CLONING OF THE ESSENTIAL MYOTONIC-DYSTROPHY REGION AND MAPPING OF THE PUTATIVE DEFECT

被引：473

作者：

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

机构：

[1] UNIV CALIF LAWRENCE LIVERMORE NATL LAB,CTR HUMAN GENOME,DIV BIOMED SCI,L-452,LIVERMORE,CA 94550

[2] CATHOLIC UNIV NIJMEGEN,FAC MED SCI,DEPT CELL BIOL & HISTOL,6500 HB NIJMEGEN,NETHERLANDS

[3] CATHOLIC UNIV NIJMEGEN,FAC MED SCI,DEPT HUMAN GENET,6500 HB NIJMEGEN,NETHERLANDS

[4] CHILDRENS HOSP EASTERN ONTARIO,DIV GENET,OTTAWA K1H 8L1,ONTARIO,CANADA

[5] UNIV OTTAWA,DEPT MICROBIOL & IMMUNOL,OTTAWA K1N 6N5,ONTARIO,CANADA

[6] CHARING CROSS & WESTMINSTER MED SCH,DEPT ANAT,LONDON W6 8RF,ENGLAND

来源：

NATURE | 1992年 / 355卷 / 6360期

关键词：

D O I：

10.1038/355548a0

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：

MYOTONIC dystrophy is a common dominant disorder (global incidence of 1:8,000) with variable onset and a protean nature of symptoms mainly involving progressive muscle wasting, myotonia and cataracts 1. To define the molecular defect, we have cloned the essential region of chromosome 19q13.3, including proximal and distal markers 2-7 in a 700-kilobase contig formed by overlapping cosmids and yeast artificial chromosomes (YACs). The central part of the contig bridges an area of about 350 kilobases between two new flanking crossover borders 4,5. This segment has been extensively characterized through the isolation of five YAC clones and the subsequent subcloning in cosmids from which a detailed EcoRI, HindIII, MluI and NotI restriction map has been derived. Two genomic probes and two homologous complementary DNA probes were isolated using the cosmids. These probes are all situated within approximately 10 kilobases of genomic DNA and detect an unstable genomic segment in myotonic dystrophy patients. The length variation in this segment shows similarities to the instability seen at the fragile X locus 8. The physical map location and the genetic characteristics of the length polymorphism is compatible with a direct role in the pathogenesis of myotonic dystrophy.

引用

页码：548 / 551

页数：4

共 25 条

[1] OPTIMIZING RESTRICTION FRAGMENT FINGERPRINTING METHODS FOR ORDERING LARGE GENOMIC LIBRARIES
BRANSCOMB, E
SLEZAK, T
PAE, R
GALAS, D
CARRANO, AV
WATERMAN, M
[J]. GENOMICS, 1990, 8 (02) : 351 - 366
[2] IDENTIFICATION OF NEW DNA MARKERS CLOSE TO THE MYOTONIC-DYSTROPHY LOCUS
BROOK, JD
HARLEY, HG
WALSH, KV
RUNDLE, SA
SICILIANO, MJ
HARPER, PS
SHAW, DJ
[J]. JOURNAL OF MEDICAL GENETICS, 1991, 28 (02) : 84 - 88
[3] CLONING OF LARGE SEGMENTS OF EXOGENOUS DNA INTO YEAST BY MEANS OF ARTIFICIAL CHROMOSOME VECTORS
BURKE, DT
CARLE, GF
OLSON, MV
[J]. SCIENCE, 1987, 236 (4803) : 806 - 812
[4] 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
[5] BUXTON J, IN PRESS GENOMICS
[6] A HIGH-RESOLUTION, FLUORESCENCE-BASED, SEMIAUTOMATED METHOD FOR DNA FINGERPRINTING
CARRANO, AV
LAMERDIN, J
ASHWORTH, LK
WATKINS, B
BRANSCOMB, E
SLEZAK, T
RAFF, M
DEJONG, PJ
KEITH, D
MCBRIDE, L
MEISTER, S
KRONICK, M
[J]. GENOMICS, 1989, 4 (02) : 129 - 136
[7] DEJONG PJ, 1989, CYTOGENET CELL GENET, V51, P985
[8] CRITERIA FOR ESTABLISHING THE VALIDITY OF GENETIC-RECOMBINATION IN MYOTONIC-DYSTROPHY
GRIGGS, RC
WOOD, DS
[J]. NEUROLOGY, 1989, 39 (03) : 420 - 421
[9] HARLEY HG, 1991, AM J HUM GENET, V49, P68
[10] Harper P. S., 1989, MYOTONIC DYSTROPHY

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