Leigh syndrome: Clinical features and biochemical and DNA abnormalities

被引：581

作者：

Rahman, S

Blok, RB

Dahl, HHM

Danks, DM

Kirby, DM

Chow, CW

Christodoulou, J

Thorburn, DR

机构：

[1] ROYAL CHILDRENS HOSP,MURDOCH INST RES BIRTH DEFECTS,MELBOURNE,VIC,AUSTRALIA

[2] ROYAL CHILDRENS HOSP,DEPT PATHOL ANAT,MELBOURNE,VIC,AUSTRALIA

[3] CHILDRENS HOSP,DEPT PAEDIAT & CHILD HLTH,SYDNEY,NSW,AUSTRALIA

来源：

ANNALS OF NEUROLOGY | 1996年 / 39卷 / 03期

关键词：

D O I：

10.1002/ana.410390311

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

We investigated the etiology of Leigh syndrome in 67 Australian cases from 56 pedigrees, 35 with a firm diagnosis and 32 with some atypical features. Biochemical or DNA defects were determined in both groups, ie, 80% in the tightly defined group and 41% in the ''Leigh-like'' group. Eleven patients had mitochondrial DNA point mutations (nucleotide [nt] 8993 T to G, nt 8993 T to C, or nt 8344 A to G) and 1 Leigh-like patient had a heteroplasmic deletion. Twenty-nine patients had enzyme defects, ie, 13 respiratory chain complex I, 9 complex IV, and 7 pyruvate dehydrogenase complex (PDHC). Complex I deficiency is more common than recognized previously. Six PDHC-deficient patients had mutations in the X-chromosomal gene encoding the E1 alpha subunit of PDHC. Parental consanguinity suggested autosomal recessive inheritance in two complex IV-deficient sibships. We found no strong correlation between the clinical features and basic defects. An assumption of autosomal recessive inheritance (frequently made in the past) would have been wrong in nearly one-half (11 of 28 tightly defined and 18 of 41 total patients) of those in whom a cause was found. A specific defect must be identified if reliable genetic counseling is to be provided.

引用

页码：343 / 351

页数：9

共 50 条

[1] SEQUENCE AND ORGANIZATION OF THE HUMAN MITOCHONDRIAL GENOME
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
[J]. NATURE, 1981, 290 (5806) : 457 - 465
[2] PYRUVATE-CARBOXYLASE AND PHOSPHOENOLPYRUVATE CARBOXYKINASE ACTIVITY IN LEUKOCYTES AND FIBROBLASTS FROM A PATIENT WITH PYRUVATE-CARBOXYLASE DEFICIENCY
ATKIN, BM
UTTER, MF
WEINBERG, MB
[J]. PEDIATRIC RESEARCH, 1979, 13 (01) : 38 - 43
[3] X-LINKED LEIGHS SYNDROME
BENKE, PJ
PARKER, JC
LUBS, ML
BENKENDORF, J
FEUER, AE
[J]. HUMAN GENETICS, 1982, 62 (01) : 52 - 59
[4] CLINICAL SPECTRUM OF MITOCHONDRIAL-DNA MUTATION AT BASE PAIR-8344
BERKOVIC, SF
SHOUBRIDGE, EA
ANDERMANN, F
ANDERMANN, E
CARPENTER, S
KARPATI, G
[J]. LANCET, 1991, 338 (8764) : 457 - 457
[5] MULTIPLE DEFECTS OF THE MITOCHONDRIAL RESPIRATORY-CHAIN IN A MITOCHONDRIAL ENCEPHALOPATHY (MERRF) - A CLINICAL, BIOCHEMICAL AND MOLECULAR STUDY
BINDOFF, LA
DESNUELLE, C
BIRCHMACHIN, MA
PELLISSIER, JF
SERRATRICE, G
DRAVET, C
BUREAU, M
HOWELL, N
TURNBULL, DM
[J]. JOURNAL OF THE NEUROLOGICAL SCIENCES, 1991, 102 (01) : 17 - 24
[6] AN EVALUATION OF THE MEASUREMENT OF THE ACTIVITIES OF COMPLEXES I-IV IN THE RESPIRATORY-CHAIN OF HUMAN SKELETAL-MUSCLE MITOCHONDRIA
BIRCHMACHIN, MA
BRIGGS, HL
SABORIDO, AA
BINDOFF, LA
TURNBULL, DM
[J]. BIOCHEMICAL MEDICINE AND METABOLIC BIOLOGY, 1994, 51 (01): : 35 - 42
[7] BLOK RB, 1995, HUM GENET, V95, P75
[8] MTDNA DELETION IN A PATIENT WITH SYMPTOMS OF MITOCHONDRIAL CYTOPATHY BUT WITHOUT RAGGED-RED FIBERS
BLOK, RB
THORBURN, DR
DANKS, DM
DAHL, HHM
[J]. BIOCHEMICAL AND MOLECULAR MEDICINE, 1995, 56 (01) : 26 - 30
[9] ISOLATION AND CHARACTERIZATION OF MITOCHONDRIA FROM HUMAN B-LYMPHOBLASTOID CELL-LINES
BOURGERON, T
CHRETIEN, D
ROTIG, A
MUNNICH, A
RUSTIN, P
[J]. BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1992, 186 (01) : 16 - 23
[10] X-CHROMOSOME LOCALIZATION OF THE FUNCTIONAL GENE FOR THE E1-ALPHA SUBUNIT OF THE HUMAN PYRUVATE-DEHYDROGENASE COMPLEX
BROWN, RM
DAHL, HHM
BROWN, GK
[J]. GENOMICS, 1989, 4 (02) : 174 - 181

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