Congenital muscular dystrophy with primary laminin alpha 2 (merosin) deficiency presenting as inflammatory myopathy

被引：85

作者：

Pegoraro, E

Mancias, P

Swerdlow, SH

Raikow, RB

Garcia, C

Marks, H

Crawford, T

Carver, V

DiCianno, B

Hoffman, EP

机构：

[1] UNIV PITTSBURGH,SCH MED,DEPT MOL GENET & BIOCHEM,PITTSBURGH,PA 15261

[2] UNIV PITTSBURGH,SCH MED,DEPT HUMAN GENET,PITTSBURGH,PA 15261

[3] UNIV PITTSBURGH,SCH MED,DEPT PEDIAT,PITTSBURGH,PA 15261

[4] UNIV ARKANSAS MED SCI HOSP,DEPT PEDIAT,LITTLE ROCK,AR 72205

[5] UNIV PITTSBURGH,MED CTR,DEPT PATHOL,PITTSBURGH,PA 15260

[6] LOUISIANA STATE UNIV,MED CTR,SCH MED,NEW ORLEANS,LA 70112

[7] DUPONT CO INC,DEPT NEUROL,WILMINGTON,DE

[8] JOHNS HOPKINS UNIV,DEPT NEUROL,BALTIMORE,MD 21218

[9] UNIV MIAMI,MIAMI,FL 33152

来源：

ANNALS OF NEUROLOGY | 1996年 / 40卷 / 05期

关键词：

D O I：

10.1002/ana.410400515

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Ten laminin alpha 2-deficient patients were identified by both immunofluorescence and immunoblotting (30% of congenital muscular dystrophy patients tested). Three of the laminin alpha 2-deficient patients were carrying a diagnosis of infantile polymyositis prior to immunostaining studies. The clinical features in the 10 merosin-deficient patients were homogeneous, with severe floppiness at birth, delay in achievement of motor milestones, and magnetic resonance imaging findings of white matter changes with normal intelligence. The 10-kb laminin alpha 2-coding sequence was screened for causative mutations by reverse transcriptase-polymerase chain reaction/single-stranded conformational polymorphism analysis in muscle biopsy specimens from 5 patients, followed by automatic sequencing of aberrant conformers. Clear loss-of-function deletion mutations were identified in both alleles of 1 patient. Muscle histopathology in this patient showed a striking inflammatory infiltrate of T cells and B cells. Reexamination of biopsy specimens from other laminin alpha 2-deficient patients showed minor signs of inflammation in each. Based on these findings and the histological and clinical picture suggesting failure of muscle regeneration, a pathogenesis model for this major subset of congenital muscular dystrophy is proposed. Our data show that muscle histopathology showing a neonatal inflammatory process should be considered consistent with congenital muscular dystrophy.

引用

页码：782 / 791

页数：10

共 44 条

[11] LAMININ VARIANTS - WHY, WHERE AND WHEN [J].

ENGVALL, E .

KIDNEY INTERNATIONAL, 1993, 43 (01) :2-6

[12] DISTRIBUTION AND ISOLATION OF 4 LAMININ VARIANTS - TISSUE RESTRICTED DISTRIBUTION OF HETEROTRIMERS ASSEMBLED FROM 5 DIFFERENT SUBUNITS [J].

ENGVALL, E ;

EARWICKER, D ;

HAAPARANTA, T ;

RUOSLAHTI, E ;

SANES, JR .

CELL REGULATION, 1990, 1 (10) :731-740

[13] MEMBRANE ORGANIZATION OF THE DYSTROPHIN-GLYCOPROTEIN COMPLEX [J].

ERVASTI, JM ;

CAMPBELL, KP .

CELL, 1991, 66 (06) :1121-1131

[14] CONGENITAL MUSCULAR-DYSTROPHY (CMD) - A COLLAGEN FORMATIVE DISEASE [J].

FIDZIANSKA, A ;

GOEBEL, HH ;

LENARD, HG ;

HECKMANN, C .

JOURNAL OF THE NEUROLOGICAL SCIENCES, 1982, 55 (01) :79-90

[15]

FUKUYAMA Y, 1981, BRAIN DEV, V13, P1

[16]

Fukuyama Y., 1960, PAEDIATR U TOKYO, V4, P5

[17] ANTIBODIES AGAINST GALACTOSYL (ALPHA-1-]3) GALACTOSE IN CONNECTIVE-TISSUE DISEASES [J].

GABRIELLI, A ;

LEONI, P ;

DANIELI, G ;

HERRMANN, K ;

KRIEG, T ;

WIESLANDER, J .

ARTHRITIS AND RHEUMATISM, 1991, 34 (03) :375-376

[18] RIBONUCLEIC-ACID ISOLATED BY CESIUM-CHLORIDE CENTRIFUGATION [J].

GLISIN, V ;

CRKVENJAKOV, R ;

BYUS, C .

BIOCHEMISTRY, 1974, 13 (12) :2633-2637

[19] MUTATIONS IN THE LAMININ ALPHA-2-CHAIN GENE (LAMA2) CAUSE MEROSIN-DEFICIENT CONGENITAL MUSCULAR-DYSTROPHY [J].

HELBLINGLECLERC, A ;

ZHANG, X ;

TOPALOGLU, H ;

CRUAUD, C ;

TESSON, F ;

WEISSENBACH, J ;

TOME, FMS ;

SCHWARTZ, K ;

FARDEAU, M ;

TRYGGVASON, K ;

GUICHENEY, P .

NATURE GENETICS, 1995, 11 (02) :216-218

[20] LOCALIZATION OF MEROSIN-NEGATIVE CONGENITAL MUSCULAR-DYSTROPHY TO CHROMOSOME 6Q2 BY HOMOZYGOSITY MAPPING [J].

HILLAIRE, D ;

LECLERC, A ;

FAURE, S ;

TOPALOGLU, H ;

CHIANNILKULCHAI, N ;

GUICHENEY, P ;

GRINAS, L ;

LEGOS, P ;

PHILPOT, J ;

EVANGELISTA, T ;

ROUTON, MC ;

MAYER, M ;

PELLISSIER, JF ;

ESTOURNET, B ;

BAROIS, A ;

HENTATI, F ;

FEINGOLD, N ;

BECKMANN, JS ;

DUBOWITZ, V ;

TOME, FMS ;

FARDEAU, M .

HUMAN MOLECULAR GENETICS, 1994, 3 (09) :1657-1661

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