LINKAGE OF DNA MARKERS AT XQ28 TO ADRENOLEUKODYSTROPHY AND ADRENOMYELONEUROPATHY PRESENT WITHIN THE SAME FAMILY

被引：13

作者：

WILLEMS, PJ

VITS, L

WANDERS, RJA

COUCKE, PJ

VANDERAUWERA, BJ

VANELSEN, AF

RAEYMAEKERS, P

VAN BROECKHOVEN, C

SCHUTGENS, RBH

DACREMONT, G

LEROY, JG

MARTIN, JJ

DUMON, JE

机构：

[1] STATE UNIV GHENT HOSP, DEPT PEDIAT, B-9000 GHENT, BELGIUM

[2] UNIV INSTELLING ANTWERP, DEPT BIOCHEM, B-2610 WILRIJK, BELGIUM

[3] UNIV INSTELLING ANTWERP, DEPT NEUROL, B-2610 WILRIJK, BELGIUM

[4] UNIV AMSTERDAM HOSP, DEPT PEDIAT, AMSTERDAM, NETHERLANDS

来源：

ARCHIVES OF NEUROLOGY | 1990年 / 47卷 / 06期

关键词：

D O I：

10.1001/archneur.1990.00530060077022

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

We present a large kindred that contained patients with either adrenoleukodystrophy (ALD) or adrenomyeloneuropathy (AMN). The pedigree clearly supported the X-linked mode of inheritance of the nonneonatal form of ALD/AMN. Analysis with DNA markers at Xq28 suggested segregation of both ALD and AMN with an identical haplotype. This indicated that nonneonatal ALD and AMN are caused by a mutation in the same gene at Xq28. It showed, furthermore, that phenotypic differences between ALD and AMN are not necessarily the consequence of allelic heterogeneity due to different mutations within the same gene. The maximal lod score for linkage of the ALD/AMN gene and the multiallelic anonymous DNA marker at DXS52 was 3.0 at a recombination fraction of 0.00. This made a prenatal or presymptomatic diagnosis and heterozygote detection by DNA analysis with this marker reliable. © 1990, American Medical Association. All rights reserved.

引用

页码：665 / 669

页数：5

共 33 条

[1]

AUBURG PR, 1988, AM J HUM GENET, V42, P408

[2]

AUBURG PR, 1987, ANN NEUROL, V21, P349

[3] 1ST TRIMESTER PRENATAL-DIAGNOSIS OF ADRENOLEUKODYSTROPHY BY DETERMINATION OF VERY LONG-CHAIN FATTY-ACID LEVELS AND BY LINKAGE ANALYSIS TO A DNA PROBE [J].

BOUE, J ;

OBERLE, I ;

HEILIG, R ;

MANDEL, JL ;

MOSER, A ;

MOSER, H ;

LARSEN, JW ;

DUMEZ, Y ;

BOUE, A .

HUMAN GENETICS, 1985, 69 (03) :272-274

[4]

DRUMMONDBORG M, 1988, AM J HUM GENET, V43, P675

[5] PEROXISOMAL DEFECTS IN NEONATAL-ONSET AND X-LINKED ADRENOLEUKODYSTROPHIES [J].

GOLDFISCHER, S ;

COLLINS, J ;

RAPIN, I ;

COLTOFFSCHILLER, B ;

CHANG, CH ;

NIGRO, M ;

BLACK, VH ;

JAVITT, NB ;

MOSER, HW ;

LAZAROW, PB .

SCIENCE, 1985, 227 (4682) :67-70

[6]

GRAHAM G E, 1988, American Journal of Human Genetics, V43, pA144

[7]

HALL JG, 1988, AM J HUM GENET, V43, P355

[8] LIGNOCEROYL-COASH LIGASE - ENZYME DEFECT IN FATTY-ACID BETA-OXIDATION SYSTEM IN X-LINKED CHILDHOOD ADRENOLEUKODYSTROPHY [J].

HASHMI, M ;

STANLEY, W ;

SINGH, I .

FEBS LETTERS, 1986, 196 (02) :247-250

[9] FATTY-ACID ABNORMALITY IN ADRENOLEUKODYSTROPHY [J].

IGARASHI, M ;

SCHAUMBURG, HH ;

POWERS, J ;

KISHIMOTO, Y ;

KOLODNY, E ;

SUZUKI, K .

JOURNAL OF NEUROCHEMISTRY, 1976, 26 (04) :851-&

[10]

LATHROP GM, 1984, AM J HUM GENET, V36, P460

← 1 2 3 4 →