Charcot-Marie-Tooth disease type 1E: clinical natural history and molecular impact of PMP22 variants

Kailee S Ward; Christopher P Ptak; Natalya Pashkova; Tiffany Grider; Tabitha A Peterson; Davide Pareyson; Chiara Pisciotta; Paola Saveri; Isabella Moroni; Matilde Laura; Joshua Burns; Manoj P Menezes; Kayla Cornett; Richard Finkel; Bipasha Mukherjee-Clavin; Charlotte J Sumner; Maxwell Greene; Omer Abdul Hamid; David Herrmann; Reza Sadjadi; David Walk; Stephan Züchner; Mary M Reilly; Steven S Scherer; Robert C Piper; Michael E Shy; Inherited Neuropathy Consortium

doi:10.1093/brain/awaf219

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Charcot-Marie-Tooth disease type 1E: clinical natural history and molecular impact of PMP22 variants

Journal article

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Charcot-Marie-Tooth disease type 1E: clinical natural history and molecular impact of PMP22 variants

Kailee S Ward, Christopher P Ptak, Natalya Pashkova, Tiffany Grider, Tabitha A Peterson, Davide Pareyson, Chiara Pisciotta, Paola Saveri, Isabella Moroni, Matilde Laura, …

Brain (London, England : 1878), Vol.149(3), pp.1070-1085

03/2026

DOI: 10.1093/brain/awaf219

PMCID: PMC13016674

PMID: 40488457

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Abstract

Charcot-Marie-Tooth disease type 1E (CMT1E) is a rare, autosomal dominant peripheral neuropathy caused by missense variants, deletions, and truncations within the peripheral myelin protein-22 (PMP22) gene. CMT1E phenotypes vary depending on the specific variant, ranging from mild to severe, and there is little natural history and phenotypic progression data on individuals with CMT1E. Patients with CMT1E were evaluated during initial and follow-up visits at sites within the Inherited Neuropathy Consortium. Clinical characteristics were obtained from history, neurological exams, and nerve conduction studies. Clinical outcome measures were used to quantify baseline and longitudinal changes, including the Rasch-modified CMT Examination Score version 2 (CMTESv2-R) and the CMT Pediatric Scale (CMTPedS). The trafficking of PMP22 variants in transfected cells was correlated to disease severity. Twenty-four presumed disease-causing PMP22 variants were identified in 50 individuals from 35 families, including 19 missense variants, three in-frame deletions, and two truncations. Twenty-nine patients presented with delayed walking during childhood. At their baseline evaluation, the mean CMTESv2-R in 46 patients was 16 ± 7.72 (out of 32), and the mean CMTPedS from 17 patients was 28 ± 6.35 (out of 44). Six individuals presented with hearing loss, eleven with scoliosis, three with hip dysplasia, and one with both scoliosis and hip dysplasia. Twenty variants were localized within in transmembrane domains; 31 of 35 individuals with these variants had moderate to severe phenotypes. Three variants were found in the extracellular domain and were associated with milder phenotypes. Reduced expression of PMP22 at the cell surface, and the location of missense variants within in the transmembrane domain correlated with disease severity. Pathogenic PMP22 variants located within the transmembrane regions usually cause a moderate to severe clinical phenotype, beginning in early childhood, and have impaired trafficking to the plasma membrane.

Natural History

Charcot-Marie-Tooth type 1E (CMT1E)

PMP22

Details

Title: Subtitle: Charcot-Marie-Tooth disease type 1E: clinical natural history and molecular impact of PMP22 variants
Creators: Kailee S Ward - University of Iowa
Christopher P Ptak - University of Iowa
Natalya Pashkova - University of Iowa
Tiffany Grider - University of Iowa
Tabitha A Peterson - University of Iowa
Davide Pareyson - Mylan (Switzerland)
Chiara Pisciotta - Mylan (Switzerland)
Paola Saveri - Mylan (Switzerland)
Isabella Moroni - Fondazione IRCCS Istituto Neurologico Carlo Besta
Matilde Laura - National Hospital for Neurology and Neurosurgery
Joshua Burns - St. Jude Children's Research Hospital
Manoj P Menezes
Kayla Cornett
Richard Finkel - St. Jude Children's Research Hospital
Bipasha Mukherjee-Clavin - Johns Hopkins University School of Medicine
Charlotte J Sumner - Johns Hopkins University School of Medicine
Maxwell Greene - Stanford University
Omer Abdul Hamid - Nemours Children's Clinic
David Herrmann - University of Rochester
Reza Sadjadi - Massachusetts General Hospital
David Walk - University of Minnesota
Stephan Züchner - University of Miami
Mary M Reilly - National Hospital for Neurology and Neurosurgery
Steven S Scherer - University of Pennsylvania
Robert C Piper - Department of Molecular Physiology and Biophysics, University of Iowa Carver College of Medicine, Iowa City, IA 52242, USA
Michael E Shy - University of Iowa
Inherited Neuropathy Consortium
Resource Type: Journal article
Publication Details: Brain (London, England : 1878), Vol.149(3), pp.1070-1085
DOI: 10.1093/brain/awaf219
PMID: 40488457
PMCID: PMC13016674
NLM abbreviation: Brain
ISSN: 1460-2156
eISSN: 1460-2156
Publisher: Oxford University Press
Language: English
Electronic publication date: 06/09/2025
Date published: 03/2026
Academic Unit: Neurology; Molecular Physiology and Biophysics; Anatomy and Cell Biology; Iowa Neuroscience Institute; Medicine Administration; Internal Medicine
Record Identifier: 9984829888102771

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