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

被引：28

作者：

Meijerink, PHS

Hoogendijk, JE

GabreelsFesten, AAWM

Zorn, I

Veldman, H

Baas, F

deVisser, M

Bolhuis, PA

机构：

[1] UNIV AMSTERDAM,ACAD MED CTR,DEPT NEUROL,NL-1105 AZ AMSTERDAM,NETHERLANDS

[2] UNIV UTRECHT HOSP,DEPT NEUROL,UTRECHT,NETHERLANDS

[3] UNIV NIJMEGEN HOSP,INST NEUROL,NL-6500 HB NIJMEGEN,NETHERLANDS

来源：

ANNALS OF NEUROLOGY | 1996年 / 40卷 / 04期

关键词：

D O I：

10.1002/ana.410400418

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

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 far the mutation, which in both appeared to be de novo. Histological examination of sural nerve biopsy specimens revealed defective myelin as cell as marked differences, confirming the importance of P0 in the compaction of myelin.

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页码：672 / 675

页数：4

相关论文

共 19 条

[1] LOCAL MODULATION OF NEUROFILAMENT PHOSPHORYLATION, AXONAL CALIBER, AND SLOW AXONAL-TRANSPORT BY MYELINATING SCHWANN-CELLS [J].

DEWAEGH, SM ;

LEE, VMY ;

BRADY, ST .

CELL, 1992, 68 (03) :451-463

[2]

DING YG, 1994, J BIOL CHEM, V269, P10764

[3] HOMOPHILIC ADHESION OF THE MYELIN PO PROTEIN REQUIRES GLYCOSYLATION OF BOTH MOLECULES IN THE HOMOPHILIC PAIR [J].

FILBIN, MT ;

TENNEKOON, GI .

JOURNAL OF CELL BIOLOGY, 1993, 122 (02) :451-459

[4] ROLE OF MYELIN PO PROTEIN AS A HOMOPHILIC ADHESION MOLECULE [J].

FILBIN, MT ;

WALSH, FS ;

TRAPP, BD ;

PIZZEY, JA ;

TENNEKOON, GI .

NATURE, 1990, 344 (6269) :871-872

[5] EARLY MORPHOLOGICAL FEATURES IN DOMINANTLY INHERITED DEMYELINATING MOTOR AND SENSORY NEUROPATHY (HMSN TYPE-I) [J].

GABREELSFESTEN, AAWM ;

JOOSTEN, EMG ;

GABREELS, FJM ;

JENNEKENS, FGI ;

KEMPEN, TWJ .

JOURNAL OF THE NEUROLOGICAL SCIENCES, 1992, 107 (02) :145-154

[6] MOUSE P(0) GENE DISRUPTION LEADS TO HYPOMYELINATION, ABNORMAL EXPRESSION OF RECOGNITION MOLECULES, AND DEGENERATION OF MYELIN AND AXONS [J].

GIESE, KP ;

MARTINI, R ;

LEMKE, G ;

SORIANO, P ;

SCHACHNER, M .

CELL, 1992, 71 (04) :565-576

[7] ISOLATION AND SEQUENCE DETERMINATION OF CDNA-ENCODING THE MAJOR STRUCTURAL PROTEIN OF HUMAN PERIPHERAL MYELIN [J].

HAYASAKA, K ;

NANAO, K ;

TAHARA, M ;

SATO, W ;

TAKADA, G ;

MIURA, M ;

UYEMURA, K .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1991, 180 (02) :515-518

[8] CHARCOT-MARIE-TOOTH NEUROPATHY TYPE-1B IS ASSOCIATED WITH MUTATIONS OF THE MYELIN-P(0) GENE [J].

HAYASAKA, K ;

HIMORO, M ;

SATO, W ;

TAKADA, G ;

UYEMURA, K ;

SHIMIZU, N ;

BIRD, TD ;

CONNEALLY, PM ;

CHANCE, PF .

NATURE GENETICS, 1993, 5 (01) :31-34

[9] MUTATION OF THE MYELIN PO GENE IN CHARCOT-MARIE-TOOTH NEUROPATHY TYPE-1 [J].

HAYASAKA, K ;

OHNISHI, A ;

TAKADA, G ;

FUKUSHIMA, Y ;

MURAI, Y .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1993, 194 (03) :1317-1322

[10] DE-NOVO MUTATION OF THE MYELIN P(O) GENE IN DEJERINE-SOTTAS DISEASE (HEREDITARY MOTOR AND SENSORY NEUROPATHY TYPE-III) [J].

HAYASAKA, K ;

HIMORO, M ;

SAWAISHI, Y ;

NANAO, K ;

TAKAHASHI, T ;

TAKADA, G ;

NICHOLSON, GA ;

OUVRIER, RA ;

TACHI, N .

NATURE GENETICS, 1993, 5 (03) :266-268