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. 2019 Feb 1;173(2):134-139.
doi: 10.1001/jamapediatrics.2018.4890.

Clinical Subpopulations in a Sample of North American Children Diagnosed With Acute Flaccid Myelitis, 2012-2016

Matthew J Elrick  1 Eliza Gordon-Lipkin  2 Thomas O Crawford  1 Keith Van Haren  3 Kevin Messacar  4 Nicole Thornton  5 Elizabeth Dee  5 Annie Voskertchian  6 Jessica R Nance  1 Laura S Muñoz  1 Mark P Gorman  7 Leslie A Benson  7 David L Thomas  8 Carlos A Pardo  1 Aaron M Milstone  5   6 Priya Duggal  5
Affiliations

Clinical Subpopulations in a Sample of North American Children Diagnosed With Acute Flaccid Myelitis, 2012-2016

Matthew J Elrick et al. JAMA Pediatr. .

Abstract

Importance: Acute flaccid myelitis (AFM) is an emerging poliolike illness of children whose clinical spectrum and associated pathogens are only partially described. The case definition is intentionally encompassing for epidemiologic surveillance to capture all potential AFM cases. Defining a restrictive, homogenous subpopulation may aid our understanding of this emerging disease.

Objective: To evaluate the extent to which the US Centers for Disease Control and Prevention (CDC) case definition of AFM incorporates possible alternative diagnoses and to assess the plausibility of a case definition that enriches the biological homogeneity of AFM for inclusion in research studies.

Design, setting, and participants: Retrospective case analysis of children younger than 18 years diagnosed as having AFM between 2012 and 2016 using the CDC case definition. Group 1 included patients recruited from the United States and Canada based on the CDC case definition of AFM. Group 2 included patients referred to the Johns Hopkins Transverse Myelitis Center for evaluation of suspected AFM. Patients' records and imaging data were critically reviewed by 3 neurologists to identify those cases with definable alternative diagnoses, and the remaining patients were categorized as having restrictively defined AFM (rAFM). Clinical characteristics were compared between patients with rAFM (cases) and those with alternative diagnoses, and a case description distinguishing these AFM groups was identified. Interrater reliability of this description was confirmed for a subset of cases by a fourth neurologist. Data were analyzed between May 2017 and November 2018.

Main outcomes and measures: Proportion of patients with possible alternative diagnosis.

Results: Of the 45 patients who met the CDC AFM case definition and were included, the mean age was 6.1 years; 27 were boys (60%); and 37 were white (82%), 3 were Asian (7%), 1 was Hispanic (2%), and 4 were mixed race/ethnicity (9%). Of the included patients, 34 were classified as having rAFM, and 11 had alternate diagnoses (including transverse myelitis, other demyelinating syndromes, spinal cord stroke, Guillain-Barre syndrome, Chiari I myelopathy, and meningitis). Factors differing between groups were primarily asymmetry of weakness, lower motor neuron signs, preceding viral syndrome, symptoms evolving over hours to days, absence of sensory deficits, and magnetic resonance imaging findings. A case description was able to reliably define the rAFM group.

Conclusions and relevance: We present an approach for defining a homogeneous research population that may more accurately reflect the pathogenesis of the prototypical poliomyelitis-like subgroup of AFM. The definition of rAFM forms a blueprint for inclusion criteria in future research efforts, but more work is required for refinement and external validation.

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Conflict of interest statement

Conflict of Interest Disclosures: Dr Van Haren reported work as an unpaid adviser to the US Centers for Disease Control and Prevention on clinical considerations for treatment of acute flaccid myelitis. Dr Messacar reported grant K23AI28069 from the National Institutes of Health/National Institute of Allergy and Infectious Diseases during the conduct of the study. Dr Benson reported personal fees from Biogen outside the submitted work. Dr Thomas reported grants from the National Institutes of Health during the conduct of the study. Dr Pardo reported other support from the Bart McLean Fund for Neuroimmunology Research and grants from the Transverse Myelitis Association during the conduct of the study. Dr Milstone reported personal fees from BD Biosciences outside the submitted work. Dr Duggal reported grants from the Burroughs-Wellcome Fund outside the submitted work. No other disclosures were reported.

Comment in

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