MUTATIONS IN CU/ZN SUPEROXIDE-DISMUTASE GENE ARE ASSOCIATED WITH FAMILIAL AMYOTROPHIC-LATERAL-SCLEROSIS

被引：5495

作者：

ROSEN, DR

SIDDIQUE, T

PATTERSON, D

FIGLEWICZ, DA

SAPP, P

HENTATI, A

DONALDSON, D

GOTO, J

OREGAN, JP

DENG, HX

RAHMANI, Z

KRIZUS, A

MCKENNAYASEK, D

CAYABYAB, A

GASTON, SM

BERGER, R

TANZI, RE

HALPERIN, JJ

HERZFELDT, B

VANDENBERGH, R

HUNG, WY

BIRD, T

DENG, G

MULDER, DW

SMYTH, C

LAING, NG

SORIANO, E

PERICAKVANCE, MA

HAINES, J

ROULEAU, GA

GUSELLA, JS

HORVITZ, HR

BROWN, RH

机构：

[1] MASSACHUSETTS GEN HOSP, DAY NEUROMUSCULAR RES LAB,ROOM 6627,MGH-E, BLDG 149,13TH ST, BOSTON, MA 02129 USA

[2] NORTHWESTERN UNIV, SCH MED, DEPT NEUROL, CHICAGO, IL 60611 USA

[3] ELEANOR ROOSEVELT INST CANC RES, DENVER, CO 80206 USA

[4] UNIV COLORADO, HLTH SCI CTR, DENVER, CO 80206 USA

[5] MCGILL UNIV, CTR RES NEUROSCI, MONTREAL H3A 2T5, QUEBEC, CANADA

[6] MONTREAL GEN HOSP, RES INST, MONTREAL H3G 1A4, QUEBEC, CANADA

[7] MIT, DEPT BIOL, HOWARD HUGHES MED INST, CAMBRIDGE, MA 02139 USA

[8] MASSACHUSETTS GEN HOSP, CTR NEUROSCI, GENET & AGING LAB, BOSTON, MA 02129 USA

[9] NORTHSHORE UNIV HOSP, DEPT NEUROL, MANHASSET, NY 11030 USA

[10] UNIV ZIEKENHUIZEN, DEPT NEUROL, B-3000 LOUVAIN, BELGIUM

[11] UNIV WASHINGTON, SCH MED, DEPT NEUROL, SEATTLE, WA 98195 USA

[12] MAYO CLIN & MAYO FDN, DEPT NEUROL, ROCHESTER, MN 55905 USA

[13] AUSTRALIAN NEUROMUSCULAR RES INST, NEDLANDS, WA, AUSTRALIA

[14] DUKE UNIV, MED CTR, DEPT MED NEUROL, DURHAM, NC 27710 USA

[15] MASSACHUSETTS GEN HOSP, CTR NEUROSCI, MOLEC NEUROGENET LAB, BOSTON, MA 02129 USA

来源：

NATURE | 1993年 / 362卷 / 6415期

关键词：

D O I：

10.1038/362059a0

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

AMYOTROPHIC lateral sclerosis (ALS) is a degenerative disorder of motor neurons in the cortex, brainstem and spinal cord1,2. Its cause is unknown and it is uniformly fatal, typically within five years3. About 10% of cases are inherited as an autosomal dominant trait, with high penetrance after the sixth decade4,5. In most instances, sporadic and autosomal dominant familial ALS (FALS) are clinically similar4,6,7. We have previously shown that in some but not all FALS pedigrees the disease is linked to a genetic defect on chromosome 21q (refs 8, 9). Here we report tight genetic linkage between FALS and a gene that encodes a cytosolic, Cu/Zn-binding superoxide dismutase (SOD1), a homodimeric metalloenzyme that catalyzes the dismutation of the toxic superoxide anion O2.- to O2 and H2O2 (ref. 10). Given this linkage and the potential role of free radical toxicity in other neurodenegerative disorders11, we investigated SOD1 as a candidate gene in FALS. We identified 11 different SOD1 missense mutations in 13 different FALS families.

引用

页码：59 / 62

页数：4

共 47 条

[1] PARTIAL MONOSOMY-21, DIMINISHED ACTIVITY OF SUPEROXIDE-DISMUTASE, AND PULMONARY OXYGEN-TOXICITY [J].