MATERNALLY INHERITED HEARING-LOSS, ATAXIA AND MYOCLONUS ASSOCIATED WITH A NOVEL POINT MUTATION IN MITOCHONDRIAL TRNA(SER(UCN)) GENE

被引：178

作者：

TIRANTI, V

CHARIOT, P

CARELLA, F

TOSCANO, A

SOLIVERI, P

GIRLANDA, P

CARRARA, F

FRATTA, GM

REID, FM

MARIOTTI, C

ZEVIANI, M

机构：

[1] NATL NEUROL INST CARLO BESTA,DIV BIOCHEM & GENET,MILAN,ITALY

[2] NATL NEUROL INST CARLO BESTA,DIV NEUROL,MILAN,ITALY

[3] STATE UNIV,SCH MED,NEUROL CLIN,MESSINA,ITALY

[4] SAN GIOVANNI ROTONDO,CSS,IRCCS,DIV NEUROL,FOGGIA,ITALY

[5] UNIV GLASGOW,FAC SCI,ROBERTSON INST BIOTECHNOL,GLASGOW G61 1BD,LANARK,SCOTLAND

来源：

HUMAN MOLECULAR GENETICS | 1995年 / 4卷 / 08期

关键词：

D O I：

10.1093/hmg/4.8.1421

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：

We report on a new maternally-inherited syndrome characterized by a combination of sensorineural hearing loss, ataxia and myoclonus in a large kindred from Sicily, Hearing loss was the most widespread and sometimes the only symptom found in family members. Sequence analysis of the mitochondrial DNA regions encompassing the tRNA genes revealed the presence of a heteroplasmic insertion at nucleotide position 7472. The insertion adds a seventh cytosine to a six-cytosine run that is part of the mitochondrial tRNA(Ser(UCN)) gene, Conformational analysis showed that this mutation is likely to alter the structure of the T Psi C loop in the tRNA(Ser(UCN)) clover leaf secondary structure, Moreover, the degree of heteroplasmy in blood and muscle was correlated with the clinical phenotype, and homoplasmic mutant cybrids showed decreased complex I activity, low oxygen consumption and high lactic acid output, indicating faulty oxidative phosphorylation, Finally, mutation was absent in 381 unrelated maternal lineages, suggesting specific segregation with the disease. We propose that the C7472 insertion-mutation is pathogenic, and etiologically related to hearing loss and other symptoms that define a novel maternally-inherited clinical entity.

引用

页码：1421 / 1427

页数：7

共 32 条

[11] HUMAN-CELLS LACKING MTDNA - REPOPULATION WITH EXOGENOUS MITOCHONDRIA BY COMPLEMENTATION
KING, MP
ATTARDI, G
[J]. SCIENCE, 1989, 246 (4929) : 500 - 503
[12] DEFECTS IN MITOCHONDRIAL PROTEIN-SYNTHESIS AND RESPIRATORY-CHAIN ACTIVITY SEGREGATE WITH THE TRANSFER RNA(LEU)(UUR) MUTATION ASSOCIATED WITH MITOCHONDRIAL MYOPATHY, ENCEPHALOPATHY, LACTIC-ACIDOSIS, AND STROKE-LIKE EPISODES
KING, MP
KOGA, Y
DAVIDSON, M
SCHON, EA
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1992, 12 (02) : 480 - 490
[13] LUDWIG EH, 1989, AM J HUM GENET, V45, P458
[14] DEFECTIVE RESPIRATORY CAPACITY AND MITOCHONDRIAL PROTEIN-SYNTHESIS IN TRANSFORMANT CYBRIDS HARBORING THE TRNA(LEU(UUR)) MUTATION ASSOCIATED WITH MATERNALLY INHERITED MYOPATHY AND CARDIOMYOPATHY
MARIOTTI, C
TIRANTI, V
CARRARA, F
DALLAPICCOLA, B
DIDONATO, S
ZEVIANI, M
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1994, 93 (03) : 1102 - 1107
[15] RECOMBINATION VIA FLANKING DIRECT REPEATS IS A MAJOR CAUSE OF LARGE-SCALE DELETIONS OF HUMAN MITOCHONDRIAL-DNA
MITA, S
RIZZUTO, R
MORAES, CT
SHANSKE, S
ARNAUDO, E
FABRIZI, GM
KOGA, Y
DIMAURO, S
SCHON, EA
[J]. NUCLEIC ACIDS RESEARCH, 1990, 18 (03) : 561 - 567
[16] Noll F., 1974, METHOD ENZYMAT AN, P1475
[17] THE CLINICAL-FEATURES OF MITOCHONDRIAL MYOPATHY
PETTY, RKH
HARDING, AE
MORGANHUGHES, JA
[J]. BRAIN, 1986, 109 : 915 - 938
[18] MITOCHONDRIAL RIBOSOMAL-RNA MUTATION ASSOCIATED WITH BOTH ANTIBIOTIC-INDUCED AND NON-SYNDROMIC DEAFNESS
PREZANT, TR
AGAPIAN, JV
BOHLMAN, MC
BU, XD
OZTAS, S
QIU, WQ
ARNOS, KS
CORTOPASSI, GA
JABER, L
ROTTER, JI
SHOHAT, M
FISCHELGHODSIAN, N
[J]. NATURE GENETICS, 1993, 4 (03) : 289 - 294
[19] A NOVEL MITOCHONDRIAL POINT MUTATION IN A MATERNAL PEDIGREE WITH SENSORINEURAL DEAFNESS
REID, FM
VERNHAM, GA
JACOBS, HT
[J]. HUMAN MUTATION, 1994, 3 (03) : 243 - 247
[20] BIOCHEMICAL AND MOLECULAR INVESTIGATIONS IN RESPIRATORY-CHAIN DEFICIENCIES
RUSTIN, P
CHRETIEN, D
BOURGERON, T
GERARD, B
ROTIG, A
SAUDUBRAY, JM
MUNNICH, A
[J]. CLINICA CHIMICA ACTA, 1994, 228 (01) : 35 - 51

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