4.4 Article

Validity of the Neurology Quality-of-Life (Neuro-QoL) measurement system in adult epilepsy

期刊

EPILEPSY & BEHAVIOR
卷 31, 期 -, 页码 77-84

出版社

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.yebeh.2013.11.008

关键词

Epilepsy; Quality of life; Neuro-QoL; Measurement; Psychometrics; Validation

资金

  1. National Institute for Neurological Disorders and Stroke [HHSN 2652004236-01C, HHSN 271201200036C-0-0-1]

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Epilepsy is a chronic neurological disorder that results in recurring seizures and can have a significant adverse effect on health-related quality of life (HRQL). The Neuro-QoL measurement initiative is an NINDS-funded system of patient-reported outcome measures for neurology clinical research, which was designed to provide a precise and standardized way to measure HRQL in epilepsy and other neurological disorders. Using mixed-method and item response theory-based approaches, we developed generic item banks and targeted scales for adults and children with major neurological disorders. This paper provides empirical results from a clinical validation study with a sample of adults diagnosed with epilepsy. One hundred twenty-one people diagnosed with epilepsy participated, the majority of which were male (62%) and Caucasian (95%), with a mean age of 47.3 (SD = 16.9). Baseline assessments included Neuro-QoL short forms and general and external validity measures. The Neuro-QoL short forms that are not typically found in other epilepsy-specific HRQL instruments include Stigma, Sleep Disturbance, Emotional and Behavioral Dyscontrol, and Positive Affect and Well-Being. Neurology Quality-of-Life short forms demonstrated adequate reliability (internal consistency range =.86-. 96; test-retest range =.57-. 89). Pearson correlations (p < .01) between Neuro-QoL forms of emotional distress (anxiety, depression, stigma) and the QOLIE-31 Emotional Well-Being subscale were in the moderate-to-strong range (r's =.66,.71 and.53, respectively), as were relations with the PROMIS Global Mental Health subscale (r's =.59,.74 and.52, respectively). Moderate correlations were observed between Neuro-QoL Social Role Performance and Satisfaction and the QOLIE-31 Social Function (r's =.58 and.52, respectively). In measuring aspects of physical function, the Neuro-QoL Mobility and Upper Extremity forms demonstrated moderate associations with the PROMIS Global Physical Function subscale (r's =.60 and.61, respectively). Neuro-QoL measures of perceived cognitive function (executive function and general concerns) produced moderate-to-strong correlations with the QOLIE-31 Cognition subscale (r's =.65 and.75, respectively) and moderate relations with the Liverpool Adverse Events Profile (r's =.51 and.69, respectively). Finally, the Neuro-QoL Fatigue measure demonstrated moderate associations with the QOLIE-31 Energy/Fatigue subscale (r = -. 65), Liverpool Adverse Events Profile (r =.69), and the Liverpool Seizure Severity Scale (r =.50). Five Neuro-QoL short forms demonstrated statistically significant responsiveness to change at 5-7 months, including Fatigue, Sleep Disturbance, Depression, Positive Affect and Well-Being, and Emotional and Behavioral Dyscontrol. Overall, Neuro-QoL instruments showed good evidence for internal consistency, test-retest reliability, convergent validity, and responsiveness to change over several months. These results support the validity of Neuro-QoL to measure HRQL in adults with epilepsy. (C) 2013 Elsevier Inc. All rights reserved.

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