LINKAGE DISEQUILIBRIUM BETWEEN THE FES, D15S127, AND BLM LOCI IN ASHKENAZI JEWS WITH BLOOM-SYNDROME

被引:0
|
作者
ELLIS, NA
ROE, AM
KOZLOSKI, J
PROYTCHEVA, M
FALK, C
GERMAN, J
机构
来源
AMERICAN JOURNAL OF HUMAN GENETICS | 1994年 / 55卷 / 03期
关键词
D O I
暂无
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Bloom syndrome (BS) is more common in the Ashkenazi Jewish than in any other population. Approximately 1 in 110 Ashkenazi Jews carries blm, the BS mutation. The locus mutated in BS, BLM, maps to chromosome subband 15q26.1, tightly linked to the proto-oncogene FES. We have investigated the basis for the increased frequency of blm in the Ashkenazim by genotyping polymorphic microsatellite loci tightly linked to BLM in affected and unaffected individuals from Ashkenazi Jewish and non-Ash-kenazi populations. A striking association of the C3 allele at FES with blm (Delta = .422; p = 5.52 X 10(-7)) and of the 145-bp and 147-bp alleles at D15S127 with blm (Delta = .392 and Delta = .483, respectively; p = 2.8 X 10(-5) and p = 5.4 X 10(-7), respectively) was detected in Ashkenazi Jews with BS. This linkage disequilibrium constitutes strong support for a founder-effect hypothesis: the chromosome in the hypothetical founder who carried blm also carried the C3 allele at FES and either the 145-bp or the 147-bp allele at D15S127.
引用
收藏
页码:453 / 460
页数:8
相关论文
共 6 条
  • [1] ALLELE ASSOCIATION BETWEEN THE MUTATED BLM LOCUS AND THE C3 ALLELE OF FES IN ASHKENAZI JEWS WITH BLOOMS SYNDROME (BS)
    ELLIS, NA
    ROE, AM
    KOZLOSKI, J
    PROYTCHEVA, M
    GERMAN, J
    AMERICAN JOURNAL OF HUMAN GENETICS, 1993, 53 (03) : 797 - 797
  • [2] LINKAGE DISEQUILIBRIUM BETWEEN SPINOCEREBELLAR ATAXIA (SCA1) AND D6S89 LOCI
    TERRENATO, L
    JODICE, C
    MALASPINA, P
    NOVELLETTO, A
    PERSICHETTI, F
    SCHINAIA, G
    FRONTALI, M
    LULLI, P
    CAPPELLACCI, S
    GIUNTI, P
    SPADARO, M
    ANTONELLI, A
    PANDOLFO, M
    CYTOGENETICS AND CELL GENETICS, 1993, 62 (2-3): : 80 - 80
  • [3] FRIEDREICH ATAXIA IN ITALIAN FAMILIES - GENETIC HOMOGENEITY AND LINKAGE DISEQUILIBRIUM WITH THE MARKER LOCI D9S5 AND D9S15
    PANDOLFO, M
    SIRUGO, G
    ANTONELLI, A
    WEITNAUER, L
    FERRETTI, L
    LEONE, M
    DONES, I
    CERINO, A
    FUJITA, R
    HANAUER, A
    MANDEL, JL
    DIDONATO, S
    AMERICAN JOURNAL OF HUMAN GENETICS, 1990, 47 (02) : 228 - 235
  • [4] ADDITIONAL POLYMORPHISMS AT MARKER LOCI D9S5 AND D9S15 GENERATE EXTENDED HAPLOTYPES IN LINKAGE DISEQUILIBRIUM WITH FRIEDREICH ATAXIA
    FUJITA, R
    HANAUER, A
    SIRUGO, G
    HEILIG, R
    MANDEL, JL
    PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1990, 87 (05) : 1796 - 1800
  • [5] SIGNIFICANT LINKAGE DISEQUILIBRIUM BETWEEN THE HUNTINGTON DISEASE GENE AND THE LOCI D4S10 AND D4S95 IN THE DUTCH POPULATION
    SKRAASTAD, MI
    VAN DE VOSSE, E
    BELFROID, R
    HOLD, K
    VEGTERVANDERVLIS, M
    SANDKUIJL, LA
    BAKKER, E
    VANOMMEN, GJB
    AMERICAN JOURNAL OF HUMAN GENETICS, 1992, 51 (04) : 730 - 735
  • [6] SIGNIFICANT LINKAGE DISEQUILIBRIUM BETWEEN THE HUNTINGTONS-DISEASE LOCUS AND MARKERS AT LOCI D4S10, D4S95, AND D4S111 IN NORTHERN-IRELAND
    MORRISON, PJ
    GRAHAM, CA
    NEVIN, NC
    JOURNAL OF MEDICAL GENETICS, 1993, 30 (12) : 1018 - 1019
1