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MAPPING OF FACIOSCAPULOHUMERAL MUSCULAR-DYSTROPHY GENE TO CHROMOSOME 4Q35-QTER BY MULTIPOINT LINKAGE ANALYSIS AND INSITU HYBRIDIZATION

被引:127
作者
WIJMENGA, C
PADBERG, GW
MOERER, P
WIEGANT, J
LIEM, L
BROUWER, OF
MILNER, ECB
WEBER, JL
VANOMMEN, GB
SANDKUYL, LA
FRANTS, RR
机构
[1] VIRGINIA MASON RES CTR,SEATTLE,WA 98101
[2] MARSHFIELD MED RES FDN,MARSHFIELD,WI 54449
[3] ERASMUS UNIV,DEPT CLIN GENET,3000 DR ROTTERDAM,NETHERLANDS
[4] LEIDEN STATE UNIV,DEPT HUMAN GENET,2312 AV LEIDEN,NETHERLANDS
[5] LEIDEN STATE UNIV,DEPT CYTOCHEM & CYTOMETRY,2312 AV LEIDEN,NETHERLANDS
来源
GENOMICS | 1991年 / 9卷 / 04期
关键词
D O I
10.1016/0888-7543(91)90348-I
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
We have recently assigned the facioscapulohumeral muscular dystrophy (FSHD) gene to chromosome 4 by linkage to the microsatellite marker Mfd 22 (locus D4S171). We now report that D4S139, a VNTR locus, is much more closely linked to FSHD. Two-point linkage analysis between FSHD and D4S139 in nine informative families showed a maximum combined lod score (Zmax) of 17.28 at a recombination fraction θ of 0.027. Multipoint linkage analysis between FSHD and the loci D4S139 and D4S171 resulted in a peak lod score of 20.21 at 2.7 cM from D4S139. Due to the small number of recombinants found with D4S139, the position of the FSHD gene relative to that of D4S139 could not be established with certainty. D4S139 was mapped to chromosome 4q35-qter by in situ hybridization, thus firmly establishing the location of the FSHD gene in the subtelomeric region of chromosome 4q. One small family yielded a negative lod score for D4S139. In the other families no significant evidence for genetic heterogeneity was obtained. Studies of additional markers and new families will improve the map of the FSHD region, reveal possible genetic heterogeneity, and allow better diagnostic reliability. © 1991.
引用
收藏
页码:570 / 575
页数:6
相关论文
共 20 条
[1]   BUFFER GRADIENT GELS AND S-35 LABEL AS AN AID TO RAPID DNA-SEQUENCE DETERMINATION [J].
BIGGIN, MD ;
GIBSON, TJ ;
HONG, GF .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1983, 80 (13) :3963-3965
[2]   AN ALGORITHM TO IMPROVE THE COMPUTATIONAL-EFFICIENCY OF GENETIC-LINKAGE ANALYSIS [J].
BRAVERMAN, MS .
COMPUTERS AND BIOMEDICAL RESEARCH, 1985, 18 (01) :24-36
[3]   GENOMIC SEQUENCING [J].
CHURCH, GM ;
GILBERT, W .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1984, 81 (07) :1991-1995
[4]   RETINAL VASCULAR ABNORMALITIES IN FACIOSCAPULOHUMERAL MUSCULAR-DYSTROPHY - A GENERAL ASSOCIATION WITH GENETIC AND THERAPEUTIC IMPLICATIONS [J].
FITZSIMONS, RB ;
GURWIN, EB ;
BIRD, AC .
BRAIN, 1987, 110 :631-648
[5]  
LANGER PR, 1981, P NATL ACAD SCI USA, V78, P6663
[6]  
LATHROP GM, 1988, AM J HUM GENET, V42, P498
[7]   ESTIMATION OF AGE-DEPENDENT PENETRANCE IN FACIOSCAPULOHUMERAL MUSCULAR-DYSTROPHY BY MINIMIZING ASCERTAINMENT BIAS [J].
LUNT, PW ;
COMPSTON, DAS ;
HARPER, PS .
JOURNAL OF MEDICAL GENETICS, 1989, 26 (12) :755-760
[8]   RECOMBINATION EVENTS SUGGEST POTENTIAL SITES FOR THE HUNTINGTONS-DISEASE GENE [J].
MACDONALD, ME ;
HAINES, JL ;
ZIMMER, M ;
CHENG, SV ;
YOUNGMAN, S ;
WHALEY, WL ;
WEXLER, N ;
BUCAN, M ;
ALLITTO, BA ;
SMITH, B ;
LEAVITT, J ;
POUSTKA, A ;
HARPER, P ;
LEHRACH, H ;
WASMUTH, JJ ;
FRISCHAUF, AM ;
GUSELLA, JF .
NEURON, 1989, 3 (02) :183-190
[9]   RELEASE OF INFECTIOUS EPSTEIN-BARR VIRUS BY TRANSFORMED MARMOSET LEUKOCYTES [J].
MILLER, G ;
LIPMAN, M .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1973, 70 (01) :190-194
[10]   ISOLATION AND MAPPING OF A POLYMORPHIC DNA-SEQUENCE PH30 ON CHROMOSOME 4 [HGM PROVISIONAL NO D4S139] [J].
MILNER, ECB ;
LOTSHAW, CL ;
VANDIJK, KW ;
CHARMLEY, P ;
CONCANNON, P ;
SCHROEDER, HW .
NUCLEIC ACIDS RESEARCH, 1989, 17 (10) :4002-4002
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