Clinically distinct codon 69 mutations in major myelin protein zero in demyelinating neuropathies

P. H. Meijerink; J. E. Hoogendijk; A. A. Gabreëls-Festen; I. Zorn; H. Veldman; F. Baas; M. de Visser; P. A. Bolhuis

doi:https://doi.org/10.1002/ana.410400418

Clinically distinct codon 69 mutations in major myelin protein zero in demyelinating neuropathies

P. H. Meijerink, J. E. Hoogendijk, A. A. Gabreëls-Festen, I. Zorn, H. Veldman, F. Baas, M. de Visser, P. A. Bolhuis

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Abstract

Mutations in the major peripheral myelin protein zero (P0) gene on chromosome 1q21-q23 have been found with the hereditary demyelinating polyneuropathy Charcot-Marie-Tooth type 1B. Here, we describe 2 patients with distinct neurological characteristics, carrying different substitutions at the same codon--Arg69His and Arg69Cys. The patients were heterozygous for the mutation, which in both appeared to be de novo. Histological examination of sural nerve biopsy specimens revealed defective myelin as well as marked differences, confirming the importance of P0 in the compaction of myelin

Original language	English
Pages (from-to)	672-675
Journal	Annals of neurology
Volume	40
Issue number	4
DOIs	https://doi.org/10.1002/ana.410400418
Publication status	Published - 1996

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https://doi.org/10.1002/ana.410400418

Cite this

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title = "Clinically distinct codon 69 mutations in major myelin protein zero in demyelinating neuropathies",

abstract = "Mutations in the major peripheral myelin protein zero (P0) gene on chromosome 1q21-q23 have been found with the hereditary demyelinating polyneuropathy Charcot-Marie-Tooth type 1B. Here, we describe 2 patients with distinct neurological characteristics, carrying different substitutions at the same codon--Arg69His and Arg69Cys. The patients were heterozygous for the mutation, which in both appeared to be de novo. Histological examination of sural nerve biopsy specimens revealed defective myelin as well as marked differences, confirming the importance of P0 in the compaction of myelin",

author = "Meijerink, {P. H.} and Hoogendijk, {J. E.} and Gabre{\"e}ls-Festen, {A. A.} and I. Zorn and H. Veldman and F. Baas and {de Visser}, M. and Bolhuis, {P. A.}",

year = "1996",

doi = "https://doi.org/10.1002/ana.410400418",

language = "English",

volume = "40",

pages = "672--675",

journal = "Annals of neurology",

issn = "0364-5134",

publisher = "John Wiley and Sons Inc.",

number = "4",

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TY - JOUR

T1 - Clinically distinct codon 69 mutations in major myelin protein zero in demyelinating neuropathies

AU - Meijerink, P. H.

AU - Hoogendijk, J. E.

AU - Gabreëls-Festen, A. A.

AU - Zorn, I.

AU - Veldman, H.

AU - Baas, F.

AU - de Visser, M.

AU - Bolhuis, P. A.

PY - 1996

Y1 - 1996

N2 - Mutations in the major peripheral myelin protein zero (P0) gene on chromosome 1q21-q23 have been found with the hereditary demyelinating polyneuropathy Charcot-Marie-Tooth type 1B. Here, we describe 2 patients with distinct neurological characteristics, carrying different substitutions at the same codon--Arg69His and Arg69Cys. The patients were heterozygous for the mutation, which in both appeared to be de novo. Histological examination of sural nerve biopsy specimens revealed defective myelin as well as marked differences, confirming the importance of P0 in the compaction of myelin

AB - Mutations in the major peripheral myelin protein zero (P0) gene on chromosome 1q21-q23 have been found with the hereditary demyelinating polyneuropathy Charcot-Marie-Tooth type 1B. Here, we describe 2 patients with distinct neurological characteristics, carrying different substitutions at the same codon--Arg69His and Arg69Cys. The patients were heterozygous for the mutation, which in both appeared to be de novo. Histological examination of sural nerve biopsy specimens revealed defective myelin as well as marked differences, confirming the importance of P0 in the compaction of myelin

U2 - https://doi.org/10.1002/ana.410400418

DO - https://doi.org/10.1002/ana.410400418

M3 - Article

C2 - 8871588

SN - 0364-5134

VL - 40

SP - 672

EP - 675

JO - Annals of neurology

JF - Annals of neurology

IS - 4

ER -