HUMAN DYSTROPHIN EXPRESSION IN MDX MICE AFTER INTRAMUSCULAR INJECTION OF DNA CONSTRUCTS

被引:391
作者
ACSADI, G
DICKSON, G
LOVE, DR
JANI, A
WALSH, FS
GURUSINGHE, A
WOLFF, JA
DAVIES, KE
机构
[1] UNIV WISCONSIN,WAISMAN CTR MENTAL RETARDAT & HUMAN DEV,DEPT PEDIAT,MADISON,WI 53706
[2] UNIV WISCONSIN,WAISMAN CTR MENTAL RETARDAT & HUMAN DEV,DEPT MED GENET,MADISON,WI 53706
[3] UNITED MED & DENT SCH GUYS & ST THOMAS HOSP,GUYS HOSP,DEPT EXPTL PATHOL,LONDON SE1 9RT,ENGLAND
[4] JOHN RADCLIFFE HOSP,INST MOLEC MED,MOLEC GENET GRP,OXFORD OX3 9DU,ENGLAND
来源
NATURE | 1991年 / 352卷 / 6338期
关键词
D O I
10.1038/352815a0
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
DUCHENNE'S muscular dystrophy (DMD), which affects one in 3,500 males, causes progressive myopathy of skeletal and cardiac muscles and premature death 1. One approach to treatment would be to introduce the normal dystrophin gene into diseased muscle cells. When pure plasmid DNA is injected into rodent skeletal 2 or cardiac muscle 3-5, the cells express reporter genes. We now show that a 12-kilobase full-length human dystrophin complementary DNA gene and a 6.3-kilobase Becker-like gene 6 can be expressed in cultured cells and in vivo. When the human dystrophin expression plasmids are injected intramuscularly into dystrophin-deficient mdx mice, the human dystrophin proteins are present in the cytoplasm and sarcolemma of approximately 1% of the myofibres. Myofibres expressing human dystrophin contain an increased proportion of peripheral nuclei. The results indicate that transfer of the dystrophin gene into the myofibres of DMD patients could be beneficial, but a larger number of genetically modified myofibres will be necessary for clinical efficacy.
引用
收藏
页码:815 / 818
页数:4
相关论文
共 30 条
[1]  
ACSADI G, 1991, NEW BIOL, V3, P71
[2]   THE MDX MOUSE SKELETAL-MUSCLE MYOPATHY .1. A HISTOLOGICAL, MORPHOMETRIC AND BIOCHEMICAL INVESTIGATION [J].
COULTON, GR ;
MORGAN, JE ;
PARTRIDGE, TA ;
SLOPER, JC .
NEUROPATHOLOGY AND APPLIED NEUROBIOLOGY, 1988, 14 (01) :53-70
[3]  
DICKSON G, IN PRESS HUMAN GENET
[4]   SPECIFICITY OF DYSTROPHIN ANALYSIS IMPROVED WITH MONOCLONAL-ANTIBODIES [J].
ELLIS, JM ;
MAN, NT ;
MORRIS, GE ;
GINJAAR, IB ;
MOORMAN, AFM ;
VANOMMEN, GJB .
LANCET, 1990, 336 (8719) :881-882
[5]   VERY MILD MUSCULAR-DYSTROPHY ASSOCIATED WITH THE DELETION OF 46-PERCENT OF DYSTROPHIN [J].
ENGLAND, SB ;
NICHOLSON, LVB ;
JOHNSON, MA ;
FORREST, SM ;
LOVE, DR ;
ZUBRZYCKAGAARN, EE ;
BULMAN, DE ;
HARRIS, JB ;
DAVIES, KE .
NATURE, 1990, 343 (6254) :180-182
[6]   DEFICIENCY OF A GLYCOPROTEIN COMPONENT OF THE DYSTROPHIN COMPLEX IN DYSTROPHIC MUSCLE [J].
ERVASTI, JM ;
OHLENDIECK, K ;
KAHL, SD ;
GAVER, MG ;
CAMPBELL, KP .
NATURE, 1990, 345 (6273) :315-319
[7]   LIPOFECTION - A HIGHLY EFFICIENT, LIPID-MEDIATED DNA-TRANSFECTION PROCEDURE [J].
FELGNER, PL ;
GADEK, TR ;
HOLM, M ;
ROMAN, R ;
CHAN, HW ;
WENZ, M ;
NORTHROP, JP ;
RINGOLD, GM ;
DANIELSEN, M .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1987, 84 (21) :7413-7417
[8]  
FORREST S M, 1988, Genomics, V2, P109, DOI 10.1016/0888-7543(88)90091-2
[9]   FACTORS AFFECTING POLYACRYLAMIDE-GEL ELECTROPHORESIS AND ELECTROBLOTTING OF HIGH-MOLECULAR-WEIGHT MYOFIBRILLAR PROTEINS [J].
FRITZ, JD ;
SWARTZ, DR ;
GREASER, ML .
ANALYTICAL BIOCHEMISTRY, 1989, 180 (02) :205-210
[10]   THE ROUS-SARCOMA VIRUS LONG TERMINAL REPEAT IS A STRONG PROMOTER WHEN INTRODUCED INTO A VARIETY OF EUKARYOTIC CELLS BY DNA-MEDIATED TRANSFECTION [J].
GORMAN, CM ;
MERLINO, GT ;
WILLINGHAM, MC ;
PASTAN, I ;
HOWARD, BH .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1982, 79 (22) :6777-6781
123