PREVENTION OF DYSTROPHIC PATHOLOGY IN MDX MICE BY A TRUNCATED DYSTROPHIN ISOFORM

被引：80

作者：

RAFAEL, JA

SUNADA, Y

COLE, NM

CAMPBELL, KP

FAULKNER, JA

CHAMBERLAIN, JS

机构：

[1] UNIV MICHIGAN,SCH MED,DEPT HUMAN GENET,ANN ARBOR,MI 48109

[2] UNIV MICHIGAN,SCH MED,CTR HUMAN GENOME,ANN ARBOR,MI 48109

[3] UNIV MICHIGAN,SCH MED,DEPT PHYSIOL,ANN ARBOR,MI 48109

[4] UNIV MICHIGAN,SCH MED,INST GERONTOL,ANN ARBOR,MI 48109

[5] UNIV IOWA,COLL MED,HOWARD HUGHES MED INST,DEPT PHYSIOL & BIOPHYS,IOWA CITY,IA 52242

来源：

HUMAN MOLECULAR GENETICS | 1994年 / 3卷 / 10期

关键词：

D O I：

10.1093/hmg/3.10.1725

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：

The C-terminal domain of dystrophin is alternatively spliced to produce a variety of tissue and developmental stage-specific isoforms. Recent studies suggest that the C-terminal domain binds to the dystrophin-associated glycoprotein complex (DGC) in muscle, but little is known about the functional significance of the alternative splicing or what role individual isoforms may play in specific tissues. The major dystrophin transcript in brain lacks exons 71 - 74, and encodes an isoform not observed in skeletal muscle. To explore the capacity of this truncated isoform to function in muscle, we have generated transgenic mice expressing a murine dystrophin mini-gene missing exons 71 - 74. Uniform expression of this construct on a mutant mdx mouse background results in normal muscle morphology and physiology, and prevents the development of muscular dystrophy. These mice also display normal expression and localization of the DGC, suggesting that the alternatively spliced exons are not required for dystrophin function in skeletal muscle. An additional line of mice was analyzed that had a mosaic pattern of expression. These mice display a markedly milder phenotype than mdx mice, despite the expression of dystrophin in only half the muscle fibers. These results indicate that viral delivery of dystrophin to a simple majority of fibers in a muscle group would greatly reduce the dystrophic pathology associated with Duchenne muscular dystrophy.

引用

页码：1725 / 1733

页数：9

共 29 条

[1] HUMAN DYSTROPHIN EXPRESSION IN MDX MICE AFTER INTRAMUSCULAR INJECTION OF DNA CONSTRUCTS
ACSADI, G
DICKSON, G
LOVE, DR
JANI, A
WALSH, FS
GURUSINGHE, A
WOLFF, JA
DAVIES, KE
[J]. NATURE, 1991, 352 (6338) : 815 - 818
[2] THE STRUCTURAL AND FUNCTIONAL DIVERSITY OF DYSTROPHIN
AHN, AH
KUNKEL, LM
[J]. NATURE GENETICS, 1993, 3 (04) : 283 - 291
[3] AZIBI K, 1993, HUM MOL GENET, V2, P1423
[4] BEGGS AH, 1991, AM J HUM GENET, V49, P54
[5] PACKAGING CAPACITY AND STABILITY OF HUMAN ADENOVIRUS TYPE-5 VECTORS
BETT, AJ
PREVEC, L
GRAHAM, FL
[J]. JOURNAL OF VIROLOGY, 1993, 67 (10) : 5911 - 5921
[6] HUMAN AND MURINE DYSTROPHIN MESSENGER-RNA TRANSCRIPTS ARE DIFFERENTIALLY EXPRESSED DURING SKELETAL-MUSCLE, HEART, AND BRAIN-DEVELOPMENT
BIES, RD
PHELPS, SF
CORTEZ, MD
ROBERTS, R
CASKEY, CT
CHAMBERLAIN, JS
[J]. NUCLEIC ACIDS RESEARCH, 1992, 20 (07) : 1725 - 1731
[7] CONTRACTILE PROPERTIES OF SKELETAL-MUSCLES FROM YOUNG, ADULT AND AGED MICE
BROOKS, SV
FAULKNER, JA
[J]. JOURNAL OF PHYSIOLOGY-LONDON, 1988, 404 : 71 - 82
[8] X-CHROMOSOME-LINKED MUSCULAR-DYSTROPHY (MDX) IN THE MOUSE
BULFIELD, G
SILLER, WG
WIGHT, PAL
MOORE, KJ
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1984, 81 (04): : 1189 - 1192
[9] RECOVERY OF INDUCED MUTATIONS FOR X-CHROMOSOME-LINKED MUSCULAR-DYSTROPHY IN MICE
CHAPMAN, VM
MILLER, DR
ARMSTRONG, D
CASKEY, CT
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (04) : 1292 - 1296
[10] NEW MDX MUTATION DISRUPTS EXPRESSION OF MUSCLE AND NONMUSCLE ISOFORMS OF DYSTROPHIN
COX, GA
PHELPS, SF
CHAPMAN, VM
CHAMBERLAIN, JS
[J]. NATURE GENETICS, 1993, 4 (01) : 87 - 93

← 1 2 3 →