DIRECT-DETECTION OF NOVEL EXPANDED TRINUCLEOTIDE REPEATS IN THE HUMAN GENOME

被引：250

作者：

SCHALLING, M

HUDSON, TJ

BUETOW, KH

HOUSMAN, DE

机构：

[1] MIT,CTR CANC RES,CAMBRIDGE,MA 02139

[2] FOX CHASE CANC CTR,PHILADELPHIA,PA 19111

来源：

NATURE GENETICS | 1993年 / 4卷 / 02期

关键词：

D O I：

10.1038/ng0693-135

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Expansion of trinucleotide repeats can give rise to genetic disease. We have developed a technique, repeat expansion detection (RED), that can identify potentially pathological repeat expansion without prior knowledge of chromosomal location. Human genomic DNA is used as a template for a two-step cycling process that generates oligonucleotide multimers when expanded trinucleotide sequences are present at the level found in myotonic dystrophy and fragile-X patients. We have identified at least one new locus exhibiting trinucleotide expansion. Analysis of three families transmitting a long CTG repeat shows that the allele in these families corresponds to a locus on chromosome 18. RED constitutes a powerful tool to identify other diseases caused by this mechanism, particularly diseases associated with anticipation.

引用

页码：135 / 139

页数：5

共 20 条

[1] CLONING OF THE ESSENTIAL MYOTONIC-DYSTROPHY REGION AND MAPPING OF THE PUTATIVE DEFECT
ASLANIDIS, C
JANSEN, G
AMEMIYA, C
SHUTLER, G
MAHADEVAN, M
TSILFIDIS, C
CHEN, C
ALLEMAN, J
WORMSKAMP, NGM
VOOIJS, M
BUXTON, J
JOHNSON, K
SMEETS, HJM
LENNON, GG
CARRANO, AV
KORNELUK, RG
WIERINGA, B
DEJONG, PJ
[J]. NATURE, 1992, 355 (6360) : 548 - 551
[2] GENETIC-DISEASE DETECTION AND DNA AMPLIFICATION USING CLONED THERMOSTABLE LIGASE
BARANY, F
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (01) : 189 - 193
[3] SURVEY OF HUMAN AND RAT MICROSATELLITES
BECKMANN, JS
WEBER, JL
[J]. GENOMICS, 1992, 12 (04) : 627 - 631
[4] Biancalana V., 1992, Human Molecular Genetics, V1, P255, DOI 10.1093/hmg/1.4.255
[5] MOLECULAR-BASIS OF MYOTONIC-DYSTROPHY - EXPANSION OF A TRINUCLEOTIDE (CTG) REPEAT AT THE 3' END OF A TRANSCRIPT ENCODING A PROTEIN-KINASE FAMILY MEMBER
BROOK, JD
MCCURRACH, ME
HARLEY, HG
BUCKLER, AJ
CHURCH, D
ABURATANI, H
HUNTER, K
STANTON, VP
THIRION, JP
HUDSON, T
SOHN, R
ZEMELMAN, B
SNELL, RG
RUNDLE, SA
CROW, S
DAVIES, J
SHELBOURNE, P
BUXTON, J
JONES, C
JUVONEN, V
JOHNSON, K
HARPER, PS
SHAW, DJ
HOUSMAN, DE
[J]. CELL, 1992, 68 (04) : 799 - 808
[6] DETECTION OF AN UNSTABLE FRAGMENT OF DNA SPECIFIC TO INDIVIDUALS WITH MYOTONIC-DYSTROPHY
BUXTON, J
SHELBOURNE, P
DAVIES, J
JONES, C
VANTONGEREN, T
ASLANIDIS, C
DEJONG, P
JANSEN, G
ANVRET, M
RILEY, B
WILLIAMSON, R
JOHNSON, K
[J]. NATURE, 1992, 355 (6360) : 547 - 548
[7] AN UNSTABLE TRIPLET REPEAT IN A GENE RELATED TO MYOTONIC MUSCULAR-DYSTROPHY
FU, YH
PIZZUTI, A
FENWICK, RG
KING, J
RAJNARAYAN, S
DUNNE, PW
DUBEL, J
NASSER, GA
ASHIZAWA, T
DEJONG, P
WIERINGA, B
KORNELUK, R
PERRYMAN, MB
EPSTEIN, HF
CASKEY, CT
[J]. SCIENCE, 1992, 255 (5049) : 1256 - 1258
[8] PREVALENCE OF THE FRAGILE-X SYNDROME IN MENTALLY-RETARDED BOYS IN A SWEDISH COUNTY
GUSTAVSON, KH
BLOMQUIST, H
HOLMGREN, G
[J]. AMERICAN JOURNAL OF MEDICAL GENETICS, 1986, 23 (1-2): : 581 - 587
[9] EXPANSION OF AN UNSTABLE DNA REGION AND PHENOTYPIC VARIATION IN MYOTONIC-DYSTROPHY
HARLEY, HG
BROOK, JD
RUNDLE, SA
CROW, S
REARDON, W
BUCKLER, AJ
HARPER, PS
HOUSMAN, DE
SHAW, DJ
[J]. NATURE, 1992, 355 (6360) : 545 - 546
[10] Harper P. S., 1989, MYOTONIC DYSTROPHY

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