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1. Creatine and glutamine therapeutic trial in Duchenne muscular dystrophy (DMD) by the Cooperative International Neuromuscular Research Group (CINRG)

Author

Escolar, Dm, Buyse, G, Henricson, E, Leshner, R, Florence, J, Mayhew, J, Tesi Rocha, C, Gorni, K, Pasquali, Livia, Patel, Km, Mccarter, R, Huang, J, Mayhew, T, Bertorini, T, Carlo, J, Connolly, Am, Clemens, Pr, Goemans, N, Iannaccone, St, Igarashi, M, Nevo, Y, Pestronk, A, Subramony, Sh, Vedanarayanan, Vv, Wessel, H, and Cinrg, Group

Published
2003

10. Cobomarsen, an Oligonucleotide Inhibitor of miR-155, Slows DLBCL Tumor Cell Growth In Vitro and In Vivo .

Author

Anastasiadou E, Seto AG, Beatty X, Hermreck M, Gilles ME, Stroopinsky D, Pinter-Brown LC, Pestano L, Marchese C, Avigan D, Trivedi P, Escolar DM, Jackson AL, and Slack FJ

Subjects
Animals, Apoptosis drug effects, Apoptosis genetics, Cell Line, Tumor, Cell Proliferation drug effects, Cell Proliferation genetics, Female, Gene Expression Regulation, Neoplastic drug effects, Humans, Lymphoma, Large B-Cell, Diffuse genetics, Lymphoma, Large B-Cell, Diffuse pathology, Mice, MicroRNAs metabolism, Oligonucleotides therapeutic use, Oligonucleotides, Antisense therapeutic use, Xenograft Model Antitumor Assays, Lymphoma, Large B-Cell, Diffuse drug therapy, MicroRNAs antagonists & inhibitors, Oligonucleotides pharmacology, Oligonucleotides, Antisense pharmacology
Abstract

Purpose: miRNA-155 is an oncogenic miRNA highly expressed in B-cell malignancies, particularly in the non-germinal center B-cell or activated B-cell subtype of diffuse large B-cell lymphoma (ABC-DLBCL), where it is considered a potential diagnostic and prognostic biomarker. Thus, miR-155 inhibition represents an important therapeutic strategy for B-cell lymphomas. In this study, we tested the efficacy and pharmacodynamic activity of an oligonucleotide inhibitor of miR-155, cobomarsen, in ABC-DLBCL cell lines and in corresponding xenograft mouse models. In addition, we assessed the therapeutic efficacy and safety of cobomarsen in a patient diagnosed with aggressive ABC-DLBCL., Experimental Design: Preclinical studies included the delivery of cobomarsen to highly miR-155-expressing ABC-DLBCL cell lines to assess any phenotypic changes, as well as intravenous injections of cobomarsen in NSG mice carrying ABC-DLBCL xenografts, to study tumor growth and pharmacodynamics of the compound over time. To begin to test its safety and therapeutic efficacy, a patient was recruited who underwent five cycles of cobomarsen treatment., Results: Cobomarsen decreased cell proliferation and induced apoptosis in ABC-DLBCL cell lines. Intravenous administration of cobomarsen in a xenograft NSG mouse model of ABC-DLBCL reduced tumor volume, triggered apoptosis, and derepressed direct miR-155 target genes. Finally, the compound reduced and stabilized tumor growth without any toxic effects for the patient., Conclusions: Our findings support the potential therapeutic application of cobomarsen in ABC-DLBCL and other types of lymphoma with elevated miR-155 expression., (©2020 American Association for Cancer Research.)

Published
2021
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11. Barriers and facilitators to clinical trial participation among parents of children with pediatric neuromuscular disorders.

Author

Peay HL, Biesecker BB, Wilfond BS, Jarecki J, Umstead KL, Escolar DM, and Tibben A

Subjects
Child, Communication Barriers, Female, Health Knowledge, Attitudes, Practice, Humans, Logistic Models, Male, Professional-Family Relations, Surveys and Questionnaires, Muscular Dystrophy, Duchenne, Parents psychology, Patient Selection, Randomized Controlled Trials as Topic psychology, Spinal Muscular Atrophies of Childhood
Abstract

Background/aims: Pediatric rare disease presents a challenging situation of high unmet need and a limited pool of potential clinical trial participants. Understanding perspectives of parents of children who have not participated in trials may facilitate approaches to optimize participation rates. The objective of this study was to explore factors associated with parental interest in enrolling children with pediatric neuromuscular disorders in clinical trials., Methods: Parents of individuals with Duchenne or Becker muscular dystrophy and spinal muscular atrophy were recruited through advocacy organizations, a registry, and clinics. These parents ( N = 203) completed a questionnaire including assessments of barriers and facilitators to clinical trial participation, parents' interest in trial participation, and their perceptions of others' views about participation in a clinical trial., Results: Trial interest in participating parents was high (64% combined group). The most highly endorsed barrier to participation was the possibility of receiving placebo, followed by not having enough information on risks and trial procedures. Compared to parents of children with Duchenne or Becker muscular dystrophy, parents of children with spinal muscular atrophy endorsed significantly more information and knowledge barriers. The greatest facilitators of participation were (1) confidence in improving disease understanding and (2) guarantee to receive the treatment after a successful trial. A logistic regression model, χ 2 (4, n = 188) = 80.64, p < .001, indicated that higher perceived barriers and more frequent trial communication by the provider were associated with lower interest, while positive trial perceptions by the child's providers and concordance in trial perceptions among those close to the decision-maker were associated with higher interest., Conclusion: We found high parental interest in pediatric neuromuscular trials that was tempered by concerns about the potential for randomization to a placebo arm. Participants perceived that their trial participation would be facilitated by additional education and guidance from their clinicians. Yet, intentions were negatively associated with frequency of provider communication, perhaps reflecting waning parental interest with a greater understanding of limitations in trial access, increased sophistication in their understanding of trial design, and appreciation of potential burden. To support parents' informed decisions, it is important to educate them to evaluate the quality of research, as well as providing lay information explaining the use of placebo, trial processes, and potential barriers to long-term drug access. Our findings should inform the development of targeted educational content, clinician training, and decision support tools.

Published
2018
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12. The cooperative international neuromuscular research group Duchenne natural history study: glucocorticoid treatment preserves clinically meaningful functional milestones and reduces rate of disease progression as measured by manual muscle testing and other commonly used clinical trial outcome measures.

Author

Henricson EK, Abresch RT, Cnaan A, Hu F, Duong T, Arrieta A, Han J, Escolar DM, Florence JM, Clemens PR, Hoffman EP, and McDonald CM

Subjects
Adolescent, Adult, Biomedical Research methods, Biomedical Research standards, Child, Child, Preschool, Clinical Trials as Topic methods, Clinical Trials as Topic standards, Cohort Studies, Cross-Sectional Studies, Humans, Longitudinal Studies, Male, Muscle Strength physiology, Muscular Dystrophy, Duchenne diagnosis, Muscular Dystrophy, Duchenne epidemiology, Outcome Assessment, Health Care standards, Prospective Studies, Treatment Outcome, Young Adult, Diagnostic Techniques, Neurological standards, Disease Progression, Glucocorticoids therapeutic use, International Cooperation, Muscular Dystrophy, Duchenne drug therapy, Outcome Assessment, Health Care methods
Abstract

Unlabelled: introduction: Glucocorticoid (GC) therapy in Duchenne muscular dystrophy (DMD) has altered disease progression, necessitating contemporary natural history studies., Methods: The Cooperative Neuromuscular Research Group (CINRG) DMD Natural History Study (DMD-NHS) enrolled 340 DMD males, ages 2-28 years. A comprehensive battery of measures was obtained., Results: A novel composite functional "milestone" scale scale showed clinically meaningful mobility and upper limb abilities were significantly preserved in GC-treated adolescents/young adults. Manual muscle test (MMT)-based calculations of global strength showed that those patients <10 years of age treated with steroids declined by 0.4 ± 0.39 MMT unit/year, compared with -0.4 ± 0.39 MMT unit/year in historical steroid-naive subjects. Pulmonary function tests (PFTs) were relatively preserved in steroid-treated adolescents. The linearity and magnitude of decline in measures were affected by maturational changes and functional status., Conclusions: In DMD, long-term use of GCs showed reduced strength loss and preserved functional capabilities and PFTs compared with previous natural history studies performed prior to the widespread use of GC therapy., (Copyright © 2013 Wiley Periodicals, Inc.)

Published
2013
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13. The cooperative international neuromuscular research group Duchenne natural history study--a longitudinal investigation in the era of glucocorticoid therapy: design of protocol and the methods used.

Author

McDonald CM, Henricson EK, Abresch RT, Han JJ, Escolar DM, Florence JM, Duong T, Arrieta A, Clemens PR, Hoffman EP, and Cnaan A

Subjects
Adolescent, Adult, Child, Child, Preschool, Humans, Internationality, Longitudinal Studies, Male, Prospective Studies, Young Adult, Glucocorticoids therapeutic use, International Cooperation, Muscular Dystrophy, Duchenne drug therapy, Muscular Dystrophy, Duchenne epidemiology, Research Design
Abstract

Unlabelled: Contemporary natural history data in Duchenne muscular dystrophy (DMD) is needed to assess care recommendations and aid in planning future trials., Methods: The Cooperative International Neuromuscular Research Group (CINRG) DMD Natural History Study (DMD-NHS) enrolled 340 individuals, aged 2-28 years, with DMD in a longitudinal, observational study at 20 centers. Assessments obtained every 3 months for 1 year, at 18 months, and annually thereafter included: clinical history; anthropometrics; goniometry; manual muscle testing; quantitative muscle strength; timed function tests; pulmonary function; and patient-reported outcomes/health-related quality-of-life instruments., Results: Glucocorticoid (GC) use at baseline was 62% present, 14% past, and 24% GC-naive. In those ≥6 years of age, 16% lost ambulation over the first 12 months (mean age 10.8 years)., Conclusions: Detailed information on the study methodology of the CINRG DMD-NHS lays the groundwork for future analyses of prospective longitudinal natural history data. These data will assist investigators in designing clinical trials of novel therapeutics., (Copyright © 2013 Wiley Periodicals, Inc.)

Published
2013
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14. Liquid formulation of pentoxifylline is a poorly tolerated treatment for duchenne dystrophy.

Author

Zimmerman A, Clemens PR, Tesi-Rocha C, Connolly A, Iannaccone ST, Kuntz N, Arrieta A, Hache L, Henricson E, Hu F, Mayhew J, and Escolar DM

Subjects
Administration, Oral, Child, Child, Preschool, Gastrointestinal Diseases chemically induced, Humans, Leukopenia chemically induced, Male, Muscle Strength drug effects, Pentoxifylline administration & dosage, Pentoxifylline adverse effects, Pilot Projects, Treatment Outcome, Muscular Dystrophy, Duchenne drug therapy, Pentoxifylline therapeutic use
Abstract

Introduction: In this study we performed an open-label, pilot study of an orally administered liquid formulation of immediate-release pentoxifylline (PTX) on patients with Duchenne muscular dystrophy (DMD). Treatment efficacy, safety, and tolerability were assessed., Methods: The tolerability and safety of PTX and measures of muscle strength and function were evaluated during 12 months of treatment., Results: Seventeen boys with DMD, between 4 and 8 years of age, were enrolled at one of five Cooperative International Neuromuscular Research Group (CINRG) centers. Only 9 were able to complete the 12-month PTX treatment phase; the primary reason for discontinuation was adverse events. Intolerable gastrointestinal side effects were experienced by 65% of participants. Two participants had severe leukopenia that resolved with medication withdrawal., Conclusions: Open-label treatment with a liquid formulation of immediate-release PTX resulted in a high incidence of adverse events in boys with DMD. Poor tolerability of this PTX formulation precluded adequate assessment of efficacy., (Copyright © 2011 Wiley Periodicals, Inc.)

Published
2011
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15. CINRG pilot trial of coenzyme Q10 in steroid-treated Duchenne muscular dystrophy.

Author

Spurney CF, Rocha CT, Henricson E, Florence J, Mayhew J, Gorni K, Pasquali L, Pestronk A, Martin GR, Hu F, Nie L, Connolly AM, and Escolar DM

Subjects
Child, Child, Preschool, Disease Progression, Drug Therapy, Combination, Female, Humans, Male, Muscle Strength drug effects, Pilot Projects, Prospective Studies, Treatment Outcome, Ubiquinone administration & dosage, Ubiquinone therapeutic use, Adrenal Cortex Hormones therapeutic use, Muscular Dystrophy, Duchenne drug therapy, Ubiquinone analogs & derivatives, Vitamins therapeutic use
Abstract

Introduction: Corticosteroid treatment slows disease progression and is the standard of care for Duchenne muscular dystrophy (DMD). Coenzyme Q10 (CoQ10) is a potent antioxidant that may improve function in dystrophin-deficient muscle., Methods: We performed an open-label, "add-on" pilot study of CoQ10 in thirteen 5-10-year-old DMD patients on steroids. The primary outcome measure was the total quantitative muscle testing (QMT) score., Results: Twelve of 16 children (mean age 8.03 ± 1.64 years) completed the trial. Target serum levels of CoQ10 (≥2.5 μg/ml) were shown to be subject- and administration-dependent. Nine of 12 subjects showed an increase in total QMT score. Overall, CoQ10 treatment resulted in an 8.5% increase in muscle strength (P = 0.03)., Conclusions: Addition of CoQ10 to prednisone therapy in DMD patients resulted in an increase in muscle strength. These results warrant a larger, controlled trial of CoQ10 in DMD., (Copyright © 2011 Wiley Periodicals, Inc.)

Published
2011
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16. Congenital muscular dystrophies.

Author

Sparks SE and Escolar DM

Subjects
Humans, Muscular Dystrophies congenital, Muscular Dystrophies genetics
Abstract

Congenital muscular dystrophies (CMDs) are a heterogeneous group of disorders characterized by muscle weakness from birth, or shortly after, and variable clinical manifestations of the eye and central nervous system. Some of these disorders are fatal in the first years of life, whereas others have a milder course, with survival into adulthood. The CMDs were initially classified by clinical features and country of origin; however, with new molecular techniques it is now possible to classify these patients better. More than 10 genes have been identified to date that cause forms of CMD. However, even with current molecular diagnostic techniques, only approximately 25-50% of patients with CMD have an identifiable genetic mutation. In addition, some phenotypic classifications have been attempted. There is significant overlap between the phenotypic and molecular classifications, making diagnosis within this heterogeneous group of disorders difficult., (Copyright © 2011 Elsevier B.V. All rights reserved.)

Published
2011
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17. Functional and molecular effects of arginine butyrate and prednisone on muscle and heart in the mdx mouse model of Duchenne Muscular Dystrophy.

Author

Guerron AD, Rawat R, Sali A, Spurney CF, Pistilli E, Cha HJ, Pandey GS, Gernapudi R, Francia D, Farajian V, Escolar DM, Bossi L, Becker M, Zerr P, de la Porte S, Gordish-Dressman H, Partridge T, Hoffman EP, and Nagaraju K

Subjects
Animals, Arginine pharmacology, Arginine therapeutic use, Behavior, Animal drug effects, Butyrates therapeutic use, Disease Models, Animal, Drug Therapy, Combination, Female, Gene Expression Profiling, Gene Expression Regulation drug effects, Mice, Mice, Inbred mdx, Muscles metabolism, Muscles pathology, Muscles physiopathology, Muscular Dystrophy, Duchenne drug therapy, Muscular Dystrophy, Duchenne pathology, Prednisone therapeutic use, RNA, Messenger genetics, RNA, Messenger metabolism, Time Factors, Utrophin metabolism, Arginine analogs & derivatives, Butyrates pharmacology, Heart drug effects, Heart physiopathology, Muscles drug effects, Muscular Dystrophy, Duchenne metabolism, Muscular Dystrophy, Duchenne physiopathology, Prednisone pharmacology
Abstract

Background: The number of promising therapeutic interventions for Duchenne Muscular Dystrophy (DMD) is increasing rapidly. One of the proposed strategies is to use drugs that are known to act by multiple different mechanisms including inducing of homologous fetal form of adult genes, for example utrophin in place of dystrophin., Methodology/principal Findings: In this study, we have treated mdx mice with arginine butyrate, prednisone, or a combination of arginine butyrate and prednisone for 6 months, beginning at 3 months of age, and have comprehensively evaluated the functional, biochemical, histological, and molecular effects of the treatments in this DMD model. Arginine butyrate treatment improved grip strength and decreased fibrosis in the gastrocnemius muscle, but did not produce significant improvement in muscle and cardiac histology, heart function, behavioral measurements, or serum creatine kinase levels. In contrast, 6 months of chronic continuous prednisone treatment resulted in deterioration in functional, histological, and biochemical measures. Arginine butyrate-treated mice gene expression profiling experiments revealed that several genes that control cell proliferation, growth and differentiation are differentially expressed consistent with its histone deacetylase inhibitory activity when compared to control (saline-treated) mdx mice. Prednisone and combination treated groups showed alterations in the expression of genes that control fibrosis, inflammation, myogenesis and atrophy., Conclusions/significance: These data indicate that 6 months treatment with arginine butyrate can produce modest beneficial effects on dystrophic pathology in mdx mice by reducing fibrosis and promoting muscle function while chronic continuous treatment with prednisone showed deleterious effects to skeletal and cardiac muscle. Our results clearly indicate the usefulness of multiple assays systems to monitor both beneficial and toxic effects of drugs with broad range of in vivo activity.

Published
2010
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18. A randomized study of alglucosidase alfa in late-onset Pompe's disease.

Author

van der Ploeg AT, Clemens PR, Corzo D, Escolar DM, Florence J, Groeneveld GJ, Herson S, Kishnani PS, Laforet P, Lake SL, Lange DJ, Leshner RT, Mayhew JE, Morgan C, Nozaki K, Park DJ, Pestronk A, Rosenbloom B, Skrinar A, van Capelle CI, van der Beek NA, Wasserstein M, and Zivkovic SA

Subjects
Adolescent, Adult, Age of Onset, Aged, Analysis of Variance, Child, Drug Hypersensitivity etiology, Female, Glycogen Storage Disease Type II physiopathology, Humans, Immunoglobulin G blood, Infusions, Intravenous, Male, Middle Aged, Vital Capacity drug effects, Walking, Young Adult, alpha-Glucosidases adverse effects, alpha-Glucosidases immunology, Glycogen Storage Disease Type II drug therapy, alpha-Glucosidases therapeutic use
Abstract

Background: Pompe's disease is a metabolic myopathy caused by a deficiency of acid alpha glucosidase (GAA), an enzyme that degrades lysosomal glycogen. Late-onset Pompe's disease is characterized by progressive muscle weakness and loss of respiratory function, leading to early death. We conducted a randomized, placebo-controlled trial of alglucosidase alfa, a recombinant human GAA, for the treatment of late-onset Pompe's disease., Methods: Ninety patients who were 8 years of age or older, ambulatory, and free of invasive ventilation were randomly assigned to receive biweekly intravenous alglucosidase alfa (20 mg per kilogram of body weight) or placebo for 78 weeks at eight centers in the United States and Europe. The two primary end points were distance walked during a 6-minute walk test and percentage of predicted forced vital capacity (FVC)., Results: At 78 weeks, the estimated mean changes from baseline in the primary end points favored alglucosidase alfa (an increase of 28.1+/-13.1 m on the 6-minute walk test and an absolute increase of 3.4+/-1.2 percentage points in FVC; P=0.03 and P=0.006, respectively). Similar proportions of patients in the two groups had adverse events, serious adverse events, and infusion-associated reactions; events that occurred only in patients who received the active study drug included anaphylactic reactions and infusion-associated reactions of urticaria, flushing, hyperhidrosis, chest discomfort, vomiting, and increased blood pressure (each of which occurred in 5 to 8% of the patients)., Conclusions: In this study population, treatment with alglucosidase alfa was associated with improved walking distance and stabilization of pulmonary function over an 18-month period. (ClinicalTrials.gov number, NCT00158600.), (Massachusetts Medical Society)

Published
2010
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19. Clinical features of late-onset Pompe disease: a prospective cohort study.

Author

Wokke JH, Escolar DM, Pestronk A, Jaffe KM, Carter GT, van den Berg LH, Florence JM, Mayhew J, Skrinar A, Corzo D, and Laforet P

Subjects
Adult, Age of Onset, Aged, Biomarkers analysis, Chronic Disease therapy, Cohort Studies, Disability Evaluation, Disease Progression, Female, Gait Disorders, Neurologic diagnosis, Gait Disorders, Neurologic physiopathology, Humans, Male, Middle Aged, Muscle Weakness etiology, Muscle, Skeletal physiopathology, Predictive Value of Tests, Prospective Studies, Respiratory Muscles physiopathology, Severity of Illness Index, Glycogen Storage Disease Type II diagnosis, Glycogen Storage Disease Type II physiopathology, Muscle Weakness diagnosis, Muscle Weakness physiopathology, Respiratory Paralysis diagnosis, Respiratory Paralysis physiopathology
Abstract

The objective of this 12-month study was to describe the clinical features of late-onset Pompe disease and identify appropriate outcome measures for use in clinical trials. Assessments included quantitative muscle testing (QMT), functional activities (FAA), 6-min walk test (6MWT), and pulmonary function testing (PFT). Percent predicted values indicated quantifiable upper and lower extremity weakness, impaired walking ability, and respiratory muscle weakness. Significant declines in arm and leg strength and pulmonary function were observed during the study period. The outcome measures were demonstrated to be safe and reliable. Symptom duration was identified as the best predictor of the extent of skeletal and respiratory muscle weakness.

Published
2008
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20. A phase I/IItrial of MYO-029 in adult subjects with muscular dystrophy.

Author

Wagner KR, Fleckenstein JL, Amato AA, Barohn RJ, Bushby K, Escolar DM, Flanigan KM, Pestronk A, Tawil R, Wolfe GI, Eagle M, Florence JM, King WM, Pandya S, Straub V, Juneau P, Meyers K, Csimma C, Araujo T, Allen R, Parsons SA, Wozney JM, Lavallie ER, and Mendell JR

Subjects
Adult, Cohort Studies, Comorbidity, Double-Blind Method, Female, Humans, Incidence, Internationality, Male, Placebo Effect, Risk Factors, Treatment Outcome, Antibodies therapeutic use, Drug Eruptions epidemiology, Muscular Dystrophies drug therapy, Muscular Dystrophies epidemiology, Risk Assessment methods
Abstract

Objective: Myostatin is an endogenous negative regulator of muscle growth and a novel target for muscle diseases. We conducted a safety trial of a neutralizing antibody to myostatin, MYO-029, in adult muscular dystrophies (Becker muscular dystrophy, facioscapulohumeral dystrophy, and limb-girdle muscular dystrophy)., Methods: This double-blind, placebo-controlled, multinational, randomized study included 116 subjects divided into sequential dose-escalation cohorts, each receiving MYO-029 or placebo (Cohort 1 at 1 mg/kg; Cohort 2 at 3 mg/kg; Cohort 3 at 10 mg/kg; Cohort 4 at 30 mg/kg). Safety and adverse events were assessed by reported signs and symptoms, as well as by physical examinations, laboratory results, echocardiograms, electrocardiograms, and in subjects with facioscapulohumeral dystrophy, funduscopic and audiometry examinations. Biological activity of MYO-029 was assessed through manual muscle testing, quantitative muscle testing, timed function tests, subject-reported outcomes, magnetic resonance imaging studies, dual-energy radiographic absorptiometry studies, and muscle biopsy., Results: MYO-029 had good safety and tolerability with the exception of cutaneous hypersensitivity at the 10 and 30 mg/kg doses. There were no improvements noted in exploratory end points of muscle strength or function, but the study was not powered to look for efficacy. Importantly, bioactivity of MYO-029 was supported by a trend in a limited number of subjects toward increased muscle size using dual-energy radiographic absorptiometry and muscle histology., Interpretation: This trial supports the hypothesis that systemic administration of myostatin inhibitors provides an adequate safety margin for clinical studies. Further evaluation of more potent myostatin inhibitors for stimulating muscle growth in muscular dystrophy should be considered.

Published
2008
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21. CINRG pilot trial of oxatomide in steroid-naïve Duchenne muscular dystrophy.

Author

Buyse GM, Goemans N, Henricson E, Jara A, van den Hauwe M, Leshner R, Florence JM, Mayhew JE, and Escolar DM

Subjects
Child, Child, Preschool, Female, Follow-Up Studies, Humans, Linear Models, Male, Muscle Strength drug effects, Pilot Projects, Time Factors, Treatment Outcome, Histamine H1 Antagonists therapeutic use, Muscular Dystrophy, Duchenne drug therapy, Piperazines therapeutic use
Abstract

The authors report a pilot open-label two-center therapeutic trial of oxatomide in 14 steroid-naive DMD boys aged 5-10 years. Comparison of linear evolutions between 3 months medication-free lead-in periods and 6 months treatment periods showed no significant differences in quantitative (QMT) and manual (MMT) measurements of muscle strength and timed functional tests. A modest mitigation of strength deterioration over time cannot be excluded.

Published
2007
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22. Challenges in drug development for muscle disease: a stakeholders' meeting.

Author

Mendell JR, Csimma C, McDonald CM, Escolar DM, Janis S, Porter JD, Hesterlee SE, and Howell RR

Subjects
Academic Medical Centers, Animals, Clinical Trials as Topic economics, Drug Approval legislation & jurisprudence, Drug Approval methods, Drug Evaluation legislation & jurisprudence, Drug Evaluation trends, Drug Industry, Humans, Investments, National Institutes of Health (U.S.), Outcome Assessment, Health Care, Research, United States, United States Food and Drug Administration, Clinical Trials as Topic legislation & jurisprudence, Drug Design, Drug Evaluation economics, Muscular Diseases drug therapy, Research Support as Topic legislation & jurisprudence
Abstract

Current treatment benefits for patients with muscle disease are limited, but progress in legislative and scientific initiatives have set the stage for the development of new therapies. The MD-CARE Act (Public Law 107-84), which allocates federal resources to muscular dystrophy, was approved by Congress and signed into law by the President of the United States in 2001. This has shifted the emphasis toward translational research. To facilitate a push toward therapy for muscle disorders, the Muscular Dystrophy Association (MDA) sponsored a meeting with representatives from industry, the Food and Drug Administration (FDA), the National Institutes of Health (NIH), and other government agencies and academia. Each contributed in different ways. The FDA helped define the necessary data to support investigational new drug (IND) applications including the design of proof-of-principle studies, outcome measures for clinical trials, and the pathway for developing surrogate measures for fast-tracking promising new drugs. The NIH, other government agencies, and the MDA described potential funding sources for translational research. Industry delineated a complementary role with academia, and academic investigators elucidated the current strengths and weaknesses of available clinical endpoints. The meeting provided a format for communication for diverse disciplines that usually have no common meeting ground, helping to lay the foundation for bringing products to market in a timely fashion.

Published
2007
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23. Reliable surrogate outcome measures in multicenter clinical trials of Duchenne muscular dystrophy.

Author

Mayhew JE, Florence JM, Mayhew TP, Henricson EK, Leshner RT, McCarter RJ, and Escolar DM

Subjects
Adolescent, Biomarkers, Child, Child, Preschool, Humans, Male, Muscle Weakness diagnosis, Muscle Weakness physiopathology, Muscle, Skeletal physiopathology, Muscular Dystrophy, Duchenne physiopathology, Neurologic Examination methods, Neurologic Examination standards, Observer Variation, Predictive Value of Tests, Reproducibility of Results, Treatment Outcome, Clinical Trials as Topic methods, Disability Evaluation, Muscular Dystrophy, Duchenne diagnosis, Muscular Dystrophy, Duchenne drug therapy, Outcome Assessment, Health Care methods
Abstract

We studied the reliability of a series of endpoints in an evaluation of subjects with Duchenne muscular dystrophy (DMD). The endpoints included quantitative muscle tests (QMTs), timed function tests, forced vital capacity (FVC), and manual muscle tests (MMT). Thirty-one ambulatory subjects with DMD (mean age 8.9 years; range 5-16 years) were evaluated at eight sites by 15 newly trained evaluators as a test of interrater reliability of outcome measures. Both total QMT score [intraclass correlation coefficient (ICC) 0.96] and individual QMT assessments (ICC 0.85-0.96) were highly reliable. Forced vital capacity and all timed function tests were also highly reliable (ICC 0.97-0.99). MMT was the least reliable assessment method (ICC 0.61). These data suggest that primary surrogate outcome measures in large multicenter clinical trials in DMD should use QMT, FVC, or time function tests to obtain maximum power and greatest sensitivity.

Published
2007
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24. Update on diagnosis and treatment of hereditary and acquired polyneuropathies in childhood.

Author

Rocha CT and Escolar DM

Subjects
Child, Child, Preschool, Hereditary Sensory and Motor Neuropathy classification, Hereditary Sensory and Motor Neuropathy genetics, Humans, Polyneuropathies classification, Polyneuropathies genetics, Hereditary Sensory and Motor Neuropathy diagnosis, Hereditary Sensory and Motor Neuropathy therapy, Polyneuropathies diagnosis, Polyneuropathies therapy
Published
2004
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25. Genome-wide homozygosity mapping localizes a gene for autosomal recessive non-progressive infantile ataxia to 20q11-q13.

Author

Tranebjaerg L, Teslovich TM, Jones M, Barmada MM, Fagerheim T, Dahl A, Escolar DM, Trent JM, Gillanders EM, and Stephan DA

Subjects
Adolescent, Adult, Aged, Child, Child, Preschool, Consanguinity, Female, Fluorescent Dyes, Homozygote, Humans, Male, Microsatellite Repeats, Middle Aged, Norway, Pedigree, Ataxia genetics, Chromosome Mapping, Chromosomes, Human, Pair 20 genetics, Genes, Recessive, Lod Score
Abstract

Autosomal recessive ataxias represent genetic and clinical heterogeneity. Unsteady gait is often accompanied by poor coordination of limbs, speech, and eye movements. To date, seven genes have been identified. In addition, five chromosomal loci have been localized in non-related families. Here, we report homozygosity mapping of a novel locus to a 19.5-cM region on chromosome 20q11-q13 in a large inbred Norwegian family with infantile non-progressive ataxia.

Published
2003
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26. PIP2 binding residues of Kir2.1 are common targets of mutations causing Andersen syndrome.

Author

Donaldson MR, Jensen JL, Tristani-Firouzi M, Tawil R, Bendahhou S, Suarez WA, Cobo AM, Poza JJ, Behr E, Wagstaff J, Szepetowski P, Pereira S, Mozaffar T, Escolar DM, Fu YH, and Ptácek LJ

Subjects
Abnormalities, Multiple diagnosis, Abnormalities, Multiple pathology, Arrhythmias, Cardiac diagnosis, Binding Sites, Female, Genetic Predisposition to Disease, Humans, Male, Muscle Weakness genetics, Paralysis diagnosis, Pedigree, Phenotype, Potassium Channels, Inwardly Rectifying chemistry, Potassium Channels, Inwardly Rectifying metabolism, Syndrome, Abnormalities, Multiple genetics, Arrhythmias, Cardiac genetics, Mutation, Paralysis genetics, Phosphatidylinositol 4,5-Diphosphate metabolism, Potassium Channels, Inwardly Rectifying genetics
Abstract

Background: Mutations in KCNJ2, the gene encoding the inward-rectifying K+ channel Kir2.1, cause the cardiac, skeletal muscle, and developmental phenotypes of Andersen-Tawil syndrome (ATS; also known as Andersen syndrome). Although pathogenic mechanisms have been proposed for select mutations, a common mechanism has not been identified., Methods: Seventeen probands presenting with symptoms characteristic of ATS were evaluated clinically and screened for mutations in KCNJ2. The results of mutation analysis were combined with those from previously studied subjects to assess the frequency with which KCNJ2 mutations cause ATS., Results: Mutations in KCNJ2 were discovered in nine probands. These included six novel mutations (D71N, T75R, G146D, R189I, G300D, and R312C) as well as previously reported mutations R67W and R218W. Six probands possessed mutations of residues implicated in binding membrane-associated phosphatidylinositol 4,5-bisphosphate (PIP2). In total, mutations in PIP(2)-related residues accounted for disease in 18 of 29 (62%) reported KCNJ2 -based probands with ATS. Also reported is that mutation R67W causes the full clinical triad in two unrelated males., Conclusions: The novel mutations corresponding to residues involved in Kir2.1 channel-PIP2 interactions presented here as well as the overall frequency of mutations occurring in these residues indicate that defects in PIP2 binding constitute a major pathogenic mechanism of ATS. Furthermore, screening KCNJ2 in patients with the complex phenotypes of ATS was found to be invaluable in establishing or confirming a disease diagnosis as mutations in this gene can be identified in the majority of patients.

Published
2003
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27. Collaborative translational research leading to multicenter clinical trials in Duchenne muscular dystrophy: the Cooperative International Neuromuscular Research Group (CINRG).

Author

Escolar DM, Henricson EK, Pasquali L, Gorni K, and Hoffman EP

Subjects
Animals, Clinical Trials as Topic, Disease Models, Animal, Drug Evaluation, Drug Evaluation, Preclinical, Humans, Multicenter Studies as Topic, Muscular Dystrophy, Duchenne drug therapy, Research organization & administration, Muscular Dystrophy, Duchenne therapy
Abstract

Progress in the development of rationally based therapies for Duchenne muscular dystrophy has been accelerated by encouraging multidisciplinary, multi-institutional collaboration between basic science and clinical investigators in the Cooperative International Research Group. We combined existing research efforts in pathophysiology by a gene expression profiling laboratory with the efforts of animal facilities capable of conducting high-throughput drug screening and toxicity testing to identify safe and effective drug compounds that target different parts of the pathophysiologic cascade in a genome-wide drug discovery approach. Simultaneously, we developed a clinical trial coordinating center and an international network of collaborating physicians and clinics where those drugs could be tested in large-scale clinical trials. We hope that by bringing together investigators at these facilities and providing the infrastructure to support their research, we can rapidly move new bench discoveries through animal model screening and into therapeutic testing in humans in a safe, timely and cost-effective setting.

Published
2002
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28. Severe autosomal recessive rippling muscle disease.

Author

Koul RL, Chand RP, Chacko A, Ali M, Brown KM, Bushnarmuth SR, Escolar DM, and Stephan DA

Subjects
Adolescent, Arrhythmias, Cardiac diagnosis, Arrhythmias, Cardiac mortality, Electrocardiography, Family Health, Fatal Outcome, Female, Genes, Recessive, Humans, Male, Pedigree, Phenotype, Arrhythmias, Cardiac genetics, Muscle, Skeletal pathology, Muscular Diseases genetics, Muscular Diseases pathology
Abstract

Rippling muscle disease (RMD) has previously been reported as a skeletal myopathy that was attributed to a defect in the sarcomere. Here we report a new form of RMD that is more severe, characterized by fatal arrhythmic cardiomyopathy and delayed bone age. Mortality has previously not been associated with RMD. With this report we hope to raise awareness that a subset of patients with this clinical entity are predisposed to severe cardiac disease., (Copyright 2001 John Wiley & Sons, Inc.)

Published
2001
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30. Gentamicin treatment of Duchenne and Becker muscular dystrophy due to nonsense mutations.

Author

Wagner KR, Hamed S, Hadley DW, Gropman AL, Burstein AH, Escolar DM, Hoffman EP, and Fischbeck KH

Subjects
Adolescent, Biopsy, Blotting, Western, Child, Creatine Kinase blood, Dystrophin biosynthesis, Dystrophin chemistry, Dystrophin genetics, Dystrophin immunology, Gentamicins administration & dosage, Gentamicins adverse effects, Humans, Muscle, Skeletal metabolism, Muscle, Skeletal physiopathology, Muscular Dystrophy, Duchenne blood, Muscular Dystrophy, Duchenne metabolism, Phenotype, Treatment Outcome, Codon, Nonsense genetics, Gentamicins therapeutic use, Muscular Dystrophy, Duchenne drug therapy, Muscular Dystrophy, Duchenne genetics
Abstract

Aminoglycosides have previously been shown to suppress nonsense mutations, allowing translation of full-length proteins in vitro and in animal models. In the mdx mouse, where muscular dystrophy is due to a nonsense mutation in the dystrophin gene, gentamicin suppressed truncation of the protein and ameliorated the phenotype. A subset of patients with Duchenne and Becker muscular dystrophy similarly possess a nonsense mutation, causing premature termination of dystrophin translation. Four such patients, with various stop codon sequences, were treated once daily with intravenous gentamicin at 7.5 mg/kg/day for 2 weeks. No ototoxicity or nephrotoxicity was detected. Full-length dystrophin was not detected in pre- and post-treatment muscle biopsies.

Published
2001

31. Clinical evaluator reliability for quantitative and manual muscle testing measures of strength in children.

Author

Escolar DM, Henricson EK, Mayhew J, Florence J, Leshner R, Patel KM, and Clemens PR

Subjects
Child, Hand, Humans, Joints physiopathology, Middle Aged, Muscular Dystrophy, Duchenne physiopathology, Observer Variation, Reproducibility of Results, Hand Strength physiology, Muscle, Skeletal physiopathology, Muscular Dystrophies physiopathology
Abstract

Measurements of muscle strength in clinical trials of Duchenne muscular dystrophy have relied heavily on manual muscle testing (MMT). The high level of intra- and interrater variability of MMT compromises clinical study results. We compared the reliability of 12 clinical evaluators in performing MMT and quantitative muscle testing (QMT) on 12 children with muscular dystrophy. QMT was reliable, with an interclass correlation coefficient (ICC) of >0.9 for biceps and grip strength, and >0.8 for quadriceps strength. Training of both subjects and evaluators was easily accomplished. MMT was not as reliable, and required repeated training of evaluators to bring all groups to an ICC >0.75 for shoulder abduction, elbow and hip flexion, knee extension, and ankle dorsiflexion. We conclude that QMT shows greater reliability and is easier to implement than MMT. Consequently, QMT will be a superior measure of strength for use in pediatric, neuromuscular, multicenter clinical trials., (Copyright 2001 John Wiley & Sons, Inc.)

Published
2001
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32. Pharmacologic and genetic therapy for childhood muscular dystrophies.

Author

Escolar DM and Scacheri CG

Subjects
Animals, Cell Transplantation, Child, Child, Preschool, Clinical Trials as Topic, Creatine therapeutic use, Cytoskeletal Proteins genetics, Cytoskeletal Proteins physiology, Drug Administration Schedule, Dystrophin genetics, Female, Gene Expression Regulation, Genetic Vectors therapeutic use, Humans, Male, Membrane Proteins genetics, Membrane Proteins physiology, Mice, Mice, Inbred mdx, Muscle, Skeletal cytology, Muscular Dystrophies drug therapy, Muscular Dystrophies physiopathology, Muscular Dystrophy, Animal therapy, Muscular Dystrophy, Duchenne drug therapy, Muscular Dystrophy, Duchenne physiopathology, Muscular Dystrophy, Duchenne therapy, Prednisone adverse effects, Prednisone therapeutic use, Pregnenediones therapeutic use, Protein Biosynthesis, Sarcolemma pathology, Utrophin, Genetic Therapy, Muscular Dystrophies therapy
Abstract

The outstanding advances in the molecular characterization of muscle diseases, including muscular dystrophies, inflammatory myopathies, and ion channel disorders, have resulted in the identification of potential targets for pharmacologic and genetic therapy in the best characterized of these diseases. The most common myopathy in children, Duchenne muscular dystrophy (DMD), is the focus of active pharmacologic clinical trials. Genetic transfer therapy research for this and other dystrophies is rapidly moving forward. However, as new approaches for treatment are being actively investigated, the current modality of treatment for all myopathies is still in the realm of physical medicine and rehabilitation. The focus of this review is on the advances in pharmacologic and genetic therapy research in DMD and limb girdle muscular dystrophies.

Published
2001
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33. Pediatric radial mononeuropathies: a clinical and electromyographic study of sixteen children with review of the literature.

Author

Escolar DM and Jones HR Jr

Subjects
Adolescent, Child, Child, Preschool, Electromyography, Female, Humans, Male, Peripheral Nervous System Diseases physiopathology, Peripheral Nervous System Diseases surgery, Prognosis, Wrist innervation, Radial Nerve surgery
Abstract

Sixteen pediatric radial mononeuropathies were seen among 2077 electromyograms performed in the electromyography laboratory at The Children's Hospital, Boston, during 16.5 years, 1979-1995. Eight (50%) of these radial neuropathies, including 2 in newborns with apparent prenatal onset, were atraumatic, primarily related to compression in 6 and entrapment in 2. The other 8 (50%) were traumatic related to fractures or lacerations. Electromyography documented the radial neuropathy to be localized to the proximal main radial nerve trunk in 2 (13%), distal main radial nerve trunk in 9 (56%), and posterior interosseous nerve in 5 (31%) children. Significant improvement was noted in 13 of the 16 radial neuropathies--within 6-12 weeks for demyelinating lesions and up to 17 months for axonal injuries. Rarely, a child with a chronic progressive radial neuropathy or a postfracture radial neuropathy that does not improve in 3 months may require exploration.

Published
1996
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