Your search keyword '"Wendy R. Galpern"' showing total 55 results

1. Cell-Mediated Delivery of Brain-Derived Neurotrophic Factor Enhances Dopamine Levels in an Mpp+ Rat Model of Substantia Nigra Degeneration

Author

Wendy R. Galpern, David M. Frim, Stephen B. Tatter, C. Anthony Altar, M. Flint Beal, and Ole Isacson

Subjects

Medicine

Abstract

Brain-derived neurotrophic factor (BDNF) promotes the survival of fetal mesencephalic dopaminergic cells and protects dopaminergic neurons against the toxicity of MPP+ in vitro. Supranigral implantation of fibroblasts genetically engineered to secrete BDNF attenuates the loss of substantia nigra pars compacta (SNc) dopaminergic neurons associated with striatal infusion of MPP+ in the adult rat. Using this MPP+ rat model of nigral degeneration, we evaluated the neurochemical effects of supranigral, cell-mediated delivery of BDNF on substantia nigra (SN) dopamine (DA) content and turnover. Genetically engineered BDNF-secreting fibroblasts (~12 ng BDNF/24 h) were implanted dorsal to the SN 7 days prior to striatal MPP+ administration. The present results demonstrate that BDNF-secreting fibroblasts, as compared to control fibroblasts, enhance SN DA levels ipsilateral as well as contralateral to the graft without altering DA turnover. This augmentation of DA levels suggests that local neurotrophic factor delivery by genetically engineered cells may provide a therapeutic strategy for preventing neuronal death or enhancing neuronal function in neurodegenerative diseases characterized by dopaminergic neuronal dysfunction, such as Parkinson's disease.

Published

1996

2. Association of Hippocampal Subfields, CSF Biomarkers, and Cognition in Patients With Parkinson Disease Without Dementia

Author

Walter Maetzler, Inga-Liepelt Scarfone, Andrea Pilotto, Wendy R. Galpern, Luc Van Nueten, Daniela Berg, Sara Becker, Oliver Granert, Giacomo Salvadore, Klaus Scheffler, Maarten Timmers, Johannes Streffer, and Benjamin Roeben

Subjects

Oncology, Male, physiopathology [Cognitive Dysfunction], cerebrospinal fluid [Amyloid beta-Peptides], Hippocampal formation, Neuropsychological Tests, Spatial memory, Hippocampus, etiology [Cognitive Dysfunction], 0302 clinical medicine, cerebrospinal fluid [Parkinson Disease], Activities of Daily Living, 030212 general & internal medicine, diagnostic imaging [Hippocampus], medicine.diagnostic_test, Subiculum, Neuropsychology, Cognition, Parkinson Disease, pathology [CA1 Region, Hippocampal], Middle Aged, diagnostic imaging [CA1 Region, Hippocampal], amyloid beta-protein (1-42), Magnetic Resonance Imaging, cerebrospinal fluid [Biomarkers], Female, physiopathology [Parkinson Disease], complications [Parkinson Disease], medicine.medical_specialty, MAPT protein, human, tau Proteins, 03 medical and health sciences, Text mining, Internal medicine, medicine, Dementia, Humans, Cognitive Dysfunction, ddc:610, cerebrospinal fluid [Peptide Fragments], CA1 Region, Hippocampal, Aged, Amyloid beta-Peptides, business.industry, Magnetic resonance imaging, medicine.disease, Peptide Fragments, pathology [Parkinson Disease], pathology [Hippocampus], nervous system, cerebrospinal fluid [tau Proteins], Neurology (clinical), Human medicine, business, 030217 neurology & neurosurgery, Biomarkers, Follow-Up Studies

Abstract

ObjectiveTo examine whether hippocampal volume loss is primarily associated with cognitive status or pathologic β-amyloid 1–42 (Aβ42) levels, this study compared hippocampal subfield volumes between patients with Parkinson disease (PD) with mild cognitive impairment (PD-MCI) and without cognitive impairment (PD-CN) and between patients with low and high Aβ42 levels, in addition exploring the relationship among hippocampal subfield volumes, CSF biomarkers (Aβ42, phosphorylated and total tau), neuropsychological tests, and activities of daily living.MethodsForty-five patients with PD without dementia underwent CSF analyses and MRI as well as comprehensive motor and neuropsychological examinations. Hippocampal segmentation was conducted using FreeSurfer image analysis suite 6.0. Regression models were used to compare hippocampal subfield volumes between groups, and partial correlations defined the association between variables while controlling for intracranial volume (ICV).ResultsLinear regressions revealed cognitive group as a statistically significant predictor of both the hippocampal–amygdaloid transition area (HATA; β = −0.23, 95% CI −0.44 to −0.02) and the cornu ammonis 1 region (CA1; β = −0.28, 95% confidence interval [CI] −0.56 to −0.02), independent of disease duration and ICV, with patients with PD-MCI showing significantly smaller volumes than PD-CN. In contrast, no subfields were predicted by Aβ42 levels. Smaller hippocampal volumes were associated with worse performance on memory, language, spatial working memory, and executive functioning tests. The subiculum was negatively correlated with total tau levels (r = −0.37, 95% CI −0.60 to −0.09).ConclusionCognitive status, but not CSF Aβ42, predicted hippocampal volumes, specifically the CA1 and HATA. Hippocampal subfields were associated with various cognitive domains, as well as with tau pathology.

Published

2021

3. Clinimetric testing of the comprehensive cervical dystonia rating scale

Author

Stewart A. Factor, Charles A. Adler, Ramon L. Rodriguez, Stephen G. Reich, Tracy Waliczek, Hyder A. Jinnah, William Severt, Joseph Jankovic, Ami Rosen, Susan H. Fox, Christopher G. Goetz, Glenn T. Stebbins, Joel S. Perlmutter, Richard L. Barbano, Mateusz Zurowski, Cynthia L. Comella, and Wendy R. Galpern

Subjects

Dystonia, medicine.medical_specialty, Construct validity, Spasmodic Torticollis, Focal dystonia, medicine.disease, Confirmatory factor analysis, 03 medical and health sciences, 0302 clinical medicine, Neurology, Cronbach's alpha, Rating scale, medicine, Physical therapy, 030212 general & internal medicine, Neurology (clinical), Cervical dystonia, Psychology, 030217 neurology & neurosurgery

Abstract

Introduction The aim of this study was to test the clinimetric properties of the Comprehensive Cervical Dystonia Rating Scale. This is a modular scale with modifications of the Toronto Western Spasmodic Torticollis Rating Scale (composed of three subscales assessing motor severity, disability, and pain) now referred to as the revised Toronto Western Spasmodic Torticollis Scale-2; a newly developed psychiatric screening instrument; and the Cervical Dystonia Impact Profile-58 as a quality of life measure. Methods Ten dystonia experts rated subjects with cervical dystonia using the comprehensive scale. Clinimetric techniques assessed each module of the scale for reliability, item correlation, and factor structure. Results There were 208 cervical dystonia patients (73% women; age, 59 ± 10 years; duration, 15 ± 12 years). Internal consistency of the motor severity subscale was acceptable (Cronbach's alpha = 0.57). Item to total correlations showed that elimination of items with low correlations (

Published

2016

4. Recent developments in dystonia

Author

Hyder A. Jinnah, Wendy R. Galpern, and Jan K. Teller

Subjects

Dystonia, medicine.medical_specialty, Extramural, business.industry, MEDLINE, medicine.disease, Article, Phenotype, Neurology, Dystonic Disorders, medicine, Humans, Neurology (clinical), Intensive care medicine, business, Neuroscience, Dystonic disorder

Abstract

The dystonias are a family of related disorders with many different clinical manifestations and causes. This review summarizes recent developments regarding these disorders, focusing mainly on advances with direct clinical relevance from the past 2 years.The dystonias are generally defined by their clinical characteristics, rather than by their underlying genetic or neuropathological defects. The many varied clinical manifestations and causes contribute to the fact that they are one of the most poorly recognized of all movement disorders. A series of recent publications has addressed these issues, offering a revised definition and more logical means for classifying the many subtypes. Our understanding of the genetic and neurobiological mechanisms responsible for different types of dystonias also has grown rapidly, creating new opportunities and challenges for diagnosis, and identifying increasing numbers of rare subtypes for which specific treatments are available.Recent advances in describing the clinical phenotypes and determining associated causes have pointed to the need for new strategies for diagnosis, classification, and treatment of the dystonias.

Published

2015

5. Secured web-based video repository for multicenter studies

Author

Korey Winslow, Ami Rosen, Ling Yan, Cynthia L. Comella, Christy L. Ludlow, Wendy R. Galpern, Matt Hicks, Hyder A. Jinnah, Laura J. Wright, and Joel S. Perlmutter

Subjects

File Transfer Protocol, Databases, Factual, Gigabyte, Video Recording, Article, World Wide Web, otorhinolaryngologic diseases, medicine, Humans, Multicenter Studies as Topic, Web application, Computer Security, Dystonia, Video recording, Internet, Random access memory, Transport Layer Security, business.industry, medicine.disease, nervous system diseases, Neurology, The Internet, Neurology (clinical), Geriatrics and Gerontology, business

Abstract

We developed a novel secured web-based dystonia video repository for the Dystonia Coalition, part of the Rare Disease Clinical Research network funded by the Office of Rare Diseases Research and the National Institute of Neurological Disorders and Stroke. A critical component of phenotypic data collection for all projects of the Dystonia Coalition includes a standardized video of each participant. We now describe our method for collecting, serving and securing these videos that is widely applicable to other studies.Each recruiting site uploads standardized videos to a centralized secured server for processing to permit website posting. The streaming technology used to view the videos from the website does not allow downloading of video files. With appropriate institutional review board approval and agreement with the hosting institution, users can search and view selected videos on the website using customizable, permissions-based access that maintains security yet facilitates research and quality control.This approach provides a convenient platform for researchers across institutions to evaluate and analyze shared video data. We have applied this methodology for quality control, confirmation of diagnoses, validation of rating scales, and implementation of new research projects.We believe our system can be a model for similar projects that require access to common video resources.

Published

2015

6. Management of impulse control disorders in Parkinson's disease: Controversies and future approaches

Author

Michael Samuel, Kallol Ray Chaudhuri, Melissa J. Nirenberg, Angelo Antonini, Richard G. Brown, Maria C. Rodriguez-Oroz, Wendy R. Galpern, Michael S. Okun, Anthony E. Lang, and Jonathan M. Brotchie

Subjects

Parkinson's disease, Psychotherapist, Deep brain stimulation, medicine.medical_treatment, Dopaminergic, Disease, medicine.disease, Dopamine agonist, Impulse control, Clinical trial, Cognitive behavioral therapy, Neurology, medicine, Neurology (clinical), Psychology, medicine.drug

Abstract

Impulse control disorders in Parkinson's disease are a group of impulsive behaviors most often associated with dopaminergic treatment. Presently, there is a lack of high quality evidence available to guide their management. This manuscript reviews current management strategies, before concentrating on the concept of dopamine agonist withdrawal syndrome and its implications for the management of impulse control disorders. Further, we focus on controversies, including the role of more recently available anti-parkinsonian drugs, and potential future approaches involving routes of drug delivery, nonpharmacological treatments (such as cognitive behavioral therapy and deep brain stimulation), and other as yet experimental strategies.

Published

2015

7. Prioritized research recommendations from the National Institute of Neurological Disorders and StrokeParkinson'sDisease 2014 conference

Author

Thomas J. Montine, Walter J. Koroshetz, Story C. Landis, Beth-Anne Sieber, Steven Finkbeiner, Kip A. Ludwig, Margaret Sutherland, John Dunlop, Katrina Gwinn, Christine L. Torborg, Hao Wang, Andrew Siderowf, Virginia M.-Y. Lee, Anna Taylor, Harry T. Orr, Wendy R. Galpern, and Randall J. Bateman

Subjects

medicine.medical_specialty, Parkinson's disease, Physical medicine and rehabilitation, Neurology, business.industry, medicine, MEDLINE, Physical therapy, Neurology (clinical), medicine.disease, business, Stroke

Published

2014

8. Recommendations of the Alzheimer's Disease-Related Dementias Conference

Author

Michael Hutton, Christine L. Torborg, Dennis W. Dickson, Debra Babcock, Margaret Sutherland, William W. Seeley, Andrey N. Kuzmichev, David S. Knopman, Creighton H. Phelps, Karen Marder, Wendy R. Galpern, Jennifer J. Manly, Roderick A. Corriveau, Thomas J. Montine, Bruce L. Miller, M. Maria Glymour, Steven M. Greenberg, Beth-Anne Sieber, Salina P. Waddy, Berislav V. Zlokovic, Nina Silverberg, and Walter J. Koroshetz

Subjects

Gerontology, medicine.medical_specialty, Views & Reviews, Lewy body, business.industry, Dementia with Lewy bodies, Research, Disease, medicine.disease, United States, Health equity, Alzheimer Disease, Health care, Humans, Medicine, Dementia, Neurology (clinical), Alzheimer's disease, business, Psychiatry, Frontotemporal dementia

Abstract

The National Alzheimer's Project Act, signed into law in 2011, mandates a National Plan to Address Alzheimer's Disease that is updated annually. In the Plan, the term Alzheimer disease includes not only Alzheimer disease (AD) proper, but also several specified related dementias, namely, frontotemporal, Lewy body, vascular, and mixed dementia. In response to a specific action item in the 2012 National Plan, the National Institute of Neurological Disorders and Stroke, in collaboration with the National Institute on Aging, convened panels of experts and conducted a 2-day public conference to develop research priorities and timelines for addressing Alzheimer disease–related dementias (ADRD) in 5 topic areas: multiple etiology dementias, health disparities, Lewy body dementias including dementia with Lewy bodies and Parkinson disease dementia, frontotemporal dementia and related tauopathies, and vascular contributions to ADRD. By design, the product was up to 8 prioritized research recommendations in each topic area including estimated timelines from when work on a recommendation is started to completion or to full implementation of an ongoing activity, and recognition of shared research themes across recommendations. These included increased education and training of both researchers and health care professionals, addressing health disparities, fundamental neurobiology research, advanced diagnostics, collaborative biosample repositories, and a focus on developing effective interventions to prevent or treat ADRD by the year 2025 as targeted by the National Plan.

Published

2014

9. The focal dystonias: Current views and challenges for future research

Author

Hyder A. Jinnah, Giovanni Defazio, Cynthia L. Comella, Mark Hallett, Ami Rosen, Christy L. Ludlow, Mahlon R. DeLong, Alfredo Berardelli, Wendy R. Galpern, Stewart A. Factor, and Joel S. Perlmutter

Subjects

Dystonia, Blepharospasm, Focal dystonia, medicine.disease, Developmental psychology, Important research, Neurology, medicine, Focal Dystonias, Neurology (clinical), medicine.symptom, Psychology, Focal Hand Dystonia, Dystonic disorder, Cognitive psychology

Abstract

The most common forms of dystonia are those that develop in adults and affect a relatively isolated region of the body. Although these adult-onset focal dystonias are most prevalent, knowledge of their etiologies and pathogenesis has lagged behind some of the rarer generalized dystonias, where the identification of genetic defects has facilitated both basic and clinical research. This summary provides a brief review of the clinical manifestations of the adult-onset focal dystonias, focussing attention on less well-understood clinical manifestations that need further study. It also provides a simple conceptual model for the similarities and differences among the different adult-onset focal dystonias, as a rationale for lumping them together as a class of disorders while at the same time splitting them into subtypes. The concluding section outlines some of the most important research questions for the future. Answers to these questions are critical for advancing our understanding of this group of disorders, and for developing novel therapeutics.

Published

2013

10. Development of the Comprehensive Cervical Dystonia Rating Scale: Methodology

Author

Tracy Waliczek, Laura Marsh, Ami Rosen, Glenn T. Stebbins, Joel S. Perlmutter, Mateusz Zurowski, Wendy R. Galpern, Hyder A. Jinnah, Laura J. Wright, Cynthia L. Comella, Kailash P. Bhatia, William M. McDonald, and Susan H. Fox

Subjects

Dystonia, medicine.medical_specialty, Modified delphi, Spasmodic Torticollis, Focal dystonia, medicine.disease, Article, Physical medicine and rehabilitation, Neurology, Quality of life, Rating scale, medicine, Physical therapy, Screening tool, Neurology (clinical), Cervical dystonia, Psychology

Abstract

We present the methodology utilized for development and clinimetric testing of the Comprehensive Cervical Dystonia (CD) Rating scale, or CCDRS. The CCDRS includes a revision of the Toronto Western Spasmodic Torticollis Rating Scale (TWSTRS-2), a newly developed psychiatric screening tool (TWSTRS-PSYCH), and the previously validated Cervical Dystonia Impact Profile (CDIP-58). For the revision of the TWSTRS, the original TWSTRS was examined by a committee of dystonia experts at a dystonia rating scales workshop organized by the Dystonia Medical Research Foundation. During this workshop, deficiencies in the standard TWSTRS were identified and recommendations for revision of the severity and pain subscales were incorporated into the TWSTRS-2. Given that no scale currently evaluates the psychiatric features of cervical dystonia (CD), we used a modified Delphi methodology and a reiterative process of item selection to develop the TWSTRS-PSYCH. We also included the CDIP-58 to capture the impact of CD on quality of life. The three scales (TWSTRS2, TWSTRS-PSYCH, and CDIP-58) were combined to construct the CCDRS. Clinimetric testing of reliability and validity of the CCDRS are described. The CCDRS was designed to be used in a modular fashion that can measure the full spectrum of CD. This scale will provide rigorous assessment for studies of natural history as well as novel symptom-based or disease-modifying therapies.

Published

2016

11. Knowledge gaps and research recommendations for essential tremor

Author

Glenn T. Stebbins, Gregor Kuhlenbäumer, Jerrold L. Vitek, Tatiana Foroud, Mark Hallett, Wendy R. Galpern, William G. Ondo, Claudia M. Testa, Charles H. Adler, Rick C. Helmich, Kailash P. Bhatia, Andrew B. Singleton, David E. Vaillancourt, Matthew P. Frosch, Roy V. Sillitoe, Ashlee Van't Veer, Elan D. Louis, Katrina Gwinn, Samantha L. White, Franziska Hopfner, Caroline M. Tanner, David Eidelberg, Günther Deuschl, Dietrich Haubenberger, Rodger J. Elble, Holly A. Shill, and Frederick A. Lenz

Subjects

0301 basic medicine, Biomedical Research, Essential Tremor, Neuropathology, Bioinformatics, Article, 03 medical and health sciences, 0302 clinical medicine, Medicine, Animals, Humans, Exome, Genetic association, Essential tremor, business.industry, medicine.disease, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Natural history, Clinical trial, 030104 developmental biology, Knowledge, Neurology, Etiology, Identification (biology), Neurology (clinical), Geriatrics and Gerontology, business, 030217 neurology & neurosurgery

Abstract

Item does not contain fulltext Essential tremor (ET) is a common cause of significant disability, but its etiologies and pathogenesis are poorly understood. Research has been hampered by the variable definition of ET and by non-standardized research approaches. The National Institute of Neurological Disorders and Stroke (USA) invited experts in ET and related fields to discuss current knowledge, controversies, and gaps in our understanding of ET and to develop recommendations for future research. Discussion focused on phenomenology and phenotypes, therapies and clinical trials, pathophysiology, pathology, and genetics. Across all areas, the need for collaborative and coordinated research on a multinational level was expressed. Standardized data collection using common data elements for genetic, clinical, neurophysiological, and pathological studies was recommended. Large cohorts of patients should be studied prospectively to collect bio-samples, characterize the natural history of the clinical syndrome including patient-oriented outcomes, investigate potential etiologies of various phenotypes, and identify pathophysiological mechanisms. In particular, cellular and system-level mechanisms of tremor oscillations should be elucidated because they may yield effective therapeutic targets and biomarkers. A neuropathology consortium was recommended to standardize postmortem analysis and further characterize neuropathological observations in the cerebellum and elsewhere. Furthermore, genome-wide association studies on large patient cohorts (>10,000 patients) may allow the identification of common genes contributing to risk, and whole exome or genome sequencing may enable the identification of genetic risk and causal mutations in cohorts and well-characterized families.

Published

2016

12. Dopamine transporter imaging is associated with long-term outcomes in Parkinson's disease

Author

Michael A. Schwarzschild, Alberto Ascherio, Caroline M. Tanner, Kenneth Marek, Shirley Eberly, Roger Kurlan, Jennifer Harman, David Oakes, Emily Flagg, Anthony E. Lang, Ira Shoulson, Bernard Ravina, Wendy R. Galpern, James C. Beck, and Flint Beal

Subjects

Psychosis, medicine.medical_specialty, Parkinson's disease, biology, Parkinsonism, Montreal Cognitive Assessment, Odds ratio, medicine.disease, Neurology, Quartile, Internal medicine, Cohort, medicine, biology.protein, Neurology (clinical), Psychology, Psychiatry, Dopamine transporter

Abstract

Dopamine (DA) transporter (DAT) imaging has been studied as a diagnostic tool for degenerative parkinsonism. Our aim was to measure the prognostic value of imaging for motor and nonmotor outcomes in Parkinson's disease (PD). We prospectively evaluated a Parkinson's cohort after enrollment in a de novo clinical trial with a battery of motor (UPDRS), cognitive (Montreal Cognitive Assessment), and behavioral measures. DAT imaging with [123I][β]-CIT and single-photon emission computerized tomography (SPECT) was performed at baseline and after 22 months. In total, 491 (91%) of the 537 subjects had evidence of DA deficiency on their baseline scan, consistent with PD, and were included in the analyses. The cohort was followed for 5.5 (0.8) years, with a mean duration of diagnosis of 6.3 (1.2). Lower striatal binding at baseline was independently associated with higher risk for clinical milestones and measures of disease severity, including motor-related disability, falling and postural instability, cognitive impairment, psychosis, and clinically important depressive symptoms. Subjects in the bottom quartile for striatal binding, compared to the top quartile, had an odds ratio (95% confidence interval) of 3.3 (1.7, 6.7) for cognitive impairment and 12.9 (2.6, 62.4) for psychosis. Change from baseline in imaging after 22 months was also independently associated with motor, cognitive, and behavioral outcomes. DAT imaging with [123I][β]-CIT and SPECT, shortly after the diagnosis of PD, was independently associated with clinically important long-term motor and nonmotor outcomes. These results should be treated as hypothesis generating and require confirmation. © 2012 Movement Disorder Society

Published

2012

13. Predictors of cognitive outcomes in early Parkinson disease patients: The National Institutes of Health Exploratory Trials in Parkinson Disease (NET-PD) experience

Author

Jay S. Schneider, Jordan J. Elm, Bernard Ravina, Sotirios A. Parashos, and Wendy R. Galpern

Subjects

Male, Research design, Repeatable Battery for the Assessment of Neuropsychological Status, medicine.medical_specialty, Parkinson's disease, Population, MEDLINE, Disease, Neuropsychological Tests, Article, Antiparkinson Agents, Cognition, Outcome Assessment, Health Care, medicine, Humans, Multicenter Studies as Topic, education, Randomized Controlled Trials as Topic, education.field_of_study, Parkinson Disease, Middle Aged, medicine.disease, United States, National Institutes of Health (U.S.), Neurology, Research Design, Cohort, Physical therapy, Female, Neurology (clinical), Geriatrics and Gerontology, Cognition Disorders, Psychology, Clinical psychology

Abstract

Cognitive dysfunction is an important aspect of Parkinson disease (PD) and is increasingly being examined in various large scale PD clinical studies. However, the sensitivity of some of the cognitive measures used for detecting change in cognitive status in early PD patients is not known nor is the relationship between cognitive outcome measures and other motor and non-motor disease characteristics and various demographic parameters in early PD patients. The current analysis of the NET-PD cohort (i.e., untreated patients) was undertaken to: 1) assess which (if any) baseline demographic parameters correlate with baseline cognitive measures and any potential change in cognitive measures over the 12-18 months evaluation period; 2) assess the extent to which cognitive measures employed (i.e., Repeatable Battery for the Assessment of Neuropsychological Status (RBANS), Frontal Assessment Battery (FAB) and Letter-Number Sequencing) are sensitive to change over time; 3) examine whether initiation of symptomatic therapy is associated with change in cognitive status. At baseline, NET-PD subjects had no significant impairment on the assessments employed. Only education and age were significant predictors of cognitive score at baseline. None of the summary measures were indicative of change in cognitive status over the 12-18 months of study. These results suggest either the cognitive domains examined are not affected in the population examined or that more sensitive measures of cognition than those currently employed may need to be considered for use in a large trial setting in which an early, highly educated PD population is studied.

Published

2010

14. A longitudinal program for biomarker development in Parkinson's disease: A feasibility study

Author

Bernard, Ravina, Caroline, Tanner, Diane, Dieuliis, Shirley, Eberly, Emily, Flagg, Wendy R, Galpern, Stanley, Fahn, Christopher G, Goetz, Stephen, Grate, Roger, Kurlan, Anthony E, Lang, Kenneth, Marek, Karl, Kieburtz, David, Oakes, Robin, Elliott, Ira, Shoulson, and Cindy, Casaceli

Subjects

Male, Oncology, medicine.medical_specialty, Pathology, Parkinson's disease, Movement, Disease, Cohort Studies, Internal medicine, Humans, Medicine, Longitudinal Studies, Aged, Clinical Trials as Topic, business.industry, Patient Selection, Parkinson Disease, DNA, Middle Aged, medicine.disease, Clinical trial, Neurology, Data Interpretation, Statistical, Cohort, Feasibility Studies, Biomarker (medicine), Female, Observational study, Neurology (clinical), Sample collection, business, Biomarkers, Follow-Up Studies, Cohort study

Abstract

Long-term follow up is necessary to understand the natural history of treated Parkinson's disease (PD). The Longitudinal and Biomarker Study in PD (LABS-PD) is an observational study designed to prospectively measure the evolution of motor and non-motor features of PD and sample promising biomarkers from early to late stage illness. LABS-PD is organized on the premise that cohorts from completed clinical trials can be re-recruited for long-term follow up. LABS-PD will eventually contain multiple cohorts, but to test the feasibility of the strategy, we examined enrollment and biomarker sampling in the initial cohorts. The first PD cohort (PostCEPT) comes from the de novo clinical trial of a mixed lineage kinase inhibitor (PRECEPT). We assessed the recruitment from PRECEPT to PostCEPT, the ability to link data from the two studies, and sample collection for a variety of biomarkers. A total of 537 of 709 eligible PRECEPT subjects (76%) enrolled in PostCEPT; 509 (95%) had repeat dopamine transporter imaging. PRECEPT clinical and imaging data were successfully linked to PostCEPT, to provide 3 to 4 year follow-up. A biomarker sub-study enrolled over 100 PD cases from PostCEPT and 100 controls to measure olfaction and blood markers of gene expression, alpha-synuclein, and proteomic profiles. We were also successful in linking clinical and biomarker data to DNA samples that have been collected in the publicly accessible Coriell repository. The PostCEPT cohort and associated studies strongly support the feasibility of the LABS-PD approach of retaining and repurposing clinical trial cohorts to collect longitudinal clinical and biomarker data.

Published

2009

15. Management of impulse control disorders in Parkinson’s disease

Author

Mark Stacy and Wendy R. Galpern

Subjects

medicine.medical_specialty, Neurology, Deep brain stimulation, Parkinson's disease, business.industry, medicine.medical_treatment, Psychological intervention, medicine.disease, Discontinuation, law.invention, Randomized controlled trial, law, Punding, medicine, Hypersexuality, Neurology (clinical), medicine.symptom, Intensive care medicine, business

Abstract

Impulse control disorders (ICDs) are a set of behaviors, including pathologic gambling, hypersexuality, compulsive shopping, compulsive eating, and punding, which are now recognized to occur in a subset of patients with Parkinson's disease (PD). Although the underlying pathophysiology of these behaviors is poorly understood, they appear to be associated with the use, and sometimes overuse, of dopaminergic agents prescribed for the treatment of the motor symptoms of PD. At present, there are limited data to support any particular therapeutic strategy. Approaches worth considering in the management of the PD patient with an ICD include reduction or discontinuation of dopamine agonist therapy, trials of various pharmacologic agents, psychosocial interventions, and deep brain stimulation of the subthalamic nucleus. However, the management of each patient must be tailored for the particular clinical setting, and the development of evidence-based treatment strategies awaits future prospective studies and randomized controlled trials.

Published

2007

16. A randomized clinical trial of coenzyme Q10 and GPI-1485 in early Parkinson disease

Author

Margaret Marie Cox, Stephanie Sendek, Margaret F. Turk, Julie H. Carter, Susan C. Fagan, Lorelei Derwent, Oksana Suchowersky, Jay S. Schneider, Linda Paul, Gwyn Vernon, Stephen Gollomp, Karl Kieburtz, Debbie Baker, I. Van Bodis-Wollner, Germaine McInnes, Marian A. Perez, G. Webster Ross, Katharine Pabst, Jorge L. Juncos, Chad W. Christine, Jessie Roth, Joseph M. Savitt, Peter A LeWitt, Hubert H. Fernandez, Matthew Brodsky, Mark F. Lew, Jay M. Gorell, Natividad R. Stover, Paulo Guimaraes, Andrew Feigin, Anita Blenke, Martha Nance, Elizabeth Hayes, Andrew Siderowf, W.R. Wayne Martin, Tammie Kelsey, Susan Bennett, Sharon McCarthy, Charles H. Adler, Beverly Olsen, Pauline LeBlanc, Richard B. Dewey, Rodger J. Elble, Richard S. Burns, Carlos Singer, Amy Parsons, John W. Taylor, Tracy Stewart, Maryan DeAngelis, Barbara C. Tilley, William J. Weiner, Brad A. Racette, Wendy R. Galpern, Michael J. Aminoff, Kapil D. Sethi, Jayaraman Rao, Robert A. Hauser, Debbie Fraser, Connie Kawai, David Coffey, Kelly E. Lyons, Kristine Wernette, Becky Dunlop, Holly Delgado, Marlene Lind, Rajesh Pahwa, Chris Weaver, Ray L. Watts, Patricia Deppen, Ryan J. Uitti, Marwan N. Sabbagh, Lynn Marlor, Joann Belden, Burton L. Scott, Theresa McClain, Roger L. Albin, John Y. Fang, Zoran Obradov, Yuko Y. Palesch, Maureen Cook, Pamela Andrews, Jeana Jaglin, Joanne Wojcieszek, Mary Louise Musante Weeks, Susan Peterson, James H. Bower, Maureen A. Leehey, Joanne Field, Lisa M. Shulman, Caroline M. Tanner, Jacob I. Sage, Jordan J. Elm, Joseph Jankovic, Patrick D. Mauldin, Aileen Shinaman, Peng Huang, G. Frederick Wooten, Alicia Brocht, Gordon H. Brown, Peggy Roberge, Dorothy Shearon, Buff Dill, Margaret F. Keller, Charlene Young, Christine Hunter, Janis M. Miyasaki, Susan Torgrimson, Cornelia Kamp, Brigid Hayward, Christopher G. Goetz, Emily Kosa, Marilyn Flewellen, David Simon, Rebecca McMurray, Sue Reichwein, Jacci Bainbridge, Robert W. Hamill, Stephanie Terashita, Kathleen M. Shannon, Frederick Wooten, Danna Jennings, Shana Krstevska, and Bernard Ravina

Subjects

Male, medicine.medical_specialty, Future studies, Neurology, Ubiquinone, Coenzymes, Disease, Placebo, Tacrolimus, law.invention, chemistry.chemical_compound, Double-Blind Method, Randomized controlled trial, law, Rating scale, Internal medicine, Humans, Medicine, Aged, Coenzyme Q10, business.industry, Headache, Nausea, Parkinson Disease, Middle Aged, Clinical trial, chemistry, Physical therapy, Female, Neurology (clinical), business

Abstract

Objective: To determine if future studies of coenzyme Q10 and GPI-1485 in Parkinson disease (PD) may be warranted. Methods: We conducted a randomized, double-blind, calibrated futility clinical trial of coenzyme Q10 and GPI-1485 in early untreated PD using placebo data from the DATATOP study to establish the futility threshold. Results: The primary outcome measure (change in total Unified Parkinson's Disease Rating Scale scores over 1 year) did not meet the prespecified criteria for futility for either agent. Secondary analyses using calibration controls and other more recent placebo data question the appropriateness of the predetermined definition of futility, and suggest that a more restrictive threshold may be needed. Conclusions: Coenzyme Q10 and GPI-1485 may warrant further study in Parkinson disease, although the data are inconsistent. Additional factors (cost, availability of other agents, more recent data on placebo outcomes, other ongoing trials) should also be considered in the selection of agents for Phase III studies. NEUROLOGY 2007;68:20-28

Published

2007

17. Clinimetric testing of the comprehensive cervical dystonia rating scale

Author

Cynthia L, Comella, Joel S, Perlmutter, Hyder A, Jinnah, Tracy A, Waliczek, Ami R, Rosen, Wendy R, Galpern, Charles A, Adler, Richard L, Barbano, Stewart A, Factor, Christopher G, Goetz, Joseph, Jankovic, Stephen G, Reich, Ramon L, Rodriguez, William L, Severt, Mateusz, Zurowski, Susan H, Fox, and Glenn T, Stebbins

Subjects

Male, Neurologic Examination, Humans, Reproducibility of Results, Female, Middle Aged, Severity of Illness Index, Torticollis, Article, Aged

Abstract

The aim of this study was to test the clinimetric properties of the Comprehensive Cervical Dystonia Rating Scale. This is a modular scale with modifications of the Toronto Western Spasmodic Torticollis Rating Scale (composed of three subscales assessing motor severity, disability, and pain) now referred to as the revised Toronto Western Spasmodic Torticollis Scale-2; a newly developed psychiatric screening instrument; and the Cervical Dystonia Impact Profile-58 as a quality of life measure.Ten dystonia experts rated subjects with cervical dystonia using the comprehensive scale. Clinimetric techniques assessed each module of the scale for reliability, item correlation, and factor structure.There were 208 cervical dystonia patients (73% women; age, 59 ± 10 years; duration, 15 ± 12 years). Internal consistency of the motor severity subscale was acceptable (Cronbach's alpha = 0.57). Item to total correlations showed that elimination of items with low correlations (0.20) increased alpha to 0.71. Internal consistency estimates for the subscales for disability and pain were 0.88 and 0.95, respectively. The psychiatric screening scale had a Cronbach's alpha of 0.84 and satisfactory item to total correlations. When the subscales of the Toronto Western Spasmodic Torticollis Scale-2 were combined with the psychiatric screening scale, Cronbach's alpha was 0.88, and construct validity assessment demonstrated four rational factors: motor; disability; pain; and psychiatric disorders. The Cervical Dystonia Impact Profile-58 had an alpha of 0.98 and its construction was validated through a confirmatory factor analysis.The modules of the Comprehensive Cervical Dystonia Rating Scale are internally consistent with a logical factor structure.

Published

2015

18. Erratum to: Commonalities and Challenges in the Development of Clinical Trial Measures in Neurology

Author

Jesse M. Cedarbaum, David Cella, Maria C. Carrillo, Jill Heemskerk, Marc K. Walton, Maria Isaac, Diane Stephenson, Richard A. Rudick, Douglas A. Kerr, Glenn T. Stebbins, Petra Kaufmann, and Wendy R. Galpern

Subjects

Pharmacology, Medical education, medicine.medical_specialty, Clinical Trials as Topic, Neurology, business.industry, Clinical trial, Outcome Assessment, Health Care, medicine, Humans, Pharmacology (medical), Neurology (clinical), Erratum, business

Abstract

As neurologists and neuroscientists, we are trained to evaluate disorders of the nervous system by thinking systematically. Clinically, we think in terms of cognition, behavior, motor function, sensation, balance and co-ordination, and autonomic system function. But when we assess symptoms of neurological disorders for the purpose of drug development, we tend to create disease-specific outcome measures, often using a variety of methods to assess the same types of dysfunction in overlapping, related disorders. To begin to explore the potential to simplify and harmonize the assessment of dysfunction across neurological disorders, a symposium, entitled, "Commonalities in the Development of Outcome Measures in Neurology" was held at the 16th annual meeting of the American Society for Experimental NeuroTherapeutics (ASENT), in February 2014. This paper summarizes the presentations at the symposium. The authors hope that readers will begin to view Clinical Outcome Assessment (COA) development in a new light. We hope that in presenting this material, we will stimulate discussions and collaborations across disease areas to develop common concepts of neurological COA development and construction.

Published

2015

19. Interface between tauopathies and synucleinopathies: A tale of two proteins

Author

Anthony E. Lang and Wendy R. Galpern

Subjects

Brain Chemistry, Synucleinopathies, Dementia with Lewy bodies, Parkinsonism, Synucleins, Neurodegenerative Diseases, tau Proteins, Disease, Biology, medicine.disease, LRRK2, nervous system diseases, Neurology, mental disorders, medicine, Synuclein, Animals, Humans, Dementia, Neurology (clinical), Tauopathy, Neuroscience

Abstract

Neurodegenerative diseases are often classified based on the abnormal accumulation of synuclein or tau. Traditionally, these disorders have been viewed as distinct clinical and pathological entities. However, advances in molecular genetics and protein biochemistry have shown intriguing overlaps. The most common synucleinopathy, Parkinson's disease, is characterized by extrapyramidal motor dysfunction, whereas the most common tauopathy, Alzheimer's disease, is defined by dementia. Yet there is overlap of clinical features; Parkinson's disease patients frequently have dementia, and Alzheimer's disease patients often manifest parkinsonism. Dementia with Lewy bodies exemplifies the existence of a continuum among these diseases. This overlap extends to the neuropathological findings; the pathognomonic hallmark for one set of disorders, Lewy bodies or neurofibrillary tangles, is present more often than expected in the other set. Moreover, mutations in LRRK2 known to cause parkinsonism are associated not only with dopaminergic neuronal degeneration, but also with the accumulation of synuclein, tau, neither, or both proteins. Other shared genetic features between tauopathies and synucleinopathies also exist. Finally, the known protein interactions between tau and synuclein further highlight the interface. Evidence for the intersection of tauopathies and synucleinopathies indicates the need for an updated disease classification scheme and may have important implications for therapeutic development.

Published

2006

20. Clinical trials for multiple system atrophy

Author

Wendy R. Galpern

Subjects

Male, medicine.medical_specialty, business.industry, MEDLINE, Multiple System Atrophy, medicine.disease, Clinical trial, Atrophy, Neuroprotective Agents, Parkinsonian Disorders, Internal medicine, Indans, Medicine, Humans, Female, Neurology (clinical), business

Published

2014

21. Commonalities and Challenges in the Development of Clinical Trial Measures in Neurology

Author

Maria Isaac, David Cella, Petra Kaufmann, Maria C. Carrillo, Richard A. Rudick, Wendy R. Galpern, Marc K. Walton, Douglas A. Kerr, Glenn T. Stebbins, Diane Stephenson, Jill Heemskerk, and Jesse M. Cedarbaum

Subjects

Pharmacology, medicine.medical_specialty, Neurology, media_common.quotation_subject, Alternative medicine, Cognition, Disease, Variety (cybernetics), Clinical trial, Drug development, medicine, Pharmacology (medical), Original Article, Neurology (clinical), Function (engineering), Psychology, Psychiatry, Clinical psychology, media_common

Abstract

As neurologists and neuroscientists, we are trained to evaluate disorders of the nervous system by thinking systematically. Clinically, we think in terms of cognition, behavior, motor function, sensation, balance and co-ordination, and autonomic system function. But when we assess symptoms of neurological disorders for the purpose of drug development, we tend to create disease-specific outcome measures, often using a variety of methods to assess the same types of dysfunction in overlapping, related disorders. To begin to explore the potential to simplify and harmonize the assessment of dysfunction across neurological disorders, a symposium, entitled, "Commonalities in the Development of Outcome Measures in Neurology" was held at the 16th annual meeting of the American Society for Experimental NeuroTherapeutics (ASENT), in February 2014. This paper summarizes the presentations at the symposium. The authors hope that readers will begin to view Clinical Outcome Assessment (COA) development in a new light. We hope that in presenting this material, we will stimulate discussions and collaborations across disease areas to develop common concepts of neurological COA development and construction.

Published

2014

22. Prioritized research recommendations from the National Institute of Neurological Disorders and Stroke Parkinson's Disease 2014 conference

Author

Beth-Anne, Sieber, Story, Landis, Walter, Koroshetz, Randall, Bateman, Andrew, Siderowf, Wendy R, Galpern, John, Dunlop, Steven, Finkbeiner, Margaret, Sutherland, Hao, Wang, Virginia M-Y, Lee, Harry T, Orr, Katrina, Gwinn, Kip, Ludwig, Anna, Taylor, Christine, Torborg, and Thomas J, Montine

Subjects

Biomedical Research, Humans, National Institute of Neurological Disorders and Stroke (U.S.), United States, Article

Published

2014

23. Management of impulse control disorders in Parkinson's disease: Controversies and future approaches

Author

Michael, Samuel, Maria, Rodriguez-Oroz, Angelo, Antonini, Jonathan M, Brotchie, Kallol, Ray Chaudhuri, Richard G, Brown, Wendy R, Galpern, Melissa J, Nirenberg, Michael S, Okun, and Anthony E, Lang

Subjects

Antiparkinson Agents, Disruptive, Impulse Control, and Conduct Disorders, Deep Brain Stimulation, Dopamine Agonists, Impulsive Behavior, Animals, Humans, Parkinson Disease, Article

Abstract

Impulse control disorders in Parkinson's disease are a group of impulsive behaviors most often associated with dopaminergic treatment. Presently, there is a lack of high quality evidence available to guide their management. This manuscript reviews current management strategies, before concentrating on the concept of dopamine agonist withdrawal syndrome and its implications for the management of impulse control disorders. Further, we focus on controversies, including the role of more recently available anti-parkinsonian drugs, and potential future approaches involving routes of drug delivery, nonpharmacological treatments (such as cognitive behavioral therapy and deep brain stimulation), and other as yet experimental strategies.

Published

2014

24. Efficacy and safety of rifampicin for multiple system atrophy: a randomised, double-blind, placebo-controlled trial

Author

Jay Mandrekar, Steven Vernino, David Robertson, Susan Perlman, William P. Cheshire, Roy Freeman, Thomas C. Chelimsky, Stephanie Lessig, Robert A. Hauser, Wendy R. Galpern, Phillip A. Low, Italo Biaggioni, Horacio Kaufmann, Wolfgang Singer, Sid Gilman, and William D. Dupont

Subjects

Male, medicine.medical_specialty, Placebo-controlled study, Placebo, Article, law.invention, Cohort Studies, Atrophy, Randomized controlled trial, Double-Blind Method, law, Internal medicine, medicine, Clinical endpoint, Humans, Aged, Nucleic Acid Synthesis Inhibitors, business.industry, Middle Aged, Multiple System Atrophy, medicine.disease, Interim analysis, Surgery, Treatment Outcome, Female, Neurology (clinical), Rifampin, business, Rifampicin, medicine.drug, Cohort study, Follow-Up Studies

Abstract

Summary Background No available treatments slow or halt progression of multiple system atrophy, which is a rare, progressive, fatal neurological disorder. In a mouse model of multiple system atrophy, rifampicin inhibited formation of α-synuclein fibrils, the neuropathological hallmark of the disease. We aimed to assess the safety and efficacy of rifampicin in patients with multiple system atrophy. Methods In this randomised, double-blind, placebo-controlled trial we recruited participants aged 30–80 years with possible or probable multiple system atrophy from ten US medical centres. Eligible participants were randomly assigned (1:1) via computer-generated permuted block randomisation to rifampicin 300 mg twice daily or matching placebo (50 mg riboflavin capsules), stratified by subtype (parkinsonian vs cerebellar), with a block size of four. The primary outcome was rate of change (slope analysis) from baseline to 12 months in Unified Multiple System Atrophy Rating Scale (UMSARS) I score, analysed in all participants with at least one post-baseline measurement. This study is registered with ClinicalTrials.gov, number NCT01287221. Findings Between April 22, 2011, and April 19, 2012, we randomly assigned 100 participants (50 to rifampicin and 50 to placebo). Four participants in the rifampicin group and five in the placebo group withdrew from study prematurely. Results of the preplanned interim analysis (n=15 in each group) of the primary endpoint showed that futility criteria had been met, and the trial was stopped (the mean rate of change [slope analysis] of UMSARS I score was 0·62 points [SD 0·85] per month in the rifampicin group vs 0·47 points [0·48] per month in the placebo group; futility p=0·032; efficacy p=0·76). At the time of study termination, 49 participants in the rifampicin group and 50 in the placebo group had follow-up data and were included in the final analysis. The primary endpoint was 0·5 points (SD 0·7) per month for rifampicin and 0·5 points (0·5) per month for placebo (difference 0·0, 95% CI −0·24 to 0·24; p=0·82). Three (6%) of 50 participants in the rifampicin group and 12 (24%) of 50 in the placebo group had one or more serious adverse events; none was thought to be related to treatment. Interpretation Our results show that rifampicin does not slow or halt progression of multiple system atrophy. Despite the negative result, the trial does provide information that could be useful in the design of future studies assessing potential disease modifying therapies in patients with multiple system atrophy. Funding National Institutes of Health, Mayo Clinic Center for Translational Science Activities, and Mayo Funds.

Published

2014

25. In vivo PET Imaging in rat of dopamine terminals reveals functional neural transplants

Author

Anna-Liisa Brownell, Wendy R. Galpern, Ole Isacson, and Eli Livni

Subjects

medicine.medical_specialty, Dopamine, Striatum, Biology, Rats, Sprague-Dawley, Central nervous system disease, Midbrain, Fetal Tissue Transplantation, Mesencephalon, In vivo, Internal medicine, medicine, Animals, Parkinson Disease, Secondary, Nerve Endings, medicine.diagnostic_test, Dopaminergic, medicine.disease, Corpus Striatum, Rats, Transplantation, Endocrinology, Neurology, Positron emission tomography, Female, Neurology (clinical), Neuroscience, Tomography, Emission-Computed, medicine.drug

Abstract

Positron emission tomography (PET) and carbon-11-labeled 2B-carbomethoxy-3B-(4-fluorophenyl)tropane (11C-CFT or 11-WIN 35,428) were used as molecular markers for striatal presynaptic dopamine (DA) transporters in a unilateral Parkinson's disease rat neurotransplantation model. In the lesioned striatum, the binding ratio measured by the DA presynaptic marker was reduced to 15% to 35% of the intact side (or unoperated control). After grafting with non-DA cells (from dorsal mesencephalon), the DA binding ratio remained reduced to levels observed before transplantation and rats showed no behavioral recovery. In contrast, after DA neuronal transplantation, behavioral recovery occurred only after the 11C-CFT binding ratio had increased to 75% to 85% of the intact side. This study provides direct in vivo evidence for the dopaminergic molecular basis of functional recovery in the lesioned nigrostriatal system after neural transplantation.

Published

1998

26. Designing Clinical Trials for Dystonia

Author

Stanley Fahn, Karl Kieburtz, John L.P. Thompson, Christopher S. Coffey, Alberto Albanese, Dixie Ecklund, Hyder A. Jinnah, Jeremy M. Shefner, Sharon D. Yeatts, Joseph Jankovic, Cynthia L. Comella, Jan K. Teller, Wendy R. Galpern, Ken Cheung, Anthony E. Lang, and Michael P. McDermott

Subjects

Pharmacology, Research design, Dystonia, medicine.medical_specialty, Clinical Trials as Topic, business.industry, Clinical study design, Alternative medicine, MEDLINE, Review, medicine.disease, Clinical trial, Tolerability, Research Design, Health care, Outcome Assessment, Health Care, Medicine, Humans, Pharmacology (medical), Neurology (clinical), business, Intensive care medicine, Clinical psychology

Abstract

With advances in the understanding of the pathophysiology of dystonia, novel therapeutics are being developed. Such therapies will require clinical investigation ranging from exploratory studies to examine safety, tolerability, dosage selection, and preliminary efficacy to confirmatory studies to evaluate efficacy definitively. As dystonia is a rare and complex disorder with clinical and etiological heterogeneity, clinical trials will require careful consideration of the trial design, including enrollment criteria, concomitant medication use, and outcome measures. Given the complexities of designing and implementing efficient clinical trials, it is important for clinicians and statisticians to collaborate closely throughout the clinical development process and that each has a basic understanding of both the clinical and statistical issues that must be addressed. To facilitate designing appropriate clinical trials in this field, we review important general clinical trial and regulatory principles, and discuss the critical components of trials with an emphasis on considerations specific to dystonia. Additionally, we discuss designs used in early exploratory, late exploratory, and confirmatory phases, including adaptive designs.

Published

2013

27. The focal dystonias: current views and challenges for future research

Author

H A, Jinnah, Alfredo, Berardelli, Cynthia, Comella, Giovanni, Defazio, Mahlon R, Delong, Stewart, Factor, Wendy R, Galpern, Mark, Hallett, Christy L, Ludlow, Joel S, Perlmutter, and Ami R, Rosen

Subjects

Biomedical Research, Dystonic Disorders, Humans, Article

Abstract

The most common forms of dystonia are those that develop in adults and affect a relatively isolated region of the body. Although these adult-onset focal dystonias are most prevalent, knowledge of their etiologies and pathogenesis has lagged behind some of the rarer generalized dystonias, where the identification of genetic defects has facilitated both basic and clinical research. This summary provides a brief review of the clinical manifestations of the adult-onset focal dystonias, focussing attention on less well-understood clinical manifestations that need further study. It also provides a simple conceptual model for the similarities and differences among the different adult-onset focal dystonias, as a rationale for lumping them together as a class of disorders while at the same time splitting them into subtypes. The concluding section outlines some of the most important research questions for the future. Answers to these questions are critical for advancing our understanding of this group of disorders, and for developing novel therapeutics.

Published

2013

28. Xenotransplantation of Porcine Fetal Ventral Mesencephalon in a Rat Model of Parkinson's Disease: Functional Recovery and Graft Morphology

Author

Terrence W. Deacon, Lindsay H. Burns, Jonathan Dinsmore, Ole Isacson, and Wendy R. Galpern

Subjects

Pathology, medicine.medical_specialty, Time Factors, Swine, Xenotransplantation, medicine.medical_treatment, Transplantation, Heterologous, Striatum, In situ hybridization, Biology, Rats, Sprague-Dawley, Developmental Neuroscience, Mesencephalon, Dopamine, medicine, Animals, Brain Tissue Transplantation, Human Fetal Tissue, Dopaminergic, Parkinson Disease, Rats, Transplantation, Disease Models, Animal, nervous system, Neurology, Cyclosporine, Female, Neuroscience, Immunostaining, medicine.drug

Abstract

Neurotransplantation of human fetal dopamine (DA) neurons is currently being investigated as a therapeutic modality for Parkinson's disease (PD). However, the practical limitations of human fetal transplantation indicate a need for alternative methodologies. Using the 6-hydroxydopamine rat model of PD, we transplanted dopaminergic neurons derived from Embryonic Day 27 porcine fetuses into the denervated striatum of cyclosporine-A (CyA)-treated or non-CyA-treated rats. Functional recovery was assessed by amphetamine-induced rotation, and graft survival and morphology were analyzed using neuronal and glial immunostaining as well as in situ hybridization with a porcine repeat element DNA probe. A significant, sustained reduction in amphetamine-induced rotational asymmetry was present in the CyA-treated rats whereas the non-CyA-treated rats showed a transient behavioral recovery. The degree of rotational recovery was highly correlated to the number of surviving transplanted porcine dopaminergic neurons. TH+ neuronal survival and graft volume were significantly greater in the CyA-treated group as compared to the non-CyA group. By donor-specific neuronal and glial immunostaining as well as donor-specific DNA labeling, we demonstrate that porcine fetal neuroblasts are able to survive in the adult brain of immunosuppressed rats, mediate functional recovery, and extensively reinnervate the host striatum. These findings suggest that porcine DA neurons may be a suitable alternative to the use of human fetal tissue in neurotransplantation for PD.

Published

1996

29. Cell-mediated delivery of brain-derived neurotrophic factor enhances dopamine levels in an MPP+ rat model of substantia nigra degeneration

Author

David M. Frim, M. Flint Beal, Wendy R. Galpern, Stephen B. Tatter, Ole Isacson, and C. Anthony Altar

Subjects

Brain-derived neurotrophic factor, Transplantation, medicine.medical_specialty, Chemistry, Pars compacta, Dopaminergic, Biomedical Engineering, Substantia nigra, Cell Biology, Neuroprotection, Endocrinology, nervous system, Dopamine, Neurotrophic factors, Internal medicine, Dopaminergic Cell, medicine, Neuroscience, medicine.drug

Abstract

Brain-derived neurotrophic factor (BDNF) promotes the survival of fetal mesencephalic dopaminergic cells and protects dopaminergic neurons against the toxicity of MPP+ in vitro. Supranigral implantation of fibroblasts genetically engineered to secrete BDNF attenuates the loss of substantia nigra pars compacta (SNc) dopaminergic neurons associated with striatal infusion of MPP+ in the adult rat. Using this MPP+ rat model of nigral degeneration, we evaluated the neurochemical effects of supranigral, cell-mediated delivery of BDNF on substantia nigra (SN) dopamine (DA) content and turnover. Genetically engineered BDNF-secreting fibroblasts (approximately 12 ng BDNF/24 h) were implanted dorsal to the SN 7 days prior to striatal MPP+ administration. The present results demonstrate that BDNF-secreting fibroblasts, as compared to control fibroblasts, enhance SN DA levels ipsilateral as well as contralateral to the graft without altering DA turnover. This augmentation of DA levels suggests that local neurotrophic factor delivery by genetically engineered cells may provide a therapeutic strategy for preventing neuronal death or enhancing neuronal function in neurodegenerative diseases characterized by dopaminergic neuronal dysfunction, such as Parkinson's disease.

Published

1996

30. Embryonic stem cells differentiated in vitro as a novel source of cells for transplantation

Author

Ole Isacson, Wendy R. Galpern, Terrence W. Deacon, Judson Ratliff, Douglas B. Jacoby, Jonathan Dinsmore, and Peyman Pakzaban

Subjects

Transplantation, CD40, Myogenesis, Cellular differentiation, Biomedical Engineering, Skeletal muscle, Cell Biology, Biology, Embryonic stem cell, Cell biology, P19 cell, medicine.anatomical_structure, Biochemistry, biology.protein, medicine, Myocyte, Stem cell

Abstract

The controlled differentiation of mouse embryonic stem (ES) cells into near homogeneous populations of both neurons and skeletal muscle cells that can survive and function in vivo after transplantation is reported. We show that treatment of pluripotent ES cells with retinoic acid (RA) and dimethylsulfoxide (DMSO) induce differentiation of these cells into highly enriched populations of gamma-aminobutyric acid (GABA) expressing neurons and skeletal myoblasts, respectively. For neuronal differentiation, RA alone is sufficient to induce ES cells to differentiate into neuronal cells that show properties of postmitotic neurons both in vitro and in vivo. In vivo function of RA-induced neuronal cells was demonstrated by transplantation into the quinolinic acid lesioned striatum of rats (a rat model for Huntington's disease), where cells integrated and survived for up to 6 wk. The response of embryonic stem cells to DMSO to form muscle was less dramatic than that observed for RA. DMSO-induced ES cells formed mixed populations of muscle cells composed of cardiac, smooth, and skeletal muscle instead of homogeneous populations of a single muscle cell type. To determine whether the response of ES cells to DMSO induction could be further controlled, ES cells were stably transfected with a gene coding for the muscle-specific regulatory factor, MyoD. When induced with DMSO, ES cells constitutively expressing high levels of MyoD differentiated exclusively into skeletal myoblasts (no cardiac or smooth muscle cells) that fused to form myotubes capable of spontaneous contraction. Thus, the specific muscle cell type formed was controlled by the expression of MyoD. These results provided evidence that the specific cell type formed (whether it be muscle, neuronal, or other cell types) can be controlled in vitro. Further, these results demonstrated that ES cells can provide a source of multiple differentiated cell types that can be used for transplantation.

Published

1996

31. Transplanted xenogeneic neural cells in neurodegenerative disease models exhibit remarkable axonal target specificity and distinct growth patterns of glial and axonal fibres

Author

Terrence W. Deacon, Lindsay H. Burns, Jonathan Dinsmore, Wendy R. Galpern, Ole Isacson, and Peyman Pakzaban

Subjects

Male, Pathology, medicine.medical_specialty, Swine, Transplantation, Heterologous, Central nervous system, Axonal loss, General Biochemistry, Genetics and Molecular Biology, Rats, Sprague-Dawley, White matter, Basal Ganglia Diseases, In vivo, medicine, Animals, Cells, Cultured, Neurons, biology, CD44, Brain, Parkinson Disease, General Medicine, Immunohistochemistry, Embryonic stem cell, Axons, Rats, Transplantation, Disease Models, Animal, Huntington Disease, medicine.anatomical_structure, nervous system, biology.protein, Neuroglia, Neuroscience, Biomarkers

Abstract

Clinical trials are under way using fetal cells to repair damaged neuronal circuitry. However, little is known about how transplanted immature neurons can grow anatomically correct connections in the adult central nervous system (CNS). We transplanted embryonic porcine neural cells in vivo into adult rat brains with neuronal and axonal loss typical of Parkinson's or Huntington's disease. Using complementary species-specific cellular markers, we found donor axons and CD44+ astroglial fibres in host white matter tracts up to 8 mm from CNS transplant sites, although only donor axons were capable of reaching correct gray matter target regions. This work demonstrates that adult host brain can orient growth of transplanted neurons and that there are differences in transplant donor glial and axonal growth patterns in cellular repair of the mature CNS.

Published

1995

32. Neurotrophic Factor Protection against Excitotoxic Neuronal Death

Author

Ole Isacson, Wendy R. Galpern, and Stephen B. Tatter

Subjects

0301 basic medicine, biology, General Neuroscience, Excitotoxicity, Ciliary neurotrophic factor, medicine.disease_cause, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, Neurotrophic factors, Epidermal growth factor, medicine, Glial cell line-derived neurotrophic factor, biology.protein, Neurology (clinical), Neuroscience, 030217 neurology & neurosurgery, Quinolinic acid, Neurotrophin, Transforming growth factor

Abstract

Neurotrophic factors are polypeptides capable of promoting neuronal survival in both the developing and the adult brain. In addition to the neurotrophins, NGF, brain-derived neurotropic factor, and NT-3 to -6, other neurotrophic factors include ciliary neurotrophic factor, fibroblast growth factors, insulin-like growth factors, members of the transforming growth factor superfamily, members of the epidermal growth factor family, and other cytokines such as leukemia inhibitory factor, oncostatin M, and interleukins-6 and -11. One condition under which these factors promote survival is the challenge of neurons with analogs of excitatory amino acid transmitters. Such analogs, including quinolinic acid, kainic acid, and ibotenic acid, are frequently employed as models of neurological diseases such as Huntington's disease, Parkinson's disease, Alzheimer's disease, epilepsy, cerebellar degenerations, and amyotrophic lateral sclerosis. Excitotoxicity also plays a role in neu ronal death caused by focal ischemia, hypoglycemia, or trauma. Although much has been learned about the mechanisms of both the action of neurotrophic factors and of cell death in response to excitotoxins, the mechanism of protection by these factors remains uncertain. This review explores the biochemical and phys iological changes mediated by neurotrophic factors that may underlie their ability to protect against excito toxic cell death. Second messenger pathways used degenerately by both excitotoxins and neurotrophic factors are discussed as a potential site of interaction mediating the protective effects of neurotrophic factors. Particular attention is also paid to the importance of the route of neurotrophic factor delivery in conferring neuroprotection in particular excitotoxic models. The Neuroscientist 1:286-297, 1995

Published

1995

33. Sham neurosurgical procedures in clinical trials for neurodegenerative diseases: scientific and ethical considerations

Author

Roger A. Barker, Steven Piantadosi, Jacqueline Corrigan-Curay, Thomas B. Freeman, Scott Y. H. Kim, Anthony E. Lang, Danilo A. Tagle, Karl Kieburtz, Jeffrey P. Kahn, Wendy R. Galpern, Christopher G. Goetz, Amy Comstock Rick, and Howard J. Federoff

Subjects

medicine.medical_specialty, Clinical Trials and Supportive Activities, Clinical Sciences, Alternative medicine, Neurodegenerative, Neurosurgical Procedures, Clinical study, Placebos, Clinical Research, Medicine, Humans, Intensive care medicine, Clinical Trials as Topic, Neurology & Neurosurgery, business.industry, Neurosciences, Neurodegenerative Diseases, Nontherapeutic Human Experimentation, Brain Disorders, Clinical trial, Neurological, Neurology (clinical), business, Clinical psychology, Biotechnology

Abstract

Summary There have been several recent scientific advances in gene-based and cell-based therapies that might translate into novel therapeutic approaches for neurodegenerative disorders. Such therapies might need to be directly delivered into the CNS, and complex scientific and ethical assessment will be needed to determine whether a sham neurosurgical arm should be included in clinical trials assessing these agents. We have developed a framework of points for investigators to consider when designing trials that involve direct delivery of a therapeutic agent to the CNS. The inclusion of a sham neurosurgical arm will be guided in part by the objectives of the clinical study (preliminary safety, optimisation, and feasibility vs preliminary efficacy vs confirmatory efficacy) and the need to minimise bias and confounds. Throughout the clinical development process, the perspectives of researchers, ethicists, and patients must be considered, and risks should be minimised whenever possible in a manner that is consistent with good trial design.

Published

2012

34. Chronic benzodiazepine administration

Author

Thomas R. Browne, George K. Szabo, Wendy R. Galpern, Lawrence G. Miller, David J. Greenblatt, and Richard I. Shader

Subjects

Pharmacology, medicine.medical_specialty, Benzodiazepine, medicine.drug_class, business.industry, GABAA receptor, medicine.medical_treatment, Carbamazepine, Biochemistry, Discontinuation, Endocrinology, Anticonvulsant, Neurochemical, Alprazolam, Internal medicine, medicine, business, medicine.drug, Benzodiazepine receptor binding

Abstract

Clinical studies suggest that carbamazepine may attenuate effects of alprazolam discontinuation. Since discontinuation of chronic alprazolam in a mouse model is associated with behavioral alterations and upregulation at the gamma-aminobutyric acidA (GABAA) receptor, we studied the effects of carbamazepine administration after alprazolam (2 mg/kg/day) discontinuation. Open-field activity was increased in mice 4 days after alprazolam discontinuation, but this effect was reduced significantly by continuous infusion of carbamazepine, 25 or 100 mg/kg/day. Benzodiazepine receptor binding in vivo was increased in cortex at 2 and 4 days after alprazolam discontinuation, and in hypothalamus at 4 days; with carbamazepine, 100 mg/kg/day, binding in both regions at these time points was similar to control values. Similar results were observed in cortex with benzodiazepine receptor binding in vitro. GABA-dependent chloride uptake was also increased at 4 days alprazolam administration. Treatment with carbamazepine attenuated (P less than 0.10) this increase. Carbamazepine alone after vehicle did not alter benzodiazepine binding or GABA-dependent chloride uptake. These results indicate that carbamazepine administration after alprazolam discontinuation attenuates behavioral and neurochemical alterations associated with discontinuation.

Published

1991

35. Chronic benzodiazepine administration

Author

Lawrence G. Miller, Richard I. Shader, Wendy R. Galpern, Monica Lumpkin, and David J. Greenblatt

Subjects

Flumazenil, Male, medicine.medical_specialty, medicine.drug_class, medicine.medical_treatment, Convulsants, Motor Activity, Pharmacology, Clonazepam, Bridged Bicyclo Compounds, Mice, Chlorides, Drug tolerance, Internal medicine, medicine, Animals, Benzodiazepine receptor binding, Cerebral Cortex, Benzodiazepine, Behavior, Animal, Muscimol, GABAA receptor, business.industry, musculoskeletal, neural, and ocular physiology, Lorazepam, Drug Tolerance, Bridged Bicyclo Compounds, Heterocyclic, Receptors, GABA-A, Substance Withdrawal Syndrome, Endocrinology, Anticonvulsant, Alprazolam, business, medicine.drug

Abstract

Clonazepam administration may lead to tolerance and "withdrawal" syndromes in clinical use. To assess the effects of this drug in a mouse model, we administered clonazepam (1.5 mg/kg/day) for 1-14 days and evaluated open-field activity, cortical clonazepam concentrations, and binding and function at the GABAA receptor. We also evaluated the same parameters at 1, 2, 4 and 7 days after discontinuation of 7 days of clonazepam administration. During chronic treatment, tolerance developed to the effects of clonazepam on motor activity at 7 days and persisted to 14 days. Cortical clonazepam concentrations did not change significantly during this period. Benzodiazepine receptor binding in vivo was decreased in cortex at days 7 and 14 of clonazepam, but was unchanged in other regions. Binding determined in vitro was also decreased at these points. TBPS (t-butylbicyclophosphorothionate) binding in cortex was slightly, but not significantly, decreased. Muscimol-stimulated chloride uptake was also decreased at days 7 and 14. After clonazepam discontinuation, open-field activity returned to control values at 1 day but was increased above baseline at 4 days. Benzodiazepine binding in vivo and in vitro, as well as TBPS binding, were increased at 4 days. Muscimol-stimulated chloride uptake was also increased at this point. These results indicate that chronic clonazepam administration is associated with tolerance to motoric effects, with discontinuation effects, and with receptor alterations in a mouse model. Clonazepam is similar to other benzodiazepines in this regard.

Published

1991

36. Prenatal exposure to benzodiazepine—I. Prenatal exposure to lorazepam in mice alters open-field activity and GABAA receptor function

Author

Wendy R. Galpern, Lawrence G. Miller, Andrew Schatzki, Monica Lumpkin, David J. Greenblatt, S. Chesley, and Richard I. Shader

Subjects

medicine.medical_specialty, Offspring, medicine.drug_class, Gestational Age, Motor Activity, Lorazepam, Open field, Mice, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Neurochemical, Chlorides, Pregnancy, Reference Values, Internal medicine, mental disorders, medicine, Animals, Maternal-Fetal Exchange, Cerebral Cortex, Pharmacology, Benzodiazepine, Muscimol, GABAA receptor, business.industry, Brain, Receptors, GABA-A, medicine.disease, Endocrinology, chemistry, Female, business, medicine.drug

Abstract

Prenatal exposure to benzodiazepines may lead to developmental abnormalities in humans and animals. To assess the behavioral and neurochemical effects of such exposure, pregnant mice were treated with lorazepam, 2 mg/kg/day, from days 13-20 of gestation, and open-field activity was assessed in offspring at 3 and 6 weeks of age and the function of GABAA receptors at 6 weeks of age. Activity was increased in mice exposed to lorazepam, compared to untreated or vehicle-treated controls at 3 weeks, but was unchanged at 6 weeks. Muscimol-stimulated uptake of chloride was decreased in lorazepam-treated mice, compared to controls, with a decrease in maximum uptake but no change in the EC50 for muscimol. Concentrations of lorazepam in maternal plasma and brain showed a similar brain:plasma ratio as previously reported and concentrations in fetal brain were about 50% of maternal levels. Lorazepam persisted for 48 hours after birth in dams but not in the offspring. These results indicate persistent behavioral and neurochemical alterations after prenatal exposure to lorazepam. This model may be useful in assessing other effects of prenatal exposure to benzodiazepine.

Published

1991

37. Neuroprotection: lessons from a spectrum of neurological disorders

Author

Wendy R. Galpern and Aneesh B. Singhal

Subjects

medicine.medical_specialty, business.industry, 030204 cardiovascular system & hematology, Neuroprotection, Stroke, 03 medical and health sciences, 0302 clinical medicine, Neuroprotective Agents, Neurology, medicine, Humans, Nervous System Diseases, Psychiatry, business, 030217 neurology & neurosurgery

Published

2008

38. Ipratropium bromide spray as treatment for sialorrhea in Parkinson's disease

Author

Abena Asante, Tamara Arenovich, Teri Thomsen, Wendy R. Galpern, and Susan H. Fox

Subjects

Male, medicine.drug_class, Ipratropium bromide, Placebo, Drooling, Cholinergic Antagonists, law.invention, Randomized controlled trial, law, medicine, Anticholinergic, Humans, Treatment Failure, Saliva, Aged, Aged, 80 and over, Sialorrhea, Cross-Over Studies, business.industry, Parkinsonism, Ipratropium, Parkinson Disease, Middle Aged, medicine.disease, Crossover study, Neurology, Anesthesia, Female, Neurology (clinical), medicine.symptom, business, medicine.drug

Abstract

Sialorrhea is a significant problem in advanced Parkinson's disease (PD). Current treatment options include systemic anticholinergics which frequently cause side effects. We hypothesized that sublingual application of ipratropium bromide spray, an anticholinergic agent that does not cross the blood brain barrier, may reduce drooling without systemic side effects. We performed a randomized, double blind, placebo-controlled, crossover study in 17 subjects with PD and bothersome drooling. Patients were randomized to receive ipratropium bromide or placebo (one to two sprays, maximum of four times per day) for 2 weeks followed by a 1 week washout and crossover for further 2 weeks of treatment. The primary outcome was an objective measure of weight of saliva production. Secondary outcomes were subjective rating of severity and frequency of sialorrhoea using home diaries, United Parkinson's Disease Rating Scale (UPDRS) part II salivation subscore, parkinsonian disability using UPDRS, and adverse events. Ipratropium bromide spray had no significant effect on weight of saliva produced. There was a mild effect of treatment on subjective measures of sialorrhea. There were no significant adverse events. Ipratropium bromide spray was well tolerated in subjects with PD. Although it did not affect objective measures of saliva production, further studies in parkinsonism may be warranted.

Published

2007

39. Diagnostic criteria for psychosis in Parkinson's disease: report of an NINDS, NIMH work group

Author

Bernard Ravina, Laura Marsh, Debra Babcock, Mark Stacy, Valerie Voon, Joseph H. Friedman, Dag Aarsland, Wendy R. Galpern, Katrina Gwinn-Hardy, Andrew J. Lees, Jean Endicott, Karen Marder, Christopher G. Goetz, William M. McDonald, Diane Murphy, J. L. Cummings, Stewart A. Factor, and Hubert H. Fernandez

Subjects

Psychosis, medicine.medical_specialty, Parkinson's disease, Consensus, Pimavanserin, Disease, Severity of Illness Index, Education, Central nervous system disease, Diagnosis, Differential, chemistry.chemical_compound, Degenerative disease, medicine, Prevalence, Dementia, Humans, Psychiatry, National Institute of Mental Health (U.S.), Publishing, Parkinson Disease, medicine.disease, United States, Neurology, chemistry, Psychotic Disorders, Schizophrenia, Neurology (clinical), Psychology

Abstract

There are no standardized diagnostic criteria for psychosis associated with Parkinson's disease (PDPsy). As part of an NIH sponsored workshop, we reviewed the existing literature on PDPsy to provide criteria that distinguish PDPsy from other causes of psychosis. Based on these data, we propose provisional criteria for PDPsy in the style of the Diagnostic and Statistical Manual of Mental Disorders IV-TR. PDPsy has a well-characterized temporal and clinical profile of hallucinations and delusions, which is different than the pattern seen in other psychotic disorders such as substance induced psychosis or schizophrenia. PDPsy is associated with a poor prognosis of chronic psychosis, nursing home placement, and death. Medications used to treat Parkinson's disease (PD) contribute to PDPsy but may not be sufficient or necessary contributors to PDPsy. PDPsy is associated with Lewy bodies pathology, imbalances of monoaminergic neurotransmitters, and visuospatial processing deficits. These findings suggest that PDPsy may result from progression of the disease process underlying PD, rather than a comorbid psychiatric disorder or drug intoxication. PDPsy is not adequately described by existing criteria for psychotic disorders. We established provisional diagnostic criteria that define a constellation of clinical features not shared by other psychotic syndromes. The criteria are inclusive and contain descriptions of the full range of characteristic symptoms, chronology of onset, duration of symptoms, exclusionary diagnoses, and associated features such as dementia. These criteria require validation and may be refined, but form a starting point for studies of the epidemiology and pathophysiology of PDPsy, and are a potential indication for therapy development.

Published

2007

40. Screening potential therapies: lessons learned from new paradigms used in Parkinson disease

Author

Wendy R. Galpern and Barbara C. Tilley

Subjects

medicine.medical_specialty, Phase iii trials, Advisory Committees, Phases of clinical research, Disease, Outcome (game theory), Antiparkinson Agents, medicine, Humans, Intensive care medicine, Stroke, Advanced and Specialized Nursing, business.industry, Medical screening, Outcome measures, Parkinson Disease, medicine.disease, United States, Surgery, Stroke treatment, Neuroprotective Agents, Clinical Trials, Phase III as Topic, National Institutes of Health (U.S.), Neurology (clinical), Cardiology and Cardiovascular Medicine, business

Abstract

In Parkinson Disease (PD) as well as in stroke research there is an urgent need to both optimize the use of resources (number of patients, costs, and time) and select potential effective neuroprotective agents. The processes used to identify and study new therapies for PD may be applicable to the search for new therapies in stroke. The National Institute of Neurological Disorders and Stroke (NINDS) organized the Committee to Identify Neuroprotective Agents for Parkinson’s (CINAPS). CINAPS broadly solicited suggestions for agents and evaluated these agents using rigorous criteria. NINDS also created the NIH Exploratory Trials in PD program (NET-PD), a clinical network where CINAPS recommendations could be tested. Given multiple recommended agents, NET-PD investigators used Phase II futility designs with calibration controls, tested against an historical standard, to screen agents for testing in Phase III trials. Investigators also used the Phase II trial to assess ancillary outcome measures for use in Phase III. The observed value for the calibration controls in the first NET-PD Phase II trial was outside the 95% CI for the historical standard. Using bootstrap methodology it appeared unlikely this outcome happened by chance. The historical standard was updated using more contemporaneous data than were available at the start of the futility trials and a re-evaluation using the new threshold was conducted. Assessment of ancillary outcome measures led to a reduced set of outcome measures for use in Phase III. The CINAPS process, and lessons learned from NET-PD futility studies, particularly with respect to calibration controls and assessment of outcome measures, could enhance the choice and testing of new agents for stroke treatment.

Published

2007

41. Coenzyme Q treatment of neurodegenerative diseases of aging

Author

Merit Cudkowicz and Wendy R. Galpern

Subjects

Aging, Antioxidant, Parkinson's disease, Time Factors, Ubiquinone, medicine.medical_treatment, macromolecular substances, Disease, Mitochondrion, medicine.disease_cause, Bioinformatics, Models, Biological, Huntington's disease, medicine, Animals, Humans, Amyotrophic lateral sclerosis, Molecular Biology, Clinical Trials as Topic, business.industry, Amyotrophic Lateral Sclerosis, Neurodegenerative Diseases, Parkinson Disease, Cell Biology, medicine.disease, Huntington Disease, Treatment Outcome, Coenzyme Q – cytochrome c reductase, Mutation, Molecular Medicine, business, Oxidative stress

Abstract

The etiology of several neurodegenerative disorders is thought to involve impaired mitochondrial function and oxidative stress. Coenzyme Q-10 (CoQ10) acts both as an antioxidant and as an electron acceptor at the level of the mitochondria. In several animal models of neurodegenerative diseases including amyotrophic lateral sclerosis, Huntington's disease, and Parkinson's disease, CoQ10 has shown beneficial effects. Based on its biochemical properties and the effects in animal models, several clinical trials evaluating CoQ10 have been undertaken in many neurodegenerative diseases. CoQ10 appears to be safe and well tolerated, and several efficacy trials are planned.

Published

2006

42. Cell-mediated delivery of neurotrophic factors and neuroprotection in the neostriatum and substantia nigra

Author

Stephen B. Tatter, Xandra O. Breakefield, David M. Frim, Ole Isacson, James M. Schumacher, and Wendy R. Galpern

Subjects

Central nervous system, Substantia nigra, Biology, Neuroprotection, Cell mediated immunity, Transplantation, medicine.anatomical_structure, Developmental Neuroscience, Neurology, Neurotrophic factors, Gene expression, Basal ganglia, medicine, Neurology (clinical), Neuroscience

Published

1995

43. Transplanting Fetal Neural Xenogeneic Cells in Parkinson's and Huntington's Disease Models

Author

Ole Isacson, Peyman Pakzaban, and Wendy R. Galpern

Published

2003

44. 1.003 FACILITATING CLINICAL RESEARCH: THE NATIONAL INSTITUTE OF NEUROLOGICAL DISORDERS (NINDS) AND STROKE PARKINSON'S DISEASE COMMON DATA ELEMENTS PROJECT

Author

Andrew Siderowf, Karen Marder, Cornelia Kamp, Karl Kieburtz, Anthony E. Lang, Caroline M. Tanner, Wendy R. Galpern, Jordan J. Elm, Mahlon R. DeLong, T. Faroud, Kenneth Marek, Dennis W. Dickson, Ronald F. Pfeiffer, Daniel Weintraub, and G. W. Ross

Subjects

medicine.medical_specialty, Clinical research, Parkinson's disease, Neurology, business.industry, Medicine, Neurology (clinical), Geriatrics and Gerontology, business, Psychiatry, medicine.disease, Stroke

Published

2012

45. A Randomized Clinical Trial of High-Dosage Coenzyme Q10 in Early Parkinson Disease

Author

Diane Cote, Jeri Sieren, Alex Rajput, James W. Tetrud, Paul J. Tuite, Christopher T. Ingvoldstad, Cheryl Waters, Shari Niswonger, Roger Kurlan, David D. Song, Jennifer Young, Samuel Markind, Alicia Palao, Munira Sultana, Christine Hunter, Karen Williams, Sandra K. Kostyk, John G. Nutt, Andrew Feigin, Dragos Mihaila, Karen Blindauer, Abraham Lieberman, Annette Robinson, Adrienna Winters, Michelle Cines, Mattson Ogg, Robert A. Hauser, Ira Shoulson, Julia Spears, Jorge L. Juncos, William G. Ondo, David Simon, Mark Stacy, Stacy Merritt, Barbara Shannon, Un Jung Kang, Katie Kompoliti, Cheryl Deeley, Joanne Field, Arthur Watts, Buff Farrow, Karen Helles, Katharine Smith, Karen Thomas, Rajan Prakash, Joel S. Perlmutter, Rajeev Kumar, Mandar Jog, Pamela King, Neal Hermanowicz, Stephen G. Reich, Mark Chilton, Lawrence Severt, Vanessa K. Hinson, Kapil D. Sethi, Mark F. Lew, Pinky Agarwal, Clifford M Shults, Natividad Stover, Richard H. Haas, Jayaraman Rao, Thomas Mayer, Thyagarajan Subramanian, Althea Silver, Richard M. Zweig, Lin Zhang, Hubert H. Fernandez, Linda Cole, Charles H. Adler, Jean Rivest, Marye Kellermann, Marlene Lind, Stephanie Wilson, Jennifer Conway, Ray L. Watts, Monica Beland, Joseph H. Friedman, Michael S. Okun, Maureen Cook, Stephen Grill, Cindy Zadikoff, Irene Litvan, Donna Stuppy Ford, Karen Frei, L Pepper Lumina, David Grimes, Sofya Glazman, Edward Drasby, Wendy R. Galpern, Susan Rolandelli, Sharon Evans, Bernard Ravina, Robert W. Hamill, Jo Bergholte, Andrew Siderowf, W.R. Wayne Martin, Rajesh Pahwa, Sanja Obradov, April Langhammer, Lorelei Derwent, Barbara Sommerfeld, M. Flint Beal, Alok Sahay, Anita Blenke, Liza Reys, Melisa Pelikan, Amy Duffy, Holly A. Shill, Eric Molho, Ivan Bodis-Wollner, Candace Cotto, Marilyn Cowper, Marian L. Evatt, Ani Arkun, Johanna M Hartlein, Nancy Zappala, Clara Schindler Propsom, Matthew Brodsky, Colette Lynn Hilliard, Stephanie Lessig, Stephanie Guthrie, Joanne Wojcieszek, Deborah Fontaine, Irene H. Richard, Zoltan Mari, Kathy Davis, Carlos Singer, Samuel A. Ellias, Lawrence Elmer, Julie So, Louisette Bond, Janis M. Miyasaki, Camille Swartz, Ranjit Ranawaya, Brian Griebner, Ramon L. Rodriguez, Ronald F. Pfeiffer, Becky Dunlop, David Oakes, Michel Panisset, Tiffini Voss, Joohi Jimenez-Shahed, Karyn Boyar, Cathi-Ann Thomas, Victoria Snively, Claire Henchcliffe, Margaret C. Lannon, Maureen Gartner, Cherissa Sia, Maureen A. Leehey, Joan Young, Anwar Ahmed, David S. Russell, Melissa J. Nirenberg, Emmanuelle Pourcher, James T. Boyd, Lauren Kraics, Ted M. Dawson, Ergun Y. Uc, Shan Gao, and Angel Figueroa

Subjects

Male, medicine.medical_specialty, Ubiquinone, Population, Unified Parkinson's disease rating scale, Placebo, Antioxidants, law.invention, Double-Blind Method, Randomized controlled trial, law, Internal medicine, medicine, Humans, Prospective Studies, education, Adverse effect, Prospective cohort study, Aged, education.field_of_study, Dose-Response Relationship, Drug, business.industry, Parkinsonism, Parkinson Disease, Middle Aged, medicine.disease, Clinical trial, Early Diagnosis, Treatment Outcome, Physical therapy, Female, Neurology (clinical), business

Abstract

Importance Coenzyme Q10 (CoQ10), an antioxidant that supports mitochondrial function, has been shown in preclinical Parkinson disease (PD) models to reduce the loss of dopamine neurons, and was safe and well tolerated in early-phase human studies. A previous phase II study suggested possible clinical benefit. Objective To examine whether CoQ10 could slow disease progression in early PD. Design, Setting, and Participants A phase III randomized, placebo-controlled, double-blind clinical trial at 67 North American sites consisting of participants 30 years of age or older who received a diagnosis of PD within 5 years and who had the following inclusion criteria: the presence of a rest tremor, bradykinesia, and rigidity; a modified Hoehn and Yahr stage of 2.5 or less; and no anticipated need for dopaminergic therapy within 3 months. Exclusion criteria included the use of any PD medication within 60 days, the use of any symptomatic PD medication for more than 90 days, atypical or drug-induced parkinsonism, a Unified Parkinson’s Disease Rating Scale (UPDRS) rest tremor score of 3 or greater for any limb, a Mini-Mental State Examination score of 25 or less, a history of stroke, the use of certain supplements, and substantial recent exposure to CoQ10. Of 696 participants screened, 78 were found to be ineligible, and 18 declined participation. Interventions The remaining 600 participants were randomly assigned to receive placebo, 1200 mg/d of CoQ10, or 2400 mg/d of CoQ10; all participants received 1200 IU/d of vitamin E. Main Outcomes and Measures Participants were observed for 16 months or until a disability requiring dopaminergic treatment. The prospectively defined primary outcome measure was the change in total UPDRS score (Parts I-III) from baseline to final visit. The study was powered to detect a 3-point difference between an active treatment and placebo. Results The baseline characteristics of the participants were well balanced, the mean age was 62.5 years, 66% of participants were male, and the mean baseline total UPDRS score was 22.7. A total of 267 participants required treatment (94 received placebo, 87 received 1200 mg/d of CoQ10, and 86 received 2400 mg/d of CoQ10), and 65 participants (29 who received placebo, 19 who received 1200 mg/d of CoQ10, and 17 who received 2400 mg/d of CoQ10) withdrew prematurely. Treatments were well tolerated with no safety concerns. The study was terminated after a prespecified futility criterion was reached. At study termination, both active treatment groups showed slight adverse trends relative to placebo. Adjusted mean changes (worsening) in total UPDRS scores from baseline to final visit were 6.9 points (placebo), 7.5 points (1200 mg/d of CoQ10; P = .49 relative to placebo), and 8.0 points (2400 mg/d of CoQ10; P = .21 relative to placebo). Conclusions and Relevance Coenzyme Q10 was safe and well tolerated in this population, but showed no evidence of clinical benefit. Trial Registration clinicaltrials.gov Identifier:NCT00740714

Published

2014

46. Detection of dopaminergic cell loss and neural transplantation using pharmacological MRI, PET and behavioral assessment

Author

M F Beal, Bruce R. Rosen, Anna-Liisa Brownell, E. Livni, Mikhail B. Bogdanov, Wendy R. Galpern, Yin-Ching Iris Chen, Ole Isacson, and Bruce G. Jenkins

Subjects

Cell Transplantation, Dopamine, Microdialysis, Striatum, Biology, Rats, Sprague-Dawley, Striatonigral Degeneration, Cocaine, Dopamine Uptake Inhibitors, Dopaminergic Cell, Basal ganglia, medicine, Animals, Amphetamine, Dopamine transporter, Neurons, Behavior, Animal, General Neuroscience, Dopaminergic, Sympathectomy, Chemical, Magnetic Resonance Imaging, Rats, Transplantation, biology.protein, Female, Neuroscience, medicine.drug, Tomography, Emission-Computed

Abstract

We demonstrate the use of magnetic resonance imaging (MRI) for detection of neurotransmitter stimulation using the dopamine transporter ligands amphetamine and CFT (2beta-carbomethoxy-3beta-(4-fluorophenyl)tropane) as pharmacological challenges. We demonstrate that the unilateral loss of a hemodynamic response to either amphetamine or CFT challenge by unilateral 6-hydroxydopamine lesioning is restored by transplantation of fetal dopamine neurons in the striatum. The time course for the hemodynamic changes parallels the time courses for dopamine release, measured by prior microdialysis studies, and also for the rotational behavior in the unilaterally lesioned animals. Transplantation of the fetal cells results in hemodynamic time courses after CFT or amphetamine challenges at the graft site that are identical to those induced both before transplantation and on the intact contralateral side. The transplantation also results in complete behavioral recovery. The spatial extent of the dopaminergic recovery in the lesioned striatum is the same when measured using either PET of tracer levels of [11C]CFT binding or MRI. These results show great promise for the application of pharmacological MRI for application to studies of dopamine cell loss and potential recovery in Parkinson's disease.

Published

1999

47. Transplanting Fetal Neural Xenogeneic Cells in Parkinson’s and Huntington’s Disease Models

Author

Peyman Pakzaban, Ole Isacson, and Wendy R. Galpern

Subjects

Fetus, business.industry, Xenotransplantation, medicine.medical_treatment, Human Fetal Tissue, Disease, medicine.disease, Bioinformatics, Embryonic stem cell, Transplantation, Huntington's disease, Neuroblast, embryonic structures, medicine, business

Abstract

Fetal allogeneic neural transplants have been repeatedly shown to cause functional recovery in animal models of neurodegenerative diseases (1–8), improve symptoms, and reduce drug-induced side effects in patients with Parkinson’s disease (9–13). It has, however, proven difficult to obtain human fetal tissue for neural transplantation, both from a practical and ethical standpoint (14–16). Thus, although a therapeutic rationale exists for using allogeneic neural transplantation in Parkinson’s (and Huntington’s) disease, the limited availability of human fetal neural tissue poses serious limitations on clinical application (17). Neural xenotransplantation, which is transplantation of fetal neuroblasts obtained from homologous neural structures of a different (mammalian) species into the adult brain, overcomes many of the limitations associated with the use of human fetuses. For clinical use, neuroblasts at precisely defined embryonic ages can be prepared in large quantities and in a sterile fashion from the fetuses of especially bred pathogen-free xenogeneic donors.

Published

1998

48. Detection of dopaminergic neurotransmitter activity using pharmacologic MRI: correlation with PET, microdialysis, and behavioral data

Author

John R. Keltner, Russell T. Matthews, Bruce G. Jenkins, Yin Ching I. Chen, Ole Isacson, Mikhail B. Bogdanov, Anna-Liisa Brownell, Bruce R. Rosen, M. Flint Beal, and Wendy R. Galpern

Subjects

Cingulate cortex, medicine.medical_specialty, Dextroamphetamine, Dopamine, Microdialysis, Striatum, Sensitivity and Specificity, Receptors, Dopamine, Rats, Sprague-Dawley, chemistry.chemical_compound, Adrenergic Agents, Cocaine, Dopamine Uptake Inhibitors, Internal medicine, medicine, Animals, Radiology, Nuclear Medicine and imaging, Neurotransmitter, Amphetamine, Oxidopamine, Dopamine transporter, biology, Behavior, Animal, Chemistry, Dopaminergic, Brain, Magnetic Resonance Imaging, Rats, Endocrinology, Dopamine receptor, biology.protein, Neuroscience, medicine.drug, Tomography, Emission-Computed

Abstract

The metabolic activation resulting from direct dopaminergic stimulation can be detected using auto-radiography, positron emission tomography (PET) or, potentially, fMRI techniques. To establish the validity of the latter possibility, we have performed a number of experiments. We measured the regional selectivity of two different dopaminergic ligands: the dopamine release compound D-amphetamine and the dopamine transporter antagonist 2β-carbomethoxy-3β-(4-fluoropheny) tropane (CFT). Both compounds led to increased signal intensity in gradient echo images in regions of the brain with high dopamine receptor density (frontal cortex, striatum, cingulate cortex ≫ parietal cortex). Lesioning the animals with unilaterally administered 6-hydroxydopamine (6-OHDA) led to ablation of the phMRI response on the ipsilateral side; control measurements of rCBV and rCBF using bolus injections of Gd,-DTPA showed that the baseline rCBV and rCBF values weire intact on the lesioned side. The time course of the BOLD signal changes paralleled the changes observed by microdialyisis measurements of dopamine release in the striatum for both amphetamine and CFT; peaking at 20–40 min after injection and returning to baseline at about 70–90 min. Signal changes were not correlated with either heart rate, blood pressure or pCO2. Measurement of PET binding in the same animals showed an excellent correlation with the phMRI data when compared by either measurements of the number of pixels activated or percent signal change in a given region. The time course for the behavioral measurements of rotation in the 6-OHDA lesioned animals correlated with the phMRI. These experiments demonstrate that phMRI will become a valuable, noninvasive tool for investigation of neurotransmitter activity in vivo. Key words: fMRI; dopamine; amphetamine; CFT.

Published

1997

49. NGF attenuates 3-nitrotyrosine formation in a 3-NP model of Huntington's disease

Author

M. Flint Beal, Russell T. Matthews, Ole Isacson, and Wendy R. Galpern

Subjects

Male, medicine.medical_specialty, Programmed cell death, Oxidative phosphorylation, Neuroprotection, Nitric oxide, Rats, Sprague-Dawley, chemistry.chemical_compound, Huntington's disease, Internal medicine, medicine, Animals, Nerve Growth Factors, business.industry, General Neuroscience, Neurodegeneration, medicine.disease, Nitro Compounds, Corpus Striatum, Rats, Disease Models, Animal, Nerve growth factor, Endocrinology, Huntington Disease, nervous system, chemistry, Tyrosine, Propionates, business, Peroxynitrite

Abstract

Nerve growth factor (NGF)-secreting fibroblasts are able to protect against the Huntington-like striatal neurodegeneration induced by the mitochondrial toxin 3-nitropropionic acid (3-NP). In the present study, we investigated whether the neuroprotective effects of NGF are mediated through antioxidative mechanisms. Rats were grafted in the corpus callosum with NGF[+] or NGF[-] fibroblasts 7 days before administration of 3-NP. The generation of peroxynitrite was evaluated by measuring the striatal levels of 3-nitrotyrosine. NGF significantly decreased the 3-NP induced generation of 3-nitrotyrosine, presumably by decreasing peroxynitrite formation. These findings suggest that NGF might protect against neuronal death by inhibiting the production of nitric oxide or decreasing the levels of superoxide radicals, thereby decreasing the generation of oxidative agents such as peroxynitrite.

Published

1996

50. Implanted fibroblasts genetically engineered to produce brain-derived neurotrophic factor prevent 1-methyl-4-phenylpyridinium toxicity to dopaminergic neurons in the rat

Author

Ole Isacson, David M. Frim, M F Beal, Xandra O. Breakefield, Wendy R. Galpern, and T. A. Uhler

Subjects

Male, medicine.medical_specialty, 1-Methyl-4-phenylpyridinium, Cell Survival, Substantia nigra, Nerve Tissue Proteins, Cell Line, Receptors, Dopamine, Rats, Sprague-Dawley, chemistry.chemical_compound, Neurotrophic factors, Dopaminergic Cell, Internal medicine, medicine, Animals, Nerve Growth Factors, Cells, Cultured, Brain-derived neurotrophic factor, Neurons, Multidisciplinary, MPTP, Brain-Derived Neurotrophic Factor, Dopaminergic, Anatomy, Fibroblasts, medicine.disease, Rats, Substantia Nigra, Mitochondrial toxicity, Endocrinology, chemistry, nervous system, Nerve Degeneration, Genetic Engineering, Research Article

Abstract

The trophism of brain-derived neurotrophic factor (BDNF) for dopaminergic cells in culture has led to significant interest in the role of BDNF in the etiology and potential treatment of Parkinson disease. Previous in vivo investigation of BDNF delivery to axotomized substantia nigra dopaminergic neurons in the adult rat has shown no protective effect. In this study, we produced nigral degeneration by infusing 1-methyl-4-phenylpyridinium (MPP+), a mitochondrial complex I inhibitor and the active metabolite of 1-methyl-4-phenyl-1,2,3,6- tetrahydropyridine (MPTP), into the rat striatum. The subsequent loss of nigral neurons was presumably due to mitochondrial toxicity after MPP+ uptake and retrograde transport to the substantia nigra. We engineered immortalized rat fibroblasts to secrete human BDNF and implanted these cells near the substantia nigra 7 days before striatal MPP+ infusion. We found that BDNF-secreting fibroblasts markedly increased nigral dopaminergic neuronal survival when compared to control fibroblast implants. The observation that BDNF prevents MPTP-induced dopaminergic neuronal degeneration in the adult brain has significance for the treatment of neurodegenerative disorders, which may involve mitochondrial dysfunction, such as Parkinson disease.

Published

1994