LOCALIZATION OF MEROSIN-NEGATIVE CONGENITAL MUSCULAR-DYSTROPHY TO CHROMOSOME 6Q2 BY HOMOZYGOSITY MAPPING

被引：187

作者：

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

机构：

[1] INSERM,U153,F-75005 PARIS,FRANCE

[2] GENETHON,F-91002 EVRY,FRANCE

[3] CNRS,ERS 064,F-75005 PARIS,FRANCE

[4] HACETTEPE CHILDRENS HOSP MED CTR,DEPT PAEDIAT NEUROL,ANKARA 06100,TURKEY

[5] HAMMERSMITH HOSP,ROYAL POSTGRAD MED SCH,DEPT PAEDIAT & NEONATAL MED,LONDON W12 0NN,ENGLAND

[6] HOP ST VINCENT DE PAUL,SERV NEUROPEDIAT,F-75014 PARIS,FRANCE

[7] HOP ADULTES TIMONE,SERV ANAT PATHOL & NEUROPATHOL,F-13005 MARSEILLE,FRANCE

[8] HOP RAY POINCARE,GARCHES,FRANCE

[9] INST NATL NEUROL,TUNIS,TUNISIA

[10] INSERM,U155,F-75016 PARIS,FRANCE

[11] CTR ETUD POLYMORPHISME HUMAIN,F-75010 PARIS,FRANCE

来源：

HUMAN MOLECULAR GENETICS | 1994年 / 3卷 / 09期

关键词：

D O I：

10.1093/hmg/3.9.1657

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Congenital muscular dystrophies (CMD) are autosomal recessive, heterogeneous disorders. The commonest forms are the Fukuyama CMD (FCMD), associated with mental retardation and structural brain anomalies, and classical (occidental) CMD, with pure muscle expression. FCMD has been localized to chromosome 9q31 - q33. Following the discovery of merosin deficiency in some CMD cases, we have localized, by homozygosity mapping and linkage analysis(Zmax = 5.6; theta = 0.0 for marker AFM127xb2) in four merosin-negative families a CMD gene in a 16 cM region of chromosome 6q2 in the region of the laminin M chain gene. In three consanguineous, merosin-positive, CMD families there was no linkage to either chromosome 6q2 or 9q31 - q33.

引用

页码：1657 / 1661

页数：5

共 32 条

[1] 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
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
[J]. PROCEEDINGS OF THE JAPAN ACADEMY SERIES B-PHYSICAL AND BIOLOGICAL SCIENCES, 1993, 69 (10): : 259 - 264
[2] Banker BQ, 1994, MYOLOGY, V2
[3] BENHAMIDA C, 1993, NAT GENET, V5, P195
[4] NEURAL ABNORMALITIES IN DYSTROPHIC MOUSE
BRADLEY, WG
JENKISON, M
[J]. JOURNAL OF THE NEUROLOGICAL SCIENCES, 1975, 25 (02) : 249 - 255
[5] A ROLE FOR COLLAGEN IN THE PATHOGENESIS OF MUSCULAR-DYSTROPHY
DUANCE, VC
STEPHENS, HR
DUNN, M
BAILEY, AJ
DUBOWITZ, V
[J]. NATURE, 1980, 284 (5755) : 470 - 472
[6] 22ND ENMC SPONSORED WORKSHOP ON CONGENITAL MUSCULAR-DYSTROPHY HELD IN BAARN, THE NETHERLANDS, 14-16 MAY 1993
DUBOWITZ, V
[J]. NEUROMUSCULAR DISORDERS, 1994, 4 (01) : 75 - 81
[7] DUBOWITZ V, 1978, MUSCLE DISORDERS CHI, P59
[8] LAMININ VARIANTS - WHY, WHERE AND WHEN
ENGVALL, E
[J]. KIDNEY INTERNATIONAL, 1993, 43 (01) : 2 - 6
[9] DISTRIBUTION AND ISOLATION OF 4 LAMININ VARIANTS - TISSUE RESTRICTED DISTRIBUTION OF HETEROTRIMERS ASSEMBLED FROM 5 DIFFERENT SUBUNITS
ENGVALL, E
EARWICKER, D
HAAPARANTA, T
RUOSLAHTI, E
SANES, JR
[J]. CELL REGULATION, 1990, 1 (10): : 731 - 740
[10] MEMBRANE ORGANIZATION OF THE DYSTROPHIN-GLYCOPROTEIN COMPLEX
ERVASTI, JM
CAMPBELL, KP
[J]. CELL, 1991, 66 (06) : 1121 - 1131

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