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1. Randomized, double‐blind, placebo‐controlled study of interferon‐ γ 1b in Friedreich Ataxia

Author

Kim Schadt, Jeffrey W. Sherman, Tom Vescio, Lauren A. Hauser, Julie Ball, Ashley McCormick, S. H. Subramony, Jennifer M. Farmer, Yi Na Dong, Renee Perdok, Susan Perlman, Katherine D. Mathews, Shana E. McCormack, Amy Y. Grahn, David A. Lynch, Alicia Brocht, and McKenzie Wells

Subjects
0301 basic medicine, medicine.medical_specialty, Ataxia, Placebo-controlled study, Placebo, law.invention, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, law, Internal medicine, medicine, Interferon gamma, Young adult, biology, business.industry, General Neuroscience, Natural history, 030104 developmental biology, Frataxin, biology.protein, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery, medicine.drug
Abstract

Objective In vitro, in vivo, and open-label studies suggest that interferon gamma (IFN-γ 1b) may improve clinical features in Friedreich Ataxia through an increase in frataxin levels. The present study evaluates the efficacy and safety of IFN-γ 1b in the treatment of Friedreich Ataxia through a double-blind, multicenter, placebo-controlled trial. Methods Ninety-two subjects with FRDA between 10 and 25 years of age were enrolled. Subjects received either IFN-γ 1b or placebo for 6 months. The primary outcome measure was the modified Friedreich Ataxia Rating Scale (mFARS). Results No difference was noted between the groups after 6 months of treatment in the mFARS or secondary outcome measures. No change was noted in buccal cell or whole blood frataxin levels. However, during an open-label extension period, subjects had a more stable course than expected based on natural history data. Conclusions This study provides no direct evidence for a beneficial effect of IFN-γ1b in FRDA. The modest stabilization compared to natural history data leaves open the possibility that longer studies may demonstrate benefit.

Published
2019

2. Efficacy of Nilotinib in Patients With Moderately Advanced Parkinson Disease

Author

Jaime Adams, Samuel Frank, Deborah Baker, Saurav Brahmachari, Elizabeth A. Klingner, Jason Aldred, Jennifer Mule, Meredith Spindler, Cornelia Kamp, Phounsavath Muneath, Claudia Rocha, Liana Baker, Gian Pal, Doozie Russell, Yvette Pitchford, Tina Ward, Olga Kishchenko, Kellie Keith, Angela S Stovall, Courtney Blair, John Slevin Slevin, Vanessa K. Hinson, Grace Bwala, Brian K. Fiske, Liana S. Rosenthal, Joohi Shahed, Andrew P. Duker, Patrick Bolger, Gary Rafaloff, David Weiner, Adolfo Ramirez-Zamora, Zoltan Mari, Renee Wagner Wagner, Helen Matthews, Karen Blindauer, Derek B. Ridgeway, Alexandria Oliver, Carlinda Field, Stephanie Burrows, Binit B. Shah, Lauren Seeberger, Charles S. Venuto, Katie Sullivan, Laura Ramirez, Erika F. Augustine, Matthew Swan, Lilliana Dumitrescu, Natividad Stover, Shonna Jenkins, Sharon Evans, Lin Zhang, Anwar Ahmed, Tanya Simuni, Michael A. Schwarzschild, Christopher S. Coffey, Mark S. LeDoux, David-Erick Lafontant, Laura Trusso, Farah Ismail, John L. Goudreau, Eric Molho, Sue Henderson, Cindy Casaceli, Christine Hunter, Holly Reynolds, Albert Y. Hung, Robert A. Hauser, Burton L. Scott, Lynn Wheeler, Kalpana Merchant, Chelsea Caspell-Garcia, Claire E. Wegel, Richard K. Wyse, Patrik Brundin, Christina Gruenwald, Alicia Brocht, Candace Cromer, Lisa Gauger, Melissa Bixby, Emily Carman, Kathryn A. Chung, Nichole McMullen, David Simon, Ken Eaton, Oren A. Levy, Amber Servi, Abigail Simpson, Holly A. Shill, Kelvin L. Chou, Melissa Kostrzebski, and Ted M. Dawson

Subjects
medicine.medical_specialty, business.industry, Montreal Cognitive Assessment, Placebo, Asymptomatic, law.invention, 03 medical and health sciences, Regimen, 0302 clinical medicine, Randomized controlled trial, Tolerability, Nilotinib, law, Internal medicine, Cohort, Medicine, 030212 general & internal medicine, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery, medicine.drug
Abstract

Importance There is a critical need for careful and independent validation of reported symptomatic efficacy and dopaminergic biomarker changes induced by nilotinib in Parkinson disease (PD). Objectives To assess safety and tolerability of nilotinib in participants with moderately advanced PD. Secondary and exploratory objectives were to assess its affect on PD disability, pharmacokinetics, cerebrospinal fluid (CSF) penetration, and biomarkers. Design, Setting, and Participants This was a 6-month, multicenter, randomized parallel-group, double-blind, placebo-controlled trial. Recruitment was from November 20, 2017, to December 28, 2018, and follow-up ended on September 9, 2019. The study was conducted at 25 US sites. The study approached 173 patients, of whom 48 declined, 125 were screened, and 76 who received a stable regimen of PD medications were enrolled (39% screen failure). Interventions Participants were randomized 1:1:1 to placebo, 150-mg nilotinib, or 300-mg nilotinib once daily orally for 6 months, followed by 2-month off-drug evaluation. Main Outcomes and Measures The primary outcomes were safety and tolerability. The tolerability end point was defined as the ability to complete the study while receiving the assigned dose. An active arm was considered tolerable if the percentage of participants meeting the tolerability end point for that group was not significantly lower than the percentage observed in the placebo group. Secondary outcomes included change in PD disability (Movement Disorder Society Unified Parkinson’s Disease Rating Scale [MDS-UPDRS], Part II OFF/ON). Exploratory outcomes included serum and CSF pharmacokinetic profile, and CSF dopaminergic biomarkers. Results At baseline, mean (SD) participants’ age was 64.6 (7.5) years, 52 were male (68%), mean (SD) disease duration was 9.9 years (4.7), MDS-UPDRS Part 1-3 OFF score was 66.4 (19.3), ON score was 48.4 (16.2), and Montreal Cognitive Assessment score was 27.1 (2.2). The number of participants who completed the study receiving the assigned dose were 21 (84%), 19 (76%), and 20 (77%) in the placebo, 150-mg, and 300-mg arms, respectively. Both active doses had acceptable safety profile. The most common reasons for drug suspension were asymptomatic, dose-dependent elevations of amylase, and/or lipase. Nilotinib, 150 mg and 300 mg, exhibited worse MDS-UPDRS-3 ON scores compared with placebo, achieving significance for nilotinib, 300 mg, at month 1 (P Conclusions and Relevance While we demonstrated acceptable safety and tolerability of nilotinib in our cohort, the low CSF exposure and lack of biomarkers effect combined with the efficacy data trending in the negative direction indicate that nilotinib should not be further tested in PD. Trial Registration ClinicalTrials.gov Identifier:NCT03205488

Published
2021

3. Progression of Friedreich ataxia: quantitative characterization over 5 years

Author

Jennifer Farmer, Cassandra J Strawser, Katherine D. Mathews, Martin B. Delatycki, Charles J. Isaacs, Sarah Gelbard, Julianna E. Shinnick, Christopher M. Gomez, Eppie M. Yiu, Kimberly Schadt, Susan Perlman, S. H. Subramony, Maya Patel, Theresa A. Zesiewicz, David A. Lynch, Debbie L. Foerster, Grace Yoon, George Wilmot, Lauren Seyer, Karlla W. Brigatti, and Alicia Brocht

Subjects
0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Pediatrics, medicine.medical_specialty, Ataxia, business.industry, General Neuroscience, MEDLINE, Progressive neurodegenerative disorder, Clinical trial, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Power calculations, Physical therapy, Medicine, sense organs, Neurology (clinical), medicine.symptom, business, Research Articles, 030217 neurology & neurosurgery, Research Article
Abstract

Objective Friedreich ataxia (FRDA) is a progressive neurodegenerative disorder of adults and children. This study analyzed neurological outcomes and changes to identify predictors of progression and generate power calculations for clinical trials. Methods Eight hundred and twelve subjects in a natural history study were evaluated annually across 12 sites using the Friedreich Ataxia Rating Scale (FARS), 9‐Hole Peg Test, Timed 25‐Foot Walk, visual acuity tests, self‐reported surveys and disability scales. Cross‐sectional outcomes were assessed from recent visits, and longitudinal changes were gaged over 5 years from baseline. Results Cross‐sectional outcomes correlated with measures of disease severity. Age, genetic severity (guanine‐adenine‐adenine [GAA] repeat length), and testing site predicted performance. Serial progression was relatively linear using FARS and composite measures of performance, while individual performance outcomes were nonlinear over time. Age strongly predicted change from baseline until removing the effects of baseline FARS scores, when GAA becomes a more important factor. Progression is fastest in younger subjects and subjects with longer GAA repeats. Improved coefficients of variation show that progression results are more reproducible over longer assessment durations. Interpretation While age predicted progression speed in simple analyses and may provide an effective way to stratify cohorts, separating the effects of age and genetic severity is difficult. Controlling for baseline severity, GAA is the major determinant of progression rate in FRDA. Clinical trials will benefit from enrollment of younger subjects, and sample size requirements will shrink with longer assessment periods. These findings should prove useful in devising gene therapy trials in the near future.

Published
2016

4. Comorbid Medical Conditions in Friedreich Ataxia

Author

Christopher M. Gomez, David A. Lynch, Jennifer Farmer, Grace Yoon, Martin B. Delatycki, Cassandra J Strawser, Chad Hoyle, Alicia Brocht, S. H. Subramony, Theresa A. Zesiewicz, Julianna E. Shinnick, Susan Perlman, Katherine D. Mathews, Kimberly Schadt, George Wilmot, Nicholas S. Wilcox, and Eppie M. Yiu

Subjects
Adult, congenital, hereditary, and neonatal diseases and abnormalities, Pediatrics, medicine.medical_specialty, Pathology, Ataxia, Adolescent, Population, Comorbidity, Disease, 030204 cardiovascular system & hematology, Cohort Studies, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Degenerative disease, Prevalence, medicine, Humans, Child, education, education.field_of_study, business.industry, nutritional and metabolic diseases, Inflammatory Bowel Diseases, medicine.disease, nervous system diseases, Friedreich Ataxia, Child, Preschool, Growth Hormone, Pediatrics, Perinatology and Child Health, Cohort, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery, Natural history study, Cohort study
Abstract

Friedreich ataxia is a progressive degenerative disease with neurologic and cardiac involvement. This study characterizes comorbid medical conditions in a large cohort of patients with Friedreich ataxia. Patient diagnoses were collected in a large natural history study of 641 subjects. Prevalence of diagnoses in the cohort with Friedreich ataxia was compared with prevalence in the population without Friedreich ataxia. Ten patients (1.6%) had inflammatory bowel disease, 3.5 times more common in this cohort of individuals with Friedreich ataxia than in the general population. Four subjects were growth hormone deficient, reflecting a prevalence in Friedreich ataxia that is 28 times greater than the general population. The present study identifies specific diagnoses not traditionally associated with Friedreich ataxia that are found at higher frequency in this disease. These associations could represent coincidence, shared genetic background, or potentially interactive disease mechanisms with Friedreich ataxia.

Published
2016

5. Longitudinal analysis of contrast acuity in Friedreich ataxia

Author

Tetsuo Ashizawa, Susan Perlman, George Wilmot, Ali G. Hamedani, Alicia Brocht, Martin B. Delatycki, Katherine D. Mathews, S. H. Subramony, Lauren A. Hauser, David A. Lynch, and Theresa A. Zesiewicz

Subjects
medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Future studies, Ataxia, Visual acuity, media_common.quotation_subject, Article, 03 medical and health sciences, 0302 clinical medicine, Ophthalmology, Linear regression, Medicine, Contrast (vision), Genetics (clinical), media_common, business.industry, Surrogate endpoint, Outcome measures, nutritional and metabolic diseases, Confidence interval, 030221 ophthalmology & optometry, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery
Abstract

ObjectiveTo determine the natural history of contrast acuity in Friedreich ataxia.MethodsIn the Friedreich Ataxia–Clinical Outcome Measures Study, participants (n = 764) underwent binocular high- and low-contrast visual acuity testing at annual study visits. Mixed-effects linear regression was used to model visual acuity as a function of time, with random intercepts and slopes to account for intraindividual correlation of repeated measurements. A time-varying covariate was used to adjust for diabetes, and interaction terms were used to assess for effect modification by GAA repeat length, disease duration, and other variables.ResultsAcross a median of 4.4 years of follow-up, visual acuity decreased significantly at 100% contrast (−0.37 letters/y, 95% confidence interval [CI]: −0.52 to −0.21), 2.5% contrast (−0.81 letters/year, 95% CI: −0.99 to −0.65), and 1.25% contrast (−1.12 letters/y, 95% CI: −1.29 to −0.96 letters/year). There was a significant interaction between time and GAA repeat length such that the rate of decrease in visual acuity was greater for patients with higher GAA repeat lengths at 2.5% contrast (p = 0.018) and 1.25% contrast (p = 0.043) but not 100% contrast. There was no effect modification by age at onset after adjusting for GAA repeat length.ConclusionsLow-contrast visual acuity decreases linearly over time in Friedreich ataxia, and the rate of decrease is greater at higher GAA repeat lengths. Contrast sensitivity has the potential to serve as a biomarker and surrogate outcome in future studies of Friedreich ataxia.

Published
2018

6. 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

7. Self-reported adherence versus pill count in Parkinson's disease: The NET-PD experience

Author

Chris Weaver, Patricia Deppen, Cornelia Kamp, Paulo Guimaraes, Barbara C. Tilley, Debbie Fraser, Alicia Brocht, Susan Bennett, and Jordan J. Elm

Subjects
medicine.medical_specialty, Parkinson's disease, Study drug, Pill count, business.industry, Treatment adherence, Reproducibility of Results, Phases of clinical research, Parkinson Disease, Disease, Middle Aged, medicine.disease, Antiparkinson Agents, Clinical trial, Neurology, Predictive Value of Tests, Surveys and Questionnaires, Pill, Physical therapy, Humans, Patient Compliance, Medicine, Neurology (clinical), business
Abstract

Purpose To compare the Morisky medication adherence questionnaire to pill counts as measures of adherence in the NET-PD futility clinical trials. Background: Like in other chronic diseases, non-adherence with medications occurs in Parkinson's disease (PD), although nonadherence has not been of significant concern in most PD clinical trials. The most common approach to assessment is to do a pill count at each visit. The simple, 4-question Morisky medication adherence questionnaire may provide an alternative approach to monitoring treatment adherence in PD. Methods Adherence data from two NET-PD Phase II clinical trials enrolling a total of 413 participants were analyzed. The association between demographic and clinical characteristics and adherence was explored. Results Ninety-percent of participants took 80% or more of the study drug. However, the Morisky medication adherence questionnaires showed 56% report high and 44% report medium adherence. Agreement between the two measures is fair (ICC = 0.40). Conclusions Overall adherence as assessed by pill count appears high. The Morisky medication adherence questionnaire may be useful in PD clinical trials, since it is moderately correlated to pill count and may be more sensitive to nonadherence. © 2007 Movement Disorder Society

Published
2007

8. Depressed mood and suicidality in individuals exposed to tetrabenazine in a large Huntington disease observational study

Author

Alicia Brocht, Paige Nichols, E. Ray Dorsey, Kevin M. Biglan, Kristin C. Darwin, Sonal Singh, Ira Shoulson, Christopher A. Beck, and Karen E. Anderson

Subjects
Adult, Male, medicine.medical_specialty, Tetrabenazine, Suicidal Ideation, Cellular and Molecular Neuroscience, Huntington's disease, medicine, Humans, Psychiatry, Prospective cohort study, Suicidal ideation, Depression (differential diagnoses), Adrenergic Uptake Inhibitors, business.industry, Depression, Hazard ratio, Chorea, Middle Aged, medicine.disease, Huntington Disease, Cohort, Female, Neurology (clinical), medicine.symptom, business, medicine.drug
Abstract

Background Tetrabenazine, a treatment for chorea in Huntington disease, carries a boxed warning due to safety, especially related to suicidality. Objective To compare the frequency of depressed mood and suicidality among a closely monitored cohort of individuals with Huntington disease who were exposed and not exposed to tetrabenazine. Methods A longitudinal prospective study involving 1360 individuals with HD evaluated at 48 research centers in Australia, Canada, and the United States was examined for frequency of depressed mood that triggered a risk assessment, suicidal thoughts, suicide attempts, and completed suicide among individuals with prior, new, and no exposure to tetrabenazine.. Seventy-seven individuals were on tetrabenazine at study enrollment (prior exposure), 64 individuals were exposed to tetrabenazine during the study's course (new exposure), and 1219 individuals had no exposure to tetrabenazine. Results The hazard ratio for depressed mood among those with prior exposure to tetrabenazine compared to no exposure was 0.9 (95% CI, 0.5-1.6) and for those with new exposure compared to no exposure was 1.2 (95% CI, 0.8-1.9). One individual (1.3%) with prior exposure, one individual (1.6%) with new exposure, and 35 individuals (2.9%) with no exposure to tetrabenazine reported suicidal thoughts. The hazard ratio for suicidal ideation among those with prior exposure to tetrabenazine compared to no exposure was 0.5 (95% CI, 0.1-3.8) and for those with new exposure to tetrabenazine compared to no exposure was 0.6 (95% CI, 0.1-4.4). Among individuals with prior or new exposure to tetrabenazine, no suicide attempts or suicides occurred. Among those with no exposure to tetrabenazine 17 suicide attempts (1.4%) and four suicides (0.3%) occurred. Conclusions In a large observational study with close clinical supervision, tetrabenazine treatment was not associated with an increased risk of depressed mood, suicidal ideation, suicide attempts, or suicide.

Published
2014

9. Inosine to increase serum and cerebrospinal fluid urate in Parkinson disease: a randomized clinical trial

Author

Alberto Ascherio, Elmyra Encarnacion, Cathi-Ann Thomas, Doozie Russell, Marsha Tennis, Grace Bwala, Jayaraman Rao, Charlise Hope-Porche, Albert Y. Hung, Saloni Sharma, Maureen Gartner, Eric A. Macklin, Joshua M. Hare, Constance Orme, Candace Cotto, Stuart Isaacson, Sheila Thurlow, Lauren McClurg, Marie Saint-Hilaire, Lisa Niles, Tori Ross, Lisbeth Carvajal, Megan Murray, Joseph Weber, M. Flint Beal, Robert Logan, Alicia Brocht, Michael A. Schwarzschild, Richard Lenehan, David Oakes, Sotirios A. Parashos, Ken Eaton, David S. Russell, Merit Cudkowicz, D. Craig Hooper, Christopher G. Goetz, Ira Shoulson, Alberto J. Espay, Karl Kieburtz, Daniel M. Togasaki, Gina Barles, Daniela L. Grasso, John L. Goudreau, Alice Rudolph, Jeana Jaglin, Patricia Ede, Gary C. Curhan, Maureen Cook, Joseph H. Friedman, Richard Castillo, Lisa Gauger, Radu Constantinescu, Charles S. Venuto, Mark Stacy, Anwar Ahmed, Julia H R Johnson, Julie H. Carter, Melissa Ainslie, Raymond C. James, and J. Antonelle de Marcaida

Subjects
Male, medicine.medical_specialty, Placebo, Article, law.invention, chemistry.chemical_compound, Randomized controlled trial, Double-Blind Method, law, Internal medicine, Epidemiology, medicine, Humans, Adverse effect, Inosine, Aged, business.industry, Parkinson Disease, Middle Aged, medicine.disease, Gout, Surgery, Uric Acid, Treatment Outcome, Tolerability, chemistry, Uric acid, Female, Neurology (clinical), business, Biomarkers, medicine.drug, Follow-Up Studies
Abstract

Convergent biological, epidemiological, and clinical data identified urate elevation as a candidate strategy for slowing disability progression in Parkinson disease (PD).To determine the safety, tolerability, and urate-elevating capability of the urate precursor inosine in early PD and to assess its suitability and potential design features for a disease-modification trial.The Safety of Urate Elevation in PD (SURE-PD) study, a randomized, double-blind, placebo-controlled, dose-ranging trial of inosine, enrolled participants from 2009 to 2011 and followed them for up to 25 months at outpatient visits to 17 credentialed clinical study sites of the Parkinson Study Group across the United States. Seventy-five consenting adults (mean age, 62 years; 55% women) with early PD not yet requiring symptomatic treatment and a serum urate concentration less than 6 mg/dL (the approximate population median) were enrolled.Participants were randomized to 1 of 3 treatment arms: placebo or inosine titrated to produce mild (6.1-7.0 mg/dL) or moderate (7.1-8.0 mg/dL) serum urate elevation using 500-mg capsules taken orally up to 2 capsules 3 times per day. They were followed for up to 24 months (median, 18 months) while receiving the study drug plus 1 washout month.The prespecified primary outcomes were absence of unacceptable serious adverse events (safety), continued treatment without adverse event requiring dose reduction (tolerability), and elevation of urate assessed serially in serum and once (at 3 months) in cerebrospinal fluid. RESULTS Serious adverse events (17), including infrequent cardiovascular events, occurred at the same or lower rates in the inosine groups relative to placebo. No participant developed gout and 3 receiving inosine developed symptomatic urolithiasis. Treatment was tolerated by 95% of participants at 6 months, and no participant withdrew because of an adverse event. Serum urate rose by 2.3 and 3.0 mg/dL in the 2 inosine groups (P .001 for each) vs placebo, and cerebrospinal fluid urate level was greater in both inosine groups (P = .006 and.001, respectively). Secondary analyses demonstrated nonfutility of inosine treatment for slowing disability.Inosine was generally safe, tolerable, and effective in raising serum and cerebrospinal fluid urate levels in early PD. The findings support advancing to more definitive development of inosine as a potential disease-modifying therapy for PD.clinicaltrials.gov Identifier: NCT00833690.

Published
2013

10. Use of Tetrabenazine in Huntington Disease Patients on Antidepressants or with Advanced Disease: Results from the TETRA-HD Study

Author

Kathleen Clarence-Smith, David Oakes, Ray Dorsey, Shirley Eberly, Kevin M. Biglan, Alicia Brocht, Samuel Frank, Frederick J. Marshall, Chizoba C. Umeh, Ira Shoulson, and Peggy Auinger

Subjects
medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, business.industry, Tetrabenazine, Incidence (epidemiology), Medicine (miscellaneous), Chorea, Disease, Huntington Disease, Internal medicine, mental disorders, medicine, Advanced disease, Antidepressant, medicine.symptom, business, Depressed mood, Psychiatry, medicine.drug
Abstract

The safety and effectiveness of tetrabenazine in different sub-populations of Huntington disease (HD) is not known. In this study, we evaluated the safety of tetrabenazine in individuals on an antidepressant and its effectiveness in advanced HD. Tetrabenazine was not associated with an increased incidence of depressed mood among those taking antidepressants and was effective at reducing chorea in those with advanced HD.

Published
2011

11. Pramipexole in levodopa-treated Parkinson disease patients of African, Asian, and Hispanic heritage

Author

Mickie Welsh, Daniel Truong, Rajesh Pahwa, K. Ligon, Cynthia L. Comella, Kenneth Marek, William C. Koller, Kimberly Janko, Brenda Pfeiffer, Andrea Freimuth, Sara Rast, Lori McGee-Minnich, An Hao Tran, Cheryl H. Waters, Karl Kieburtz, Kapil D. Sethi, Howard I. Hurtig, Cindy Casaceli, Sheila Everett, Ronald F. Pfeiffer, C.D. Wood, Carmen Serrano Ramos, Sam Goldman, Jayaraman Rao, Andrew Feigin, Marian L. Evatt, Arthur Watts, Carolyn C. Weeks, Richard Trosch, David Oakes, Giselle Petzinger, Caroline M. Tanner, Janet S. Cellar, Julie H. Carter, Cornelia Kamp, Kathleen M. Shannon, Denni Day, Kathie Mistura, Susan Broshjeit, Clare Das, George W. Paulson, Adelma Rivera Cruz, Alicia Brocht, Karen Hodgeman, Carson Reider, Frederick J. Marshall, Karen Thompson, Mary Matthews, Ira Shoulson, Mariella Fernandez, Joel S. Perlmutter, Lisa M. Shulman, and Dinorah Rodriguez

Subjects
Cross-Cultural Comparison, Male, medicine.medical_specialty, Levodopa, Time Factors, Disease, Severity of Illness Index, law.invention, Antiparkinson Agents, Pramipexole, Randomized controlled trial, Double-Blind Method, law, Internal medicine, Medicine, Humans, Pharmacology (medical), Benzothiazoles, Aged, Retrospective Studies, Pharmacology, African american, Asian, business.industry, Parkinson Disease, Hispanic or Latino, Middle Aged, Black or African American, Treatment Outcome, Physical therapy, Female, Neurology (clinical), business, medicine.drug
Abstract

Little is known regarding the effects of antiparkinsonian drugs in US racial or ethnic minorities.: To evaluate the safety, tolerability, and efficacy of adjunctive pramipexole in Parkinson disease (PD) patients of African, Asian, or Hispanic heritage stably treated with levodopa.Multicenter, parallel-group, double-blind, randomized, placebo-controlled trial.: Seventeen Parkinson Study Group sites in the United States and Puerto Rico.One hundred forty-four PD patients of African, Asian, or Hispanic heritage enrolled from January 1997 to August 1998 and observed until October 1998.Subjects received pramipexole or placebo (3:1 ratio), 0.375 mg/d to a maximum tolerated dose (or=4.5 mg/d) over a 6-week period, achieving optimum levels (0.375, 1.5, 3.0, or 4.5 mg/d) in the 4-week maintenance period.Change in the sum of the Unified Parkinson's Disease Rating Scale parts 2 (activities of daily living) and 3 (motor) from baseline to week 10.Parkinsonism improved (mean [SD] reduction in Unified Parkinson's Disease Rating Scale activities of daily living + motor score at 10 weeks, 10.27 [11.96] pramipexole vs 6.54 [13.58] placebo, P = 0.012) and was similar in each group. Adverse events occurred in 85.3% on pramipexole and 68.6% on placebo. Hallucinations and insomnia were more common on pramipexole than placebo (18 vs 0, P = 0.023, and 15 vs 0, P = 0.045, respectively).Pramipexole is an effective adjunctive antiparkinsonian therapy in PD patients of African, Asian, and Hispanic heritage. Tolerability and safety overall were similar among the groups, but differences in profiles of adverse effects and tolerability were suggested.

Published
2007

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