wellcome Trust Case Control Consortium using logistic regression algorithm from PLINK. SNPs not genotyped by the array were imputed with 1000 Genomes Project data using the MaCH algorithm and minimac. Postimputation analysis was done with the mach2dat algorithm using a logistic regression model. After quality control measures, 212 cases were compared with 5173 controls. No single SNP passed the genomewide significant level of 5 × 10(-8) in the analysis of genotyped SNP in PLINK. Postimputation, there were 5 clusters of SNPs that had P value5 × 10(-6) , and the best cluster of SNPs was found near exon 1 of NALCN, (sodium leak channel) with P = 9.76 × 10(-7) . Several potential regions were found in the GWAS and imputation analysis. The lowest P value was found in NALCN. Dysfunction of this ion channel is a plausible cause for dystonia. Further replication in another cohort is needed to confirm this finding. We make this data publicly available to encourage further analyses of this disorder.

Published

2013

41. Dystonic opisthotonus: A 'red flag' for neurodegeneration with brain iron accumulation syndromes?

Author

Stamelou, Maria, Lai, Scarlett C, Aggarwal, Annu, Schneider, Susanne A, Houlden, Henry, Yeh, Tu-Hsueh, Batla, Amit, Lu, Chin-Song, Bhatt, Mohit, and Bhatia, Kailash P

Subjects

neurodegeneration with brain iron accumulation, Adult, Brain Chemistry, Male, NBIA, Brain, retrocollis, Neurodegenerative Diseases, PLA2G6, Iron Metabolism Disorders, extensor axial dystonia, PANK2, Diagnosis, Differential, Young Adult, Viewpoint, Dystonic Disorders, Humans, Female, opisthotonus

Abstract

Back arching was reported in one of the very first patients with neurodegeneration with brain iron accumulation syndrome (NBIAs) published in 1936. However, recent reports have mainly focused on the genetic and imaging aspects of these disorders, and the phenotypic characterization of the dystonia has been lost. In evaluating patients with NBIAs in our centers, we have observed that action-induced dystonic opisthotonus is a common and characteristic feature of NBIAs. Here, we present a case series of patients with NBIAs presenting this feature demonstrated by videos. We suggest that dystonic opisthotonus could be a useful “red flag” for clinicians to suspect NBIAs, and we discuss the differential diagnosis of this feature. This would be particularly useful in identifying patients with NBIAs and no iron accumulation as yet on brain imaging (for example, as in phospholipase A2, group IV (cytosolic, calcium-independent) [PLA2G6]-related disorders), and it has management implications. © 2013 The Authors. Movement Disorders published by Wiley Periodicals, Inc. on behalf of International Parkinson and Movement Disorder Society.

Published

2013

42. Advances in the Clinical Differential Diagnosis of Parkinson's Disease

Author

Schreglmann, Sebastian R. Bhatia, Kailash P. Stamelou, Maria

Published

2017

43. The Motor Syndrome of Parkinson's Disease

Author

Erro, Roberto Stamelou, Maria

Published

2017

44. Nonmotor Features in Atypical Parkinsonism

Author

Bhatia, Kailash P. Stamelou, Maria

Published

2017

45. Mutations in HPCA Cause Autosomal-Recessive Primary Isolated Dystonia

Author

Charlesworth, Gavin, Angelova, Plamena R., Bartolomé-Robledo, Fernando, Ryten, Mina, Trabzuni, Daniah, Stamelou, Maria, Abramov, Andrey Y., Bhatia, Kailash P., and Wood, Nicholas W.

Published

2015

46. ALS2 mutations

Author

Sheerin, Una-Marie, Schneider, Susanne A., Carr, Lucinda, Deuschl, Guenther, Hopfner, Franziska, Stamelou, Maria, Wood, Nicholas W., and Bhatia, Kailash P.

Subjects

Adult, Male, Adolescent, Amyotrophic Lateral Sclerosis, Homozygote, Proteins, Genes, Recessive, Article, Pedigree, Consanguinity, Phenotype, Dystonic Disorders, Mutation, Guanine Nucleotide Exchange Factors, Humans, Exome, Female, Carrier Proteins, Child, Sequence Analysis

Abstract

Objective: To determine the genetic etiology in 2 consanguineous families who presented a novel phenotype of autosomal recessive juvenile amyotrophic lateral sclerosis associated with generalized dystonia. Methods: A combination of homozygosity mapping and whole-exome sequencing in the first family and Sanger sequencing of candidate genes in the second family were used. Results: Both families were found to have homozygous loss-of-function mutations in the amyotrophic lateral sclerosis 2 (juvenile) (ALS2) gene. Conclusions: We report generalized dystonia and cerebellar signs in association with ALS2-related disease. We suggest that the ALS2 gene should be screened for mutations in patients who present with a similar phenotype.

Published

2014

47. Clinical Diagnosis of Progressive Supranuclear Palsy: The Movement Disorder Society Criteria

Author

Hoeglinger, Guenter U., Respondek, Gesine, Stamelou, Maria, Kurz, Carolin, Josephs, Keith A., Lang, Anthony E., Mollenhauer, Brit, Mueller, Ulrich, Nilsson, Christer, Whitwell, Jennifer L., Arzberger, Thomas, Englund, Elisabet, Gelpi, Ellen, Giese, Armin, Irwin, David J., Meissner, Wassilios G., Pantelyat, Alexander, Rajput, Alex, van Swieten, John C., Troakes, Claire, Antonini, Angelo, Bhatia, Kailash P., Bordelon, Yvette, Compta, Yaroslau, Corvol, Jean-Christophe, Colosimo, Carlo, Dickson, Dennis W., Dodel, Richard, Ferguson, Leslie, Grossman, Murray, Kassubek, Jan, Krismer, Florian, Levin, Johannes, Lorenzl, Stefan, Morris, Huw R., Nestor, Peter, Oertel, Wolfgang H., Poewe, Werner, Rabinovici, Gil, Rowe, James B., Schellenberg, Gerard D., Seppi, Klaus, van Eimeren, Thilo, Wenning, Gregor K., Boxer, Adam L., Golbe, Lawrence I., Litvan, Irene, Hoeglinger, Guenter U., Respondek, Gesine, Stamelou, Maria, Kurz, Carolin, Josephs, Keith A., Lang, Anthony E., Mollenhauer, Brit, Mueller, Ulrich, Nilsson, Christer, Whitwell, Jennifer L., Arzberger, Thomas, Englund, Elisabet, Gelpi, Ellen, Giese, Armin, Irwin, David J., Meissner, Wassilios G., Pantelyat, Alexander, Rajput, Alex, van Swieten, John C., Troakes, Claire, Antonini, Angelo, Bhatia, Kailash P., Bordelon, Yvette, Compta, Yaroslau, Corvol, Jean-Christophe, Colosimo, Carlo, Dickson, Dennis W., Dodel, Richard, Ferguson, Leslie, Grossman, Murray, Kassubek, Jan, Krismer, Florian, Levin, Johannes, Lorenzl, Stefan, Morris, Huw R., Nestor, Peter, Oertel, Wolfgang H., Poewe, Werner, Rabinovici, Gil, Rowe, James B., Schellenberg, Gerard D., Seppi, Klaus, van Eimeren, Thilo, Wenning, Gregor K., Boxer, Adam L., Golbe, Lawrence I., and Litvan, Irene

Abstract

Background: PSP is a neuropathologically defined disease entity. Clinical diagnostic criteria, published in 1996 by the National Institute of Neurological Disorders and Stroke/Society for PSP, have excellent specificity, but their sensitivity is limited for variant PSP syndromes with presentations other than Richardson's syndrome. Objective: We aimed to provide an evidence-and consensus-based revision of the clinical diagnostic criteria for PSP. Methods: We searched the PubMed, Cochrane, Med-line, and PSYCInfo databases for articles published in English since 1996, using postmortem diagnosis or highly specific clinical criteria as the diagnostic standard. Second, we generated retrospective standardized clinical data from patients with autopsy-confirmed PSP and control diseases. On this basis, diagnostic criteria were drafted, optimized in two modified Delphi evaluations, submitted to structured discussions with consensus procedures during a 2-day meeting, and refined in three further Delphi rounds. Results: Defined clinical, imaging, laboratory, and genetic findings serve as mandatory basic features, mandatory exclusion criteria, or context-dependent exclusion criteria. We identified four functional domains (ocular motor dysfunction, postural instability, akinesia, and cognitive dysfunction) as clinical predictors of PSP. Within each of these domains, we propose three clinical features that contribute different levels of diagnostic certainty. Specific combinations of these features define the diagnostic criteria, stratified by three degrees of diagnostic certainty (probable PSP, possible PSP, and suggestive of PSP). Clinical clues and imaging findings represent supportive features. Conclusions: Here, we present new criteria aimed to optimize early, sensitive, and specific clinical diagnosis of PSP on the basis of currently available evidence. (C) 2017 International Parkinson and Movement Disorder Society

Published

2017

48. Radiological Biomarkers for Diagnosis in PSP: Where Are We and Where Do We Need to Be?

Author

Whitwell, Jennifer L., Hoelinger, Guenter U., Antonini, Angelo, Bordelon, Yvette, Boxer, Adam L., Colosimo, Carlo, van Eimeren, Thilo, Golbe, Lawrence I., Kassubek, Jan, Kurz, Carolin, Litvan, Irene, Pantelyat, Alexander, Rabinovici, Gil, Respondek, Gesine, Rominger, Axel, Rowe, James B., Stamelou, Maria, Josephs, Keith A., Whitwell, Jennifer L., Hoelinger, Guenter U., Antonini, Angelo, Bordelon, Yvette, Boxer, Adam L., Colosimo, Carlo, van Eimeren, Thilo, Golbe, Lawrence I., Kassubek, Jan, Kurz, Carolin, Litvan, Irene, Pantelyat, Alexander, Rabinovici, Gil, Respondek, Gesine, Rominger, Axel, Rowe, James B., Stamelou, Maria, and Josephs, Keith A.

Abstract

PSP is a pathologically defined neurodegenerative tauopathy with a variety of clinical presentations including typical Richardson's syndrome and other variant PSP syndromes. A large body of neuroimaging research has been conducted over the past two decades, with many studies proposing different structural MRI and molecular PET/SPECT biomarkers for PSP. These include measures of brainstem, cortical and striatal atrophy, diffusion weighted and diffusion tensor imaging abnormalities, [18F] fluorodeoxyglucose PET hypometabolism, reductions in striatal dopamine imaging and, most recently, PET imaging with ligands that bind to tau. Our aim was to critically evaluate the degree to which structural and molecular neuroimaging metrics fulfill criteria for diagnostic biomarkers of PSP. We queried the PubMed, Cochrane, Medline, and PSYCInfo databases for original research articles published in English over the past 20 years using postmortem diagnosis or the NINDS-SPSP criteria as the diagnostic standard from 1996 to 2016. We define a five-level theoretical construct for the utility of neuroimaging biomarkers in PSP, with level 1 representing group-level findings, level 2 representing biomarkers with demonstrable individual-level diagnostic utility, level 3 representing biomarkers for early disease, level 4 representing surrogate biomarkers of PSP pathology, and level 5 representing definitive PSP biomarkers of PSP pathology. We discuss the degree to which each of the currently available biomarkers fit into this theoretical construct, consider the role of biomarkers in the diagnosis of Richardson's syndrome, variant PSP syndromes and autopsy confirmed PSP, and emphasize current shortfalls in the field. (C) 2017 The Authors. Movement Disorders published by Wiley Periodicals, Inc. on behalf of International Parkinson and Movement Disorder Society.

Published

2017

49. Diagnosis of Parkinson's disease on the basis of clinical and genetic classification: A population-based modelling study

Author

Nalls, Mike A, McLean, Cory Y, Hardy, John, Seppi, Klaus, Reiter, Eva, Shill, Holly, Fernandez, Hubert, Ahmed, Anwar, Berg, Daniela, Wurster, Isabel, Mari, Zoltan, Brooks, David, Pavese, Nicola, Gasser, Thomas, Barone, Paolo, Isaacson, Stuart, Espay, Alberto, Rowe, Dominic, Brandabur, Melanie, Tetrud, James, Liang, Grace, Marder, Karen, Corvol, Jean-Christophe, Martí Masso, Jose Felix, Brice, Alexis, Tolosa, Eduardo, Aasly, Jan O, Giladi, Nir, Stefanis, Leonidas, Leary, Laura, Riordan, Cheryl, Rees, Linda, Sommerfeld, Barbara, Wood-Siverio, Cathy, Portillo, Alicia, Price, T Ryan, Lenahan, Art, Williams, Karen, Guthrie, Stephanie, Rawlins, Ashlee, Harlan, Sherry, Hunter, Christine, Tran, Baochan, Darin, Abigail, Linder, Carly, Todd, Gretchen, Nicolas, Aude, Thomas, Cathi-Ann, James, Raymond, Deeley, Cheryl, Bishop, Courtney, Sprenger, Fabienne, Willeke, Diana, Obradov, Sanja, Mule, Jennifer, Monahan, Nancy, Gauss, Katharina, Keller, Margaux F, Comyns, Kathleen, Fontaine, Deborah, Gigliotti, Christina, McCoy, Arita, Dunlop, Becky, Shah, Bina, Ainscough, Susan, James, Angela, Silverstein, Rebecca, Espay, Kristy, Molony, Cliona, Ranola, Madelaine, Santana, Helen M, Ngono, Nelly, Rezola, Elisabet, Rolan, Delores Vilas, Waro, Bjorg, Mirlman, Anat, Stamelou, Maria, Comery, Thomas, Papapetropoulos, Spyros, Gibbs, J Raphael, Ravina, Bernard, Grachev, Igor D, Dubow, Jordan S, Ahlijanian, Michael, Soares, Holly, Ostrowizki, Suzanne, Fontoura, Paulo, Chalker, Alison, Hewitt, David L, van der Brug, Marcel, Chen-Plotkin, Alice, Reith, Alastair D, Taylor, Peggy, Egebjerg, Jan, Minton, Mark, Siderowf, Andrew, Muglia, Pierandrea, Umek, Robert, Catafau, Ana, Suh, Eunran, Rick, Jacqueline, Letson, Christopher, Fiandaca, Massimo S, Mapstone, Mark, Federoff, Howard J, Noyce, Alastair J, Morris, Huw, Van Deerlin, Vivianna M, Weintraub, Daniel, Zabetian, Cyrus, Hernandez, Dena G, Eberly, Shirley, Lesage, Suzanne, Mullins, Meghan, Conley, Emily Drabant, Northover, Carrie A M, Frasier, Mark, Marek, Ken, Day-Williams, Aaron G, Stone, David J, Ioannidis, John P A, Singleton, Andrew B, Hutten, Samantha J, investigators, Parkinson's Disease Biomarkers Program and Parkinson's Progression Marker Initiative, Bowman, Dubois, Dawson, Ted, Dewey, Richard, German, Dwight Charles, Huang, Xuemei, Petyuk, Vladislav, Scherzer, Clemens, Vaillancourt, David, Gwinn, Katrina, West, Andrew, Zhang, Jing, Marek, Kenneth, Jennings, Danna, Lasch, Shirley, Tanner, Caroline, Simuni, Tanya, Coffey, Christopher, Kieburtz, Karl, Wilson, Renee, Sutherland, Margaret, Poewe, Werner, Mollenhauer, Brit, Galasko, Douglas, Foroud, Tatiana, Sherer, Todd, Chowdhury, Sohini, Kopil, Catherine, Arnedo, Vanessa, Casaceli, Cynthia, Martinez, Maria, Seibyl, John, Mendick, Susan, Schuff, Norbert, Caspell, Chelsea, Uribe, Liz, Foster, Eric, Gloer, Katherine, Yankey, Jon, Toga, Arthur, Crawford, Karen, Heutink, Peter, Smith, Danielle Elise, Casalin, Paola, Malferrari, Giulia, Trojanowski, John, Shaw, Les, Singleton, Andrew, Halter, Cheryl, Russell, David, Factor, Stewart, Hogarth, Penelope, Williams, Nigel M, Standaert, David, Hauser, Robert, Jankovic, Joseph, Stern, Matthew, Chahine, Lama, Hu, Shu-Ching, Frank, Samuel, Trenkwalder, Claudia, Oertel, Wolfgang, and Richard, Irene

Subjects

Male, Aging, Parkinson's disease, Genome-wide association study, Disease, Neurodegenerative, Cohort Studies, genetics [Parkinson Disease], Models, 2.1 Biological and endogenous factors, Family history, Aetiology, education.field_of_study, screening and diagnosis, Parkinson's Disease, Aged, Disease Progression, Female, Humans, Middle Aged, Parkinson Disease, Prodromal Symptoms, Models, Statistical, Neurology (clinical), Statistical, Detection, Cohort, Neurological, Biomarker (medicine), diagnosis [Parkinson Disease], Cohort study, 4.2 Evaluation of markers and technologies, medicine.medical_specialty, Population, Clinical Sciences, Parkinson's Disease Biomarkers Program and Parkinson's Progression Marker Initiative investigators, Article, Clinical Research, Internal medicine, medicine, ddc:610, education, Neurology & Neurosurgery, business.industry, Prevention, Neurosciences, medicine.disease, Brain Disorders, 4.1 Discovery and preclinical testing of markers and technologies, Good Health and Well Being, Physical therapy, business

Abstract

Summary Background Accurate diagnosis and early detection of complex diseases, such as Parkinson's disease, has the potential to be of great benefit for researchers and clinical practice. We aimed to create a non-invasive, accurate classification model for the diagnosis of Parkinson's disease, which could serve as a basis for future disease prediction studies in longitudinal cohorts. Methods We developed a model for disease classification using data from the Parkinson's Progression Marker Initiative (PPMI) study for 367 patients with Parkinson's disease and phenotypically typical imaging data and 165 controls without neurological disease. Olfactory function, genetic risk, family history of Parkinson's disease, age, and gender were algorithmically selected by stepwise logistic regression as significant contributors to our classifying model. We then tested the model with data from 825 patients with Parkinson's disease and 261 controls from five independent cohorts with varying recruitment strategies and designs: the Parkinson's Disease Biomarkers Program (PDBP), the Parkinson's Associated Risk Study (PARS), 23andMe, the Longitudinal and Biomarker Study in PD (LABS-PD), and the Morris K Udall Parkinson's Disease Research Center of Excellence cohort (Penn-Udall). Additionally, we used our model to investigate patients who had imaging scans without evidence of dopaminergic deficit (SWEDD). Findings In the population from PPMI, our initial model correctly distinguished patients with Parkinson's disease from controls at an area under the curve (AUC) of 0·923 (95% CI 0·900–0·946) with high sensitivity (0·834, 95% CI 0·711–0·883) and specificity (0·903, 95% CI 0·824–0·946) at its optimum AUC threshold (0·655). All Hosmer-Lemeshow simulations suggested that when parsed into random subgroups, the subgroup data matched that of the overall cohort. External validation showed good classification of Parkinson's disease, with AUCs of 0·894 (95% CI 0·867–0·921) in the PDBP cohort, 0·998 (0·992–1·000) in PARS, 0·955 (no 95% CI available) in 23andMe, 0·929 (0·896–0·962) in LABS-PD, and 0·939 (0·891–0·986) in the Penn-Udall cohort. Four of 17 SWEDD participants who our model classified as having Parkinson's disease converted to Parkinson's disease within 1 year, whereas only one of 38 SWEDD participants who were not classified as having Parkinson's disease underwent conversion (test of proportions, p=0·003). Interpretation Our model provides a potential new approach to distinguish participants with Parkinson's disease from controls. If the model can also identify individuals with prodromal or preclinical Parkinson's disease in prospective cohorts, it could facilitate identification of biomarkers and interventions. Funding National Institute on Aging, National Institute of Neurological Disorders and Stroke, and the Michael J Fox Foundation.

Published

2015

50. Lysosomal Alterations in Peripheral Blood Mononuclear Cells of Parkinson's Disease Patients

Author

Papagiannakis, Nikolaos Xilouri, Maria Koros, Christos and Stamelou, Maria Antonelou, Roubina Maniati, Matina and Papadimitriou, Dimitra Moraitou, Marina Michelakakis, Helen and Stefanis, Leonidas

Abstract

Background: Reduced expression of lysosomal-associated membrane protein 2a and heatshock-cognate 70 proteins, involved in chaperone-mediated autophagy and of glucocerebrosidase, is reported in PD brains. The aim of this study was to identify systemic alterations in lysosomal-associated membrane protein 2a, heatshock cognate-70, and glucocerebrosidase levels/activity in peripheral blood mononuclear cells from PD patients. Methods: Protein/mRNA levels were assessed in PD patients from genetically undetermined background, alpha-synuclein (G209A/A53T), or glucocerebrosidase mutation carriers and age-/sex-matched controls. Results: Heatshock cognate 70 protein levels were reduced in all PD groups, whereas its mRNA levels were decreased only in the genetically undetermined group. Glucocerebrosidase protein levels were decreased only in the genetic PD groups, whereas increased mRNA levels and decreased activity were detected only in the glucocerebrosidase mutation group. Conclusions: Reduced heatshock cognate-70 levels are suggestive of an apparent systemic chaperone-mediated autophagy dysfunction irrespective of genetic background. Glucocerebrosidase activity may serve as a screening tool to identify glucocerebrosidase mutation carriers with PD. (C) 2015 International Parkinson and Movement Disorder Society

Published

2015