MECHANISM OF MUSCLE WASTING IN MYOTONIC-DYSTROPHY

被引：24

作者：

GRIGGS, RC ^{[1
]}

JOZEFOWICZ, R ^{[1
]}

KINGSTON, W ^{[1
]}

NAIR, KS ^{[1
]}

HERR, BE ^{[1
]}

HALLIDAY, D ^{[1
]}

机构：

[1] CLIN RES CTR,CLIN RES GRP,HARROW HA1 3UJ,MIDDX,ENGLAND

来源：

ANNALS OF NEUROLOGY | 1990年 / 27卷 / 05期

关键词：

D O I：

10.1002/ana.410270509

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Myotonic dystrophy is associated with progressive muscular atrophy. In order to determine the mechanism of muscle wasting in this condition, we measured fractional mixed skeletal muscle protein synthesis in the postabsorptive state in 8 patients with myotonic dystrophy, and compared the results with those of 10 normal subjects. Fractional muscle protein synthesis was determined by measuring the increment of 13C leucine in mixed skeletal muscle protein obtained by needle biopsy from the quadriceps muscle during a primed‐continuous infusion of L‐(1‐13C) leucine. We used plasma 13C α‐ketoisocaproate (representing intracellular leucine labeling) as the precursor pool for the calculation of fractional muscle protein synthesis and leucine kinetics. Fractional muscle protein synthesis was depressed in the patients with myotonic dystrophy (28% decrease, p < 0.02). Leucine flux, leucine oxidation, and the nonoxidative portion of leucine flux were not different between the patients with myotonic dystrophy and the normal control subjects. Muscle atrophy in myotonic dystrophy reflects a selective decrease in muscle protein synthesis without any similar decrease in nonmuscle protein synthesis. This decrease may result from an impaired end‐organ response to anabolic hormones or substrates. Copyright © 1990 American Neurological Association

引用

页码：505 / 512

页数：8

共 51 条

[1] USE OF A HEATED SUPERFICIAL HAND VEIN AS AN ALTERNATIVE SITE FOR THE MEASUREMENT OF AMINO-ACID-CONCENTRATIONS AND FOR THE STUDY OF GLUCOSE AND ALANINE KINETICS IN MAN [J].

ABUMRAD, NN ;

RABIN, D ;

DIAMOND, MP ;

LACY, WW .

METABOLISM-CLINICAL AND EXPERIMENTAL, 1981, 30 (09) :936-940

[2] A NEW PROBE FOR THE DIAGNOSIS OF MYOTONIC MUSCULAR-DYSTROPHY [J].

BARTLETT, RJ ;

PERICAKVANCE, MA ;

YAMAOKA, L ;

GILBERT, J ;

HERBSTREITH, M ;

HUNG, WY ;

LEE, JE ;

MOHANDAS, T ;

BRUNS, G ;

LABERGE, C ;

THIBAULT, MC ;

ROSS, D ;

ROSES, AD .

SCIENCE, 1987, 235 (4796) :1648-1650

[3] MUSCLE FIBER TYPES - HOW MANY AND WHAT KIND [J].

BROOKE, MH ;

KAISER, KK .

ARCHIVES OF NEUROLOGY, 1970, 23 (04) :369-&

[4] HISTOGRAPHIC ANALYSIS OF HUMAN MUCLE BIOPSIES WITH REGARD TO FIBER TYPES .3. MYOTONIAS MYASTHENIA GRAVIS AND HYPOKALEMIC PERIODIC PARALYSIS [J].

BROOKE, MH ;

ENGEL, WK .

NEUROLOGY, 1969, 19 (05) :469-&

[5] NEEDLE-BIOPSY OF SKELETAL-MUSCLE IN THE DIAGNOSIS OF MYOPATHY AND THE CLINICAL-STUDY OF MUSCLE FUNCTION AND REPAIR [J].

EDWARDS, R ;

YOUNG, A ;

WILES, M .

NEW ENGLAND JOURNAL OF MEDICINE, 1980, 302 (05) :261-271

[6]

ENGEL WK, 1971, CALIF MED, V114, P32

[7]

FORBES GB, 1976, AM J CLIN PATHOL, V35, P83

[8] ANALYSIS OF (1-C13)LEUCINE AND (C-13)KIC IN PLASMA BY CAPILLARY GAS-CHROMATOGRAPHY MASS-SPECTROMETRY IN PROTEIN-TURNOVER STUDIES [J].

FORD, GC ;

CHENG, KN ;

HALLIDAY, D .

BIOMEDICAL MASS SPECTROMETRY, 1985, 12 (08) :432-436

[9] 3-POINT LINKAGE ANALYSIS EMPLOYING C-3 AND 19CEN MARKERS ASSIGNS THE MYOTONIC-DYSTROPHY GENE TO 19Q [J].

FRIEDRICH, U ;

BRUNNER, H ;

SMEETS, D ;

LAMBERMON, E ;

ROPERS, HH .

HUMAN GENETICS, 1987, 75 (03) :291-293

[10] INSULIN-MEDIATED REDUCTION OF WHOLE-BODY PROTEIN BREAKDOWN - DOSE-RESPONSE EFFECTS ON LEUCINE METABOLISM IN POST-ABSORPTIVE MEN [J].

FUKAGAWA, NK ;

MINAKER, KL ;

ROWE, JW ;

GOODMAN, MN ;

MATTHEWS, DE ;

BIER, DM ;

YOUNG, VR .

JOURNAL OF CLINICAL INVESTIGATION, 1985, 76 (06) :2306-2311

← 1 2 3 4 5 6 →