MYOTUBES FROM TRANSGENIC MDX MICE EXPRESSING FULL-LENGTH DYSTROPHIN SHOW NORMAL CALCIUM REGULATION

被引：24

作者：

DENETCLAW, WF ^{[1
]}

HOPF, FW ^{[1
]}

COX, GA ^{[1
]}

CHAMBERLAIN, JS ^{[1
]}

STEINHARDT, RA ^{[1
]}

机构：

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

来源：

MOLECULAR BIOLOGY OF THE CELL | 1994年 / 5卷 / 10期

关键词：

D O I：

10.1091/mbc.5.10.1159

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

A lack of dystrophin results in muscle degeneration in Duchenne muscular dystrophy. Dystrophin-deficient human and mouse muscle cells have higher resting levels of intracellular free calcium ([Ca2+](i)) and show a related increase in single-channel open probabilities of calcium leak channels. Elevated [Ca2+](i) results in high levels of calcium-dependent proteolysis, which in turn increases calcium leak channel activity. This process could initiate muscle degeneration by further increasing [Ca2+](i) and proteolysis in a-positive feedback loop. Here, we tested the direct effect of restoration of dystrophin on [Ca2+](i) and channel activity in primary myotubes from mdx mice made transgenic for full-length dystrophin. : Transgenic mdx mice have been previously shown to have normal dystrophin localization and no muscle degeneration. Fura-2 calcium measurements and single-channel patch recordings showed that resting [Ca2+](i) levels and open probabilities of calcium leak channels of transgenic mdx myotubes were similar to normal levels and significantly lower than mdx littermate controls (mdx) that lack dystrophin. Thus, restoration of normal calcium regulation in transgenic mdx mice may underlie the resulting absence of degeneration.

引用

页码：1159 / 1167

页数：9

共 47 条

[1] THE CA SIGNAL FROM FURA-2 LOADED MAST-CELLS DEPENDS STRONGLY ON THE METHOD OF DYE-LOADING
ALMERS, W
NEHER, E
[J]. FEBS LETTERS, 1985, 192 (01) : 13 - 18
[2] BAKKER AJ, 1993, J PHYSIOL-LONDON, V460, P1
[3] MUSCLE CALCIUM AND MAGNESIUM CONTENT IN DUCHENNE MUSCULAR-DYSTROPHY
BERTORINI, TE
BHATTACHARYA, SK
PALMIERI, GMA
CHESNEY, CM
PIFER, D
BAKER, B
[J]. NEUROLOGY, 1982, 32 (10) : 1088 - 1092
[4] 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
[5] ASSOCIATION OF DYSTROPHIN AND AN INTEGRAL MEMBRANE GLYCOPROTEIN
CAMPBELL, KP
KAHL, SD
[J]. NATURE, 1989, 338 (6212) : 259 - 262
[6] MUSCULAR-DYSTROPHY IN THE MDX MOUSE - HISTOPATHOLOGY OF THE SOLEUS AND EXTENSOR DIGITORUM LONGUS MUSCLES
CARNWATH, JW
SHOTTON, DM
[J]. JOURNAL OF THE NEUROLOGICAL SCIENCES, 1987, 80 (01) : 39 - 54
[7] Colquhoun D., 1983, SINGLE CHANNEL RECOR, Vsecond, P191
[8] OVEREXPRESSION OF DYSTROPHIN IN TRANSGENIC MDX MICE ELIMINATES DYSTROPHIC SYMPTOMS WITHOUT TOXICITY
COX, GA
COLE, NM
MATSUMURA, K
PHELPS, SF
HAUSCHKA, SD
CAMPBELL, KP
FAULKNER, JA
CHAMBERLAIN, JS
[J]. NATURE, 1993, 364 (6439) : 725 - 729
[9] HETEROKARYON MYOTUBES WITH NORMAL MOUSE AND DUCHENNE NUCLEI EXHIBIT SARCOLEMMAL DYSTROPHIN STAINING AND EFFICIENT INTRACELLULAR FREE CALCIUM CONTROL
DENETCLAW, WF
BI, GQ
PHAM, DV
STEINHARDT, RA
[J]. MOLECULAR BIOLOGY OF THE CELL, 1993, 4 (09) : 963 - 972
[10] SATELLITE CELLS FROM DYSTROPHIC (MDX) MOUSE MUSCLE ARE STIMULATED BY FIBROBLAST GROWTH-FACTOR INVITRO
DIMARIO, J
STROHMAN, RC
[J]. DIFFERENTIATION, 1988, 39 (01) : 42 - 49

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