Specific disruption of a Schwann cell dystrophin-related protein complex in a demyelinating neuropathy

被引：149

作者：

Sherman, DL ^{[1
]}

Fabrizi, C ^{[1
]}

Gillespie, CS ^{[1
]}

Brophy, PJ ^{[1
]}

机构：

[1] Univ Edinburgh, Dept Preclin Vet Sci, Edinburgh EH9 1QH, Midlothian, Scotland

来源：

NEURON | 2001年 / 30卷 / 03期

基金：

英国惠康基金;

关键词：

D O I：

10.1016/S0896-6273(01)00327-0

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

Dystroglycan-dystrophin complexes are believed to have structural and signaling functions by linking extracellular matrix proteins to the cytoskeleton and cortical signaling molecules. Here we characterize a dystroglycan-dystrophin-related protein 2 (DRP2) complex at the surface of myelin-forming Schwann cells. The complex is clustered by the interaction of DRP2 with L-periaxin, a homodimeric PDZ domain-containing protein. In the absence of L-periaxin, DRP2 is mislocalized and depleted, although other dystrophin family proteins are unaffected. Disruption of the DRP2-dystroglycan complex is followed by hypermyelination and destabilization of the Schwann cell-axon unit in Prx(-/-) mice. Hence, the DRP2-dystroglycan complex likely has a distinct function in the terminal stages of PNS myelinogenesis, possibly in the regulation of myelin thickness.

引用

页码：677 / 687

页数：11

共 67 条

[1] The three human syntrophin genes are expressed in diverse tissues, have distinct chromosomal locations, and each bind to dystrophin and its relatives [J].

Ahn, AH ;

Freener, CA ;

Gussoni, E ;

Yoshida, M ;

Ozawa, E ;

Kunkel, LM .

JOURNAL OF BIOLOGICAL CHEMISTRY, 1996, 271 (05) :2724-2730

[2] THE STRUCTURAL AND FUNCTIONAL DIVERSITY OF DYSTROPHIN [J].

AHN, AH ;

KUNKEL, LM .

NATURE GENETICS, 1993, 3 (04) :283-291

[3] LAMININ IN ANIMAL-MODELS FOR MUSCULAR-DYSTROPHY - DEFECT OF LAMININ-M IN SKELETAL AND CARDIAC MUSCLES AND PERIPHERAL-NERVE OF THE HOMOZYGOUS DYSTROPHIC DY/DY MICE [J].

ARAHATA, K ;

HAYASHI, YK ;

KOGA, R ;

GOTO, K ;

LEE, JH ;

MIYAGOE, Y ;

ISHII, H ;

TSUKAHARA, T ;

TAKEDA, S ;

WOO, M ;

NONAKA, I ;

MATSUZAKI, T ;

SUGITA, H .

PROCEEDINGS OF THE JAPAN ACADEMY SERIES B-PHYSICAL AND BIOLOGICAL SCIENCES, 1993, 69 (10) :259-264

[4] Periaxin mutations cause recessive Dejerine-Sottas neuropathy [J].

Boerkoel, CF ;

Takashima, H ;

Stankiewicz, P ;

Garcia, CA ;

Leber, SM ;

Rhee-Morris, L ;

Lupski, JR .

AMERICAN JOURNAL OF HUMAN GENETICS, 2001, 68 (02) :325-333

[5] SCHWANN-CELL FUNCTION DEPENDS UPON AXONAL SIGNALS AND BASAL LAMINA COMPONENTS [J].

BUNGE, MB ;

CLARK, MB ;

DEAN, AC ;

ELDRIDGE, CF ;

BUNGE, RP .

ANNALS OF THE NEW YORK ACADEMY OF SCIENCES, 1990, 580 :281-287

[6]

BUNGE RP, 1986, ANNU REV NEUROSCI, V9, P305

[7] EVIDENCE THAT CONTACT WITH CONNECTIVE-TISSUE MATRIX IS REQUIRED FOR NORMAL INTERACTION BETWEEN SCHWANN-CELLS AND NERVE-FIBERS [J].

BUNGE, RP ;

BUNGE, MB .

JOURNAL OF CELL BIOLOGY, 1978, 78 (03) :943-950

[8] SCHWANN-CELL MYELINATION - INDUCTION BY EXOGENOUS BASEMENT-MEMBRANE LIKE EXTRACELLULAR-MATRIX [J].

CAREY, DJ ;

TODD, MS ;

RAFFERTY, CM .

JOURNAL OF CELL BIOLOGY, 1986, 102 (06) :2254-2263

[9] Requirement for the PDZ domain protein, INAD, for localization of the TRP store-operated channel to a signaling complex [J].

Chevesich, J ;

Kreuz, AJ ;

Montell, C .

NEURON, 1997, 18 (01) :95-105

[10] A G(+1)-]A TRANSVERSION AT THE 5'-SPLICE-SITE OF INTRON-69 OF THE DYSTROPHIN GENE CAUSING THE ABSENCE OF PERIPHERAL-NERVE DP116 AND SEVERE CLINICAL INVOLVEMENT IN A DMD PATIENT [J].

COMI, GP ;

CIAFALONI, E ;

DESILVA, HAR ;

PRELLE, A ;

BARDONI, A ;

RIGOLETTO, C ;

ROBOTTI, M ;

BRESOLIN, N ;

MOGGIO, M ;

FORTUNATO, F ;

CISCATO, P ;

TURCONI, A ;

ROSE, AD ;

SCARLATO, G .

HUMAN MOLECULAR GENETICS, 1995, 4 (11) :2171-2174

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