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A SEVERE MUSCULAR-DYSTROPHY PATIENT WITH AN INTERNALLY DELETED VERY SHORT (110 KD) DYSTROPHIN - PRESENCE OF THE BINDING-SITE FOR DYSTROPHIN-ASSOCIATED GLYCOPROTEIN (DAG) MAY NOT BE ENOUGH FOR PHYSIOLOGICAL-FUNCTION OF DYSTROPHIN
被引:10
作者:
ARIKAWAHIRASAWA, E
KOGA, R
TSUKAHARA, T
NONAKA, I
MITSUDOME, A
GOTO, K
BEGGS, AH
ARAHATA, K
机构:
[1] NATL INST NEUROSCI,NCNP,DEPT NEUROMUSCULAR RES,KODAIRA 187,TOKYO,JAPAN
[2] JUNTENDO UNIV,SCH MED,DEPT NEUROL,TOKYO 113,JAPAN
[3] FUKUOKA UNIV,SCH MED,DEPT PEDIAT,FUKUOKA 81401,JAPAN
[4] CHILDRENS HOSP,DIV GENET,BOSTON,MA 02115
关键词:
DYSTROPHIN;
ACTIN-BINDING DOMAIN;
ALTERNATIVE SPLICING;
DYSTROPHIN-ASSOCIATED GLYCOPROTEIN (DAG);
MUSCULAR DYSTROPHY;
D O I:
10.1016/0960-8966(94)00087-P
中图分类号:
R74 [神经病学与精神病学];
学科分类号:
摘要:
We report a 4-yr and 5-month-old boy with severe clinical features of an early-onset Duchenne muscular dystrophy, who had a very short (110 kDa) dystrophin at the sarcolemma. The patient had a large deletion (exons 2-44) of the dystrophin gene which was predicted to cause a reading frame shift. Sequence analysis of dystrophin mRNA in muscle revealed an alternatively spliced gene product from exons 1 to 51 that caused restoration of the reading frame, in addition to an mRNA corresponding to the DNA deletion. A consistent result was obtained by immunocytochemical analysis of muscle; i.e. positive staining for dystrophin at the sarcolemma using antibodies against the C-terminus, cysteine-rich region and last three of 24 repeat units of the central rod-domain, but not for the remaining antibodies for dystrophin that recognize the N-terminal and proximal rod-domains. Immunostaining for dystrophin-associated glycoproteins (DAGs: 43 and 50 K) and merosin were preserved. Utrophin staining was positive but fainter than other DMD muscles. These results suggest that an extremely short dystrophin lacking the entire actin-binding site in the N-terminus cannot function properly even if the protein possesses the putative DAG-binding cysteine-rich and the C-terminal domains, and still has an ability to associate with sarcolemmal membrane.
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页码:429 / 438
页数:10
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