Positional cloning of the Warner's syndrome gene

被引：1383

作者：

Yu, CE

Oshima, J

Fu, YH

Wijsman, EM

Hisama, F

Alisch, R

Matthews, S

Nakura, J

Miki, T

Ouais, S

Martin, GM

Mulligan, J

Schellenberg, GD

机构：

[1] VET AFFAIRS PUGET SOUND HLTH CARE SYST, CTR GERIATR RES EDUC & CLIN, SEATTLE, WA 98108 USA

[2] UNIV WASHINGTON, DEPT NEUROL, SEATTLE, WA 98195 USA

[3] UNIV WASHINGTON, DEPT PHARMACOL, SEATTLE, WA 98195 USA

[4] UNIV WASHINGTON, DEPT PATHOL, SEATTLE, WA 98195 USA

[5] UNIV WASHINGTON, DEPT BIOSTAT, SEATTLE, WA 98195 USA

[6] UNIV WASHINGTON, DIV MED GENET, DEPT MED, SEATTLE, WA 98195 USA

[7] DARWIN MOLEC CORP, BOTHELL, WA 98021 USA

[8] YALE UNIV, SCH MED, DEPT NEUROL, NEW HAVEN, CT 06510 USA

[9] DAMASCUS CITY HOSP, ENDOCRINOL SECT, DAMASCUS, SYRIA

[10] OSAKA UNIV, SCH MED, DEPT GERIATR MED, SUITA, OSAKA 565, JAPAN

来源：

SCIENCE | 1996年 / 272卷 / 5259期

关键词：

D O I：

10.1126/science.272.5259.258

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：

Werner's syndrome (WS) is an inherited disease with clinical symptoms resembling premature aging. Early susceptibility to a number of major age-related diseases is a key feature of this disorder. The gene responsible for WS (known as WRN) was identified by positional cloning. The predicted protein is 1432 amino acids in length and shows significant similarity to DNA helicases. Four mutations in WS patients were identified. Two of the mutations are splice-junction mutations, with the predicted result being the exclusion of exons from the final messenger RNA. One of these mutations, which results in a frameshift and a predicted truncated protein, was found in the homozygous state in 60 percent of Japanese WS patients examined. The other two mutations are nonsense mutations. The identification of a mutated putative helicase as the gene product of the WS gene suggests that defective DNA metabolism is involved in the complex process of aging in WS patients.

引用

页码：258 / 262

页数：5

共 58 条

[1] ALTSCHUL SF, 1990, J MOL BIOL, V215, P403, DOI 10.1006/jmbi.1990.9999
[2] EXON AMPLIFICATION - A STRATEGY TO ISOLATE MAMMALIAN GENES BASED ON RNA SPLICING
BUCKLER, AJ
CHANG, DD
GRAW, SL
BROOK, JD
HABER, DA
SHARP, PA
HOUSMAN, DE
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (09) : 4005 - 4009
[3] HIGH PREVALENCE OF WERNERS SYNDROME IN SARDINIA - DESCRIPTION OF 6 PATIENTS AND ESTIMATE OF THE GENE-FREQUENCY
CERIMELE, D
COTTONI, F
SCAPPATICCI, S
RABBIOSI, G
BORRONI, G
SANNA, E
ZEI, G
FRACCARO, M
[J]. HUMAN GENETICS, 1982, 62 (01) : 25 - 30
[4] CHANG M, 1994, AM J PATHOL, V144, P1
[5] HOMOLOGOUS RECOMBINATION IS ELEVATED IN SOME WERNER-LIKE SYNDROMES BUT NOT DURING NORMAL INVITRO OR INVIVO SENESCENCE OF MAMMALIAN-CELLS
CHENG, RZ
MURANO, S
KURZ, B
REIS, RJS
[J]. MUTATION RESEARCH, 1990, 237 (5-6): : 259 - 269
[6] ISOLATION OF GENES FROM COMPLEX SOURCES OF MAMMALIAN GENOMIC DNA USING EXON AMPLIFICATION
CHURCH, DM
STOTLER, CJ
RUTTER, JL
MURRELL, JR
TROFATTER, JA
BUCKLER, AJ
[J]. NATURE GENETICS, 1994, 6 (01) : 98 - 105
[7] THE BLOOMS-SYNDROME GENE-PRODUCT IS HOMOLOGOUS TO RECQ HELICASES
ELLIS, NA
GRODEN, J
YE, TZ
STRAUGHEN, J
LENNON, DJ
CIOCCI, S
PROYTCHEVA, M
GERMAN, J
[J]. CELL, 1995, 83 (04) : 655 - 666
[8] WERNERS SYNDROME - A REVIEW OF ITS SYMPTOMATOLOGY NATURAL HISTORY PATHOLOGIC FEATURES GENETICS AND RELATIONSHIP TO NATURAL AGING PROCESS
EPSTEIN, CJ
MARTIN, GM
SCHULTZ, AL
MOTULSKY, AG
[J]. MEDICINE, 1966, 45 (03) : 177 - +
[9] FREJTER WL, 1992, P NATL ACAD SCI USA, V89, P261
[10] RETARDED RATE OF DNA-REPLICATION AND NORMAL LEVEL OF DNA-REPAIR IN WERNERS SYNDROME FIBROBLASTS IN CULTURE
FUJIWARA, Y
HIGASHIKAWA, T
TATSUMI, M
[J]. JOURNAL OF CELLULAR PHYSIOLOGY, 1977, 92 (03) : 365 - 374

← 1 2 3 4 5 6 →