Your search keyword '"Roye, David P."' showing total 5 results

1. Management and treatment of musculoskeletal problems in adults with cerebral palsy: Experience gained from two lifespan clinics.

Author

Katsma, Mark, Liu, Haiqing, Pan, Xiaoyu, Ryan, Kyle J., Roye, David P., and Chambers, Henry G.

Subjects

*BACLOFEN, *BONE density, *SPONDYLOLISTHESIS, *HYDROCEPHALUS, *SPINAL injections, *SCOLIOSIS, *MUSCULOSKELETAL system abnormalities, *CEREBRAL palsy, *FOOT abnormalities, *SURGICAL complications, *HIP joint, *SUBLUXATION, *BOTULINUM toxin

Published

2024

2. Improvement in a post-stroke pediatric patient with hemiplegia: Use of a hand-arm bimanual intensive therapy with hybrid assistive limb.

Author

Matsumoto, Yoko, Yoshii, Yuji, Ikutomo, Akiyo, Yagi, Mariko, Nishimura, Mio, Kawasaki, Yoko, Sarafian, Amanda, Kim, Heakyung, Roye, David P., and Matsumoto, Hiroko

Subjects

*CHILD patients, *PHYSICAL mobility, *CEREBRAL infarction, *PEDIATRIC therapy, *BOTULINUM A toxins

Abstract

Pediatric stroke is a rare medical condition that often leads to long-lasting motor and cognitive impairments. Although therapies for adults after a stroke are well described, treatments for motor deficits following a pediatric stroke are yet to be investigated. We report a case of pediatric stroke in the chronic phase, in which a combination of novel treatments resulted in a significant improvement in physical function. A seven-year-old girl with a left hemispheric cerebral infarction lost almost all right upper extremity motor function. Following onabotulinumtoxinA treatment, she underwent hand-arm bimanual intensive therapy augmented with a hybrid assistive limb for 90 h over 15 days. Evaluation after the training revealed significant improvements in physical function, daily activities, and occupational performance. This report highlights the importance of innovative combinations of techniques in the treatment of pediatric stroke. [ABSTRACT FROM AUTHOR]

Published

2024

3. Development and Validation of a Health-Related Quality-of-Life Measure in Older Children and Adolescents with Early-Onset Scoliosis: Early-Onset Scoliosis Self-Report Questionnaire (EOSQ-SELF).

Author

Matsumoto, Hiroko, Boby, Afrain Z., Sinha, Rishi, Campbell, Megan L., Hung, Chun Wai, Gbolo, Fay C., Marciano, Gerard F., Levine, Sonya, Fano, Adam N., Simhon, Matthew E., Quan, Theodore, Bainton, Nicole M., George, Ameeka, Mizerik, Amber S., Roye, Benjamin D., Roye, David P., and Vitale, Michael G.

Subjects

*SELF-evaluation, *PSYCHOMETRICS, *QUALITY of life, *SCOLIOSIS, *QUESTIONNAIRES, *FATIGUE (Physiology), RESEARCH evaluation

Abstract

Background: The 24-question Early-Onset Scoliosis Questionnaire (EOSQ-24) is a proxy measure assessing health-related quality of life (HRQoL) among patients with early-onset scoliosis (EOS). There exists an increasing need to assess HRQoL through a child's own perspective, particularly for older children and adolescents with EOS. The purpose of this study was to develop and validate a self-reported questionnaire, the Early-Onset Scoliosis Self-Report Questionnaire (EOSQ-SELF), to assess HRQoL in older children and adolescents with EOS.Methods: A literature review, an expert focus group, and patient interviews were used to generate a preliminary survey of appropriate domains and question items. This survey was provided to English-speaking patients with EOS who were 8 to 18 years of age and capable of answering survey questions. Content validity was assessed for clarity and relevance of questions. Confirmatory factors analysis was performed to reduce the number of items and determine domains that fit items. Reliability was evaluated by measuring the internal consistency of items and test-retest reliability. Construct validity was evaluated by convergent, discriminant, and known-group validity.Results: The literature review, expert focus group, and patient interviews identified 59 questions in 14 domains. Psychometric analysis reduced these to 30 questions across 12 domains: General Health, Pain/Discomfort, Pulmonary Function, Transfer, Physical Function/Daily Living, Participation, Fatigue/Energy Level, Sleep, Appearance, Relationships, Emotion, and Satisfaction. The final questionnaire was found to have good content and construct validity and adequate reliability.Conclusions: The EOSQ-SELF is a valid and reliable instrument for measuring self-reported HRQoL among older children and adolescents with EOS (ages 8 to 18 years). This will serve as an important research outcome measure and enhance clinical care by providing a better understanding of HRQoL for these patients.Level Of Evidence: Diagnostic Level II . See Instructions for Authors for a complete description of levels of evidence. [ABSTRACT FROM AUTHOR]

Published

2022

4. A Clinical Risk Model for Surgical Site Infection Following Pediatric Spine Deformity Surgery.

Author

Matsumoto, Hiroko, Larson, Elaine L., Warren, Shay I., Hammoor, Bradley T. MS, Bonsignore-Opp, Lisa, Troy, Michael J., Barrett, Kody K., Striano, Brendan M., Li, Gen, Terry, Mary Beth, Roye, Benjamin D., Lenke, Lawrence G., Skaggs, David L. MMM, Glotzbecker, Michael P., Flynn, John M., Roye, David P., Vitale, Michael G., Hammoor, Bradley T, and Skaggs, David L

Subjects

*BONE lengthening (Orthopedics), *SURGICAL site infections, *SPINAL surgery, *SPINE abnormalities, *RECEIVER operating characteristic curves, *MOBILE apps, *SPINAL curvatures, *SPINAL fusion, *RETROSPECTIVE studies, *RISK assessment, *REOPERATION

Abstract

Background: Despite tremendous efforts, the incidence of surgical site infection (SSI) following the surgical treatment of pediatric spinal deformity remains a concern. Although previous studies have reported some risk factors for SSI, these studies have been limited by not being able to investigate multiple risk factors at the same time. The aim of the present study was to evaluate a wide range of preoperative and intraoperative factors in predicting SSI and to develop and validate a prediction model that quantifies the risk of SSI for individual pediatric spinal deformity patients.Methods: Pediatric patients with spinal deformity who underwent primary, revision, or definitive spinal fusion at 1 of 7 institutions were included. Candidate predictors were known preoperatively and were not modifiable in most cases; these included 31 patient, 12 surgical, and 4 hospital factors. The Centers for Disease Control and Prevention definition of SSI within 90 days of surgery was utilized. Following multiple imputation and multicollinearity testing, predictor selection was conducted with use of logistic regression to develop multiple models. The data set was randomly split into training and testing sets, and fivefold cross-validation was performed to compare discrimination, calibration, and overfitting of each model and to determine the final model. A risk probability calculator and a mobile device application were developed from the model in order to calculate the probability of SSI in individual patients.Results: A total of 3,092 spinal deformity surgeries were included, in which there were 132 cases of SSI (4.3%). The final model achieved adequate discrimination (area under the receiver operating characteristic curve: 0.76), as well as calibration and no overfitting. Predictors included in the model were nonambulatory status, neuromuscular etiology, pelvic instrumentation, procedure time ≥7 hours, American Society of Anesthesiologists grade >2, revision procedure, hospital spine surgical cases <100/year, abnormal hemoglobin level, and overweight or obese body mass index.Conclusions: The risk probability calculator encompassing patient, surgical, and hospital factors developed in the present study predicts the probability of 90-day SSI in pediatric spinal deformity surgery. This validated calculator can be utilized to improve informed consent and shared decision-making and may allow the deployment of additional resources and strategies selectively in high-risk patients.Level Of Evidence: Prognostic Level III. See Instructions for Authors for a complete description of levels of evidence. [ABSTRACT FROM AUTHOR]

Published

2022

5. Genetic testing in individuals with cerebral palsy.

Author

May, Halie J, Fasheun, Jennifer A, Bain, Jennifer M, Baugh, Evan H, Bier, Louise E, Revah‐Politi, Anya, Roye, David P, Goldstein, David B, Carmel, Jason B, Lippa, Natalie, Vena, Natalie, Kushary, Sulagna, Hyman, Joshua, Hewson, Barbara, Marboe, Charles, Anyane‐Yeboa, Kwame, and Aggarwal, Vimla

Subjects

*CEREBRAL palsy, *GENETIC testing, *GENETIC variation, *INTRACRANIAL hemorrhage, *PEOPLE with cerebral palsy, *STROKE, *ASPHYXIA neonatorum, *MATERNAL age

Abstract

AIM To determine which patients with cerebral palsy (CP) should undergo genetic testing, we compared the rate of likely causative genetic variants from whole‐exome sequencing in individuals with and without environmental risk factors. METHOD Patients were part of a convenience and physician‐referred cohort recruited from a single medical center, and research whole‐exome sequencing was completed. Participants were evaluated for the following risk factors: extreme preterm birth, brain bleed or stroke, birth asphyxia, brain malformations, and intrauterine infection. RESULTS A total of 151 unrelated individuals with CP (81 females, 70 males; mean age 25y 7mo [SD 17y 5mo], range 3wks–72y) participated. Causative genetic variants were identified in 14 participants (9.3%). There was no significant difference in diagnostic rate between individuals with risk factors (10 out of 123; 8.1%) and those without (4 out of 28; 14.3%) (Fisher's exact p=0.3). INTERPRETATION While the rate of genetic diagnoses among individuals without risk factors was higher than those with risk factors, the difference was not statistically significant at this sample size. The identification of genetic diagnoses in over 8% of cases with risk factors suggests that these might confer susceptibility to environmental factors, and that further research should include individuals with risk factors. What this paper addsThere is no significant difference in diagnostic rate between individuals with and without risk factors.Genetic variants may confer susceptibility to environmental risk factors.Six causative variants were identified in genes not previously associated with cerebral palsy.Global developmental delay/intellectual disability is positively associated with a genetic etiology.Extreme preterm birth, stroke/brain hemorrhage, and older age are negatively associated with a genetic etiology. What this paper adds: There is no significant difference in diagnostic rate between individuals with and without risk factors.Genetic variants may confer susceptibility to environmental risk factors.Six causative variants were identified in genes not previously associated with cerebral palsy.Global developmental delay/intellectual disability is positively associated with a genetic etiology.Extreme preterm birth, stroke/brain hemorrhage, and older age are negatively associated with a genetic etiology. This original article is commented by MacLennan on page 1369 of this issue. [ABSTRACT FROM AUTHOR]

Published

2021