学术探索
学术期刊
新闻热点
数据分析
智能评审

DXS28 (C7) MAPS CENTROMERIC TO DXS68 (L1-4) AND DXS67 (B24) BY DELETION ANALYSIS

被引:13
作者
TOWBIN, JA
CHAMBERLAIN, JS
WU, DR
PILLERS, DAM
SELTZER, WK
MCCABE, ERB
机构
[1] BAYLOR UNIV,INST MOLEC GENET,1 BAYLOR PLAZA,HOUSTON,TX 77030
[2] OREGON HLTH SCI UNIV,DEPT PEDIAT,PORTLAND,OR 97201
[3] BAYLOR UNIV,DEPT PEDIAT,HOUSTON,TX 77030
[4] BAYLOR UNIV,DEPT PEDIAT CARDIOL,HOUSTON,TX 77030
[5] UNIV COLORADO,SCH MED,DEPT PEDIAT & BIOCHEM,DENVER,CO 80262
[6] UNIV COLORADO,SCH MED,DEPT BIOPHYS,DENVER,CO 80262
[7] UNIV COLORADO,SCH MED,DEPT GENET,DENVER,CO 80262
来源
GENOMICS | 1990年 / 7卷 / 03期
关键词
D O I
10.1016/0888-7543(90)90181-S
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
Complex glycerol kinase deficiency (CGKD) is a contiguous gene syndrome consisting of glycerol kinase deficiency together with Duchenne muscular dystrophy (DMD), congenital adrenal hypoplasia, and/or Ȧland Island eye disease. Deletion mapping of genomic DNA from patients with CGKD was carried out and allowed definitive ordering of loci DXS28 (C7), DXS68 (L1-4), and DXS67 (B24). Most reports have placed DXS68 centromeric to DXS28 and DXS67 on the basis of the initial mapping of the Iowa patient 3, but others have presented evidence consistent with the placement of DXS28 telomeric to DXS68 and DXS67. Through the use of DNA from CGKD patients with a variety of genomic deletions, this controversy is resolved and the order Xcen...DMD-DXS28-DXS68-DXS67...pter is definitively demonstrated. © 1990.
引用
收藏
页码:442 / 444
页数:3
相关论文
共 21 条
[11]  
FEINBERG AP, 1984, ANAL BIOCHEM, V137, P266
[12]   REPORT OF THE COMMITTEE ON THE GENETIC CONSTITUTION OF THE X-CHROMOSOMES AND Y-CHROMOSOMES [J].
GOODFELLOW, PN ;
DAVIES, KE ;
ROPERS, HH .
CYTOGENETICS AND CELL GENETICS, 1985, 40 (1-4) :296-352
[13]   CONSTRUCTION OF A HUMAN X-CHROMOSOME-ENRICHED PHAGE LIBRARY WHICH FACILITATES ANALYSIS OF SPECIFIC LOCI [J].
KUNKEL, LM ;
LALANDE, M ;
MONACO, AP ;
FLINT, A ;
MIDDLESWORTH, W ;
LATT, SA .
GENE, 1985, 33 (03) :251-258
[14]   COMPLEMENTARY-DNA PROBES FOR THE DUCHENNE MUSCULAR-DYSTROPHY LOCUS DEMONSTRATE A PREVIOUSLY UNDETECTABLE DELETION IN A PATIENT WITH DYSTROPHIC MYOPATHY, GLYCEROL KINASE-DEFICIENCY, AND CONGENITAL ADRENAL HYPOPLASIA [J].
MCCABE, ERB ;
TOWBIN, J ;
CHAMBERLAIN, J ;
BAUMBACH, L ;
WITKOWSKI, J ;
VANOMMEN, GJB ;
KOENIG, M ;
KUNKEL, LM ;
SELTZER, WK .
JOURNAL OF CLINICAL INVESTIGATION, 1989, 83 (01) :95-99
[15]  
NORBY S, 1987, CLIN GENET, V31, P192
[16]  
PATIL SR, 1985, CYTOGENET CELL GENET, V40, P720
[17]  
PILLERS DM, 1989, CYTOGENET CELL GENET, V51, P1059
[18]  
PILLERS DM, 1989, UNPUB DELETION MAPPI
[19]   CHARACTERIZATION OF PATIENTS WITH GLYCEROL KINASE-DEFICIENCY UTILIZING CDNA PROBES FOR THE DUCHENNE MUSCULAR-DYSTROPHY LOCUS [J].
TOWBIN, JA ;
WU, D ;
CHAMBERLAIN, J ;
LARSEN, PD ;
SELTZER, WK ;
MCCABE, ERB .
HUMAN GENETICS, 1989, 83 (02) :122-126
[20]   A PHYSICAL MAP OF 4 MILLION BP AROUND THE DUCHENNE MUSCULAR-DYSTROPHY GENE ON THE HUMAN X-CHROMOSOME [J].
VANOMMEN, GJB ;
VERKERK, JMH ;
HOFKER, MH ;
MONACO, AP ;
KUNKEL, LM ;
RAY, P ;
WORTON, R ;
WIERINGA, B ;
BAKKER, E ;
PEARSON, PL .
CELL, 1986, 47 (04) :499-504
123