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ACCUMULATION OF MTDNA WITH A MUTATION AT POSITION-3271 IN TRANSFER RNA(LEU)(UUR) GENE INTRODUCED FROM A MELAS PATIENT TO HELA-CELLS LACKING MTDNA RESULTS IN PROGRESSIVE INHIBITION OF MITOCHONDRIAL RESPIRATORY-FUNCTION

被引:68
作者
HAYASHI, JI
OHTA, S
TAKAI, D
MIYABAYASHI, S
SAKUTA, R
GOTO, Y
NONAKA, I
机构
[1] JICHI MED SCH,DEPT BIOCHEM,MINAMI KAWACHI,TOCHIGI 32904,JAPAN
[2] TOHOKU UNIV,SCH MED,DEPT PEDIAT,SENDAI,MIYAGI 980,JAPAN
[3] NATL CTR NEUROL & PSYCHIAT,NATL INST NEUROSCI,DIV ULTRASTRUCTURAL RES,KODAIRA,TOKYO 187,JAPAN
来源
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS | 1993年 / 197卷 / 03期
关键词
D O I
10.1006/bbrc.1993.2584
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
A new mitochondrial DNA (mtDNA) mutation of tRNALeu(UUR) at nucleotide position 3271 (MELAS3271) was determined to be involved in the pathogenic process of mitochondrial diseases MELAS (mitochondnal myopathy, encephalopathy, lactic acidosis and stroke-like episodes) using intercellular transfer of patient-derived mtDNA to mtDNA-less HeLa cells (ρ0 HeLa cells). Cybrid clones containing imported mtDNA exclusively from a MELAS patient with MELAS3271 mtDNA were isolated, and the influence of MELAS3271 mtDNA on mitochondrial translation activity and mitochondrial respiratory complex I enzyme activity were examined. Accumulation of more than 87% MELAS3271 mutant mtDNA in the cybrid clones induced both low complex I activity and abnormal mtDNA-encoded polypeptide synthesis including at least complex I subunit ND6. suggesting involvement of the new MELAS-associated mutation in the pathogenesis. © 1993 Academic Press. All rights reserved.
引用
收藏
页码:1049 / 1055
页数:7
相关论文
共 26 条
[1]   SEQUENCE AND ORGANIZATION OF THE HUMAN MITOCHONDRIAL GENOME [J].
ANDERSON, S ;
BANKIER, AT ;
BARRELL, BG ;
DEBRUIJN, MHL ;
COULSON, AR ;
DROUIN, J ;
EPERON, IC ;
NIERLICH, DP ;
ROE, BA ;
SANGER, F ;
SCHREIER, PH ;
SMITH, AJH ;
STADEN, R ;
YOUNG, IG .
NATURE, 1981, 290 (5806) :457-465
[2]  
BINDOFF LA, 1993, J BIOL CHEM, V268, P19559
[3]  
BREEN GAM, 1986, J BIOL CHEM, V261, P1680
[4]   INVITRO GENETIC TRANSFER OF PROTEIN-SYNTHESIS AND RESPIRATION DEFECTS TO MITOCHONDRIAL DNA-LESS CELLS WITH MYOPATHY-PATIENT MITOCHONDRIA [J].
CHOMYN, A ;
MEOLA, G ;
BRESOLIN, N ;
LAI, ST ;
SCARLATO, G ;
ATTARDI, G .
MOLECULAR AND CELLULAR BIOLOGY, 1991, 11 (04) :2236-2244
[5]   MELAS MUTATION IN MTDNA BINDING-SITE FOR TRANSCRIPTION TERMINATION FACTOR CAUSES DEFECTS IN PROTEIN-SYNTHESIS AND IN RESPIRATION BUT NO CHANGE IN LEVELS OF UPSTREAM AND DOWNSTREAM MATURE TRANSCRIPTS [J].
CHOMYN, A ;
MARTINUZZI, A ;
YONEDA, M ;
DAGA, A ;
HURKO, O ;
JOHNS, D ;
LAI, ST ;
NONAKA, I ;
ANGELINI, C ;
ATTARDI, G .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (10) :4221-4225
[6]   INVITRO TRANSCRIPTION OF HUMAN MITOCHONDRIAL-DNA - ACCURATE TERMINATION REQUIRES A REGION OF DNA-SEQUENCE THAT CAN FUNCTION BIDIRECTIONALLY [J].
CHRISTIANSON, TW ;
CLAYTON, DA .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1986, 83 (17) :6277-6281
[7]   A NEW MTDNA MUTATION ASSOCIATED WITH MITOCHONDRIAL MYOPATHY, ENCEPHALOPATHY, LACTIC-ACIDOSIS AND STROKE-LIKE EPISODES (MELAS) [J].
GOTO, Y ;
NONAKA, I ;
HORAI, S .
BIOCHIMICA ET BIOPHYSICA ACTA, 1991, 1097 (03) :238-240
[8]   MITOCHONDRIAL MYOPATHY, ENCEPHALOPATHY, LACTIC-ACIDOSIS, AND STROKE-LIKE EPISODES (MELAS) - A CORRELATIVE STUDY OF THE CLINICAL-FEATURES AND MITOCHONDRIAL-DNA MUTATION [J].
GOTO, Y ;
HORAI, S ;
MATSUOKA, T ;
KOGA, Y ;
NIHEI, K ;
KOBAYASHI, M ;
NONAKA, I .
NEUROLOGY, 1992, 42 (03) :545-550
[9]   A MUTATION IN THE TRANSFER RNALEU(UUR) GENE ASSOCIATED WITH THE MELAS SUBGROUP OF MITOCHONDRIAL ENCEPHALOMYOPATHIES [J].
GOTO, Y ;
NONAKA, I ;
HORAI, S .
NATURE, 1990, 348 (6302) :651-653
[10]  
HAYASHI JI, 1989, CANCER RES, V49, P4715
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