Clinical prediction models for treatment outcomes in newly diagnosed epilepsy: A systematic review

Author:

Ratcliffe Corey12ORCID,Pradeep Vishnav3,Marson Anthony1ORCID,Keller Simon S.14ORCID,Bonnett Laura J.3ORCID

Affiliation:

1. Department of Pharmacology and Therapeutics Institute of Systems, Molecular, and Integrative Biology, University of Liverpool Liverpool UK

2. Department of Neuro Imaging and Interventional Radiology National Institute of Mental Health and Neuro Sciences Bangalore India

3. Department of Health Data Science University of Liverpool Liverpool UK

4. Walton Centre NHS Foundation Trust Liverpool UK

Abstract

AbstractUp to 35% of individuals diagnosed with epilepsy continue to have seizures despite treatment, commonly referred to as drug‐resistant epilepsy. Uncontrolled seizures can directly, or indirectly, negatively impact an individual's quality of life. To inform clinical management and life decisions, it is important to be able to predict the likelihood of seizure control. Those likely to achieve seizure control will be able to return sooner to their usual work and leisure activities and require less follow‐up, whereas those with a poor prognosis will need more frequent clinical attendance and earlier consideration of epilepsy surgery. This is a systematic review aimed at identifying demographic, clinical, physiological (e.g., electroencephalographic), and imaging (e.g., magnetic resonance imaging) factors that may be predictive of treatment outcomes in patients with newly diagnosed epilepsy (NDE). MEDLINE and Embase were searched for prediction models of treatment outcomes in patients with NDE. Study characteristics were extracted and subjected to assessment of risk of bias (and applicability concerns) using the PROBAST (Prediction Model Risk of Bias Assessment Tool) tool. Baseline variables associated with treatment outcomes are reported as prognostic factors. After screening, 48 models were identified in 32 studies, which generally scored low for concerns of applicability, but universally scored high for susceptibility to bias. Outcomes reported fit broadly into four categories: drug resistance, short‐term treatment response, seizure remission, and mortality. Prognostic factors were also heterogenous, but the predictors that were commonly significantly associated with outcomes were those related to seizure characteristics/types, epilepsy history, and age at onset. Antiseizure medication response was often included as a baseline variable, potentially obscuring other factor relationships at baseline. Currently, outcome prediction models for NDE demonstrate a high risk of bias. Model development could be improved with a stronger adherence to recommended TRIPOD (Transparent Reporting of a Multivariable Prediction Model for Individual Prognosis or Diagnosis) practices. Furthermore, we outline actionable changes to common practices that are intended to improve the overall quality of prediction model development in NDE.

Publisher

Wiley

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