HERITABLE UNSTABLE DNA-SEQUENCES AND HYPERMETHYLATION ASSOCIATED WITH FRAGILE-X SYNDROME IN JAPANESE FAMILIES

被引：13

作者：

HORI, T

YAMAUCHI, M

SEKI, N

TSUJI, S

IKUKO, K

机构：

[1] KAZUSA DNA RES INST,KISARAZU,CHIBA,JAPAN

[2] EHIME UNIV,SCH MED,HYG LAB,SHIGENOBU,EHIME 79102,JAPAN

来源：

CLINICAL GENETICS | 1993年 / 43卷 / 01期

关键词：

FRAGILE-X SYNDROME; HYPERMETHYLATION; P(CCG)N/P(CGG)N REPEAT;

D O I：

10.1111/j.1399-0004.1993.tb04423.x

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Fragile X syndrome, associated with the fragile site at Xq27.3 (FRAXA). is the most common form of familial mental retardation. The fragile X mutation has recently been characterized as a heritable unstable DNA sequence, p(CCG)n/p(CGG)n, in the FRAXA locus. In the present study, a correlation between fragile X-genotypes in the FRAXA locus and hypermethylation of an adjacent CpG island was examined in four Japanese families with fragile X syndrome. We show here that the heritable unstable DNA sequences in the fragile X chromosome usually increase in size when transmitted by female carriers, and that the degree of methylation in the CpG island correlated with the increased sizes of the unstable DNA sequences. When a hypermethylated full mutation was transmitted by a male to his daughters. both the size of the unstable DNA sequence and the degree of the methylation reduced to the premutation range. Our observations suggest that female meiosis has a greater potential for amplifying unstable DNA sequences and that amplified DNA sequences can be transmitted through germ cells, while male germ cells seem not to be able to tolerate highly amplified unstable DNA sequences.

引用

页码：34 / 38

页数：5

共 26 条

[1] PHYSICAL MAPPING ACROSS THE FRAGILE-X - HYPERMETHYLATION AND CLINICAL EXPRESSION OF THE FRAGILE-X SYNDROME
BELL, MV
HIRST, MC
NAKAHORI, Y
MACKINNON, RN
ROCHE, A
FLINT, TJ
JACOBS, PA
TOMMERUP, N
TRANEBJAERG, L
FROSTERISKENIUS, U
KERR, B
TURNER, G
LINDENBAUM, RH
WINTER, R
PEMBREY, M
THIBODEAU, S
DAVIES, KE
[J]. CELL, 1991, 64 (04) : 861 - 866
[2] VARIATION OF THE CGG REPEAT AT THE FRAGILE-X SITE RESULTS IN GENETIC INSTABILITY - RESOLUTION OF THE SHERMAN PARADOX
FU, YH
KUHL, DPA
PIZZUTI, A
PIERETTI, M
SUTCLIFFE, JS
RICHARDS, S
VERKERK, AJMH
HOLDEN, JJA
FENWICK, RG
WARREN, ST
OOSTRA, BA
NELSON, DL
CASKEY, CT
[J]. CELL, 1991, 67 (06) : 1047 - 1058
[3] MAPPING OF DNA INSTABILITY AT THE FRAGILE-X TO A TRINUCLEOTIDE REPEAT SEQUENCE P(CCG)N
KREMER, EJ
PRITCHARD, M
LYNCH, M
YU, S
HOLMAN, K
BAKER, E
WARREN, ST
SCHLESSINGER, D
SUTHERLAND, GR
RICHARDS, RI
[J]. SCIENCE, 1991, 252 (5013) : 1711 - 1714
[4] LAIRD CD, 1987, GENETICS, V117, P587
[5] EXPERIENCE WITH DIRECT MOLECULAR DIAGNOSIS OF FRAGILE-X
MULLEY, JC
YU, S
GEDEON, AK
DONNELLY, A
TURNER, G
LOESCH, D
CHAPMAN, CJ
GARDNER, RJM
RICHARDS, RI
SUTHERLAND, GR
[J]. JOURNAL OF MEDICAL GENETICS, 1992, 29 (06) : 368 - 374
[6] MOLECULAR HETEROGENEITY OF THE FRAGILE-X SYNDROME
NAKAHORI, Y
KNIGHT, SJL
HOLLAND, J
SCHWARTZ, C
ROCHE, A
TARLETON, J
WONG, S
FLINT, TJ
FROSTERISKENIUS, U
BENTLEY, D
DAVIES, KE
HIRST, MC
[J]. NUCLEIC ACIDS RESEARCH, 1991, 19 (16) : 4355 - 4359
[7] INSTABILITY OF A 550 BASE PAIR DNA SEGMENT AND ABNORMAL METHYLATION IN FRAGILE X-SYNDROME
OBERLE, I
ROUSSEAU, F
HEITZ, D
KRETZ, C
DEVYS, D
HANAUER, A
BOUE, J
BERTHEAS, MF
MANDEL, JL
[J]. SCIENCE, 1991, 252 (5009) : 1097 - 1102
[8] A PRE-MUTATION THAT GENERATES A DEFECT AT CROSSING OVER EXPLAINS THE INHERITANCE OF FRAGILE X MENTAL RETARDATION
PEMBREY, ME
WINTER, RM
DAVIES, KE
[J]. AMERICAN JOURNAL OF MEDICAL GENETICS, 1985, 21 (04): : 709 - 717
[9] ABSENCE OF EXPRESSION OF THE FMR-1 GENE IN FRAGILE-X SYNDROME
PIERETTI, M
ZHANG, FP
FU, YH
WARREN, ST
OOSTRA, BA
CASKEY, CT
NELSON, DL
[J]. CELL, 1991, 66 (04) : 817 - 822
[10] FRAGILE-X SYNDROME - GENETIC LOCALIZATION BY LINKAGE MAPPING OF 2 MICROSATELLITE REPEATS FRAXAC1 AND FRAXAC2 WHICH IMMEDIATELY FLANK THE FRAGILE SITE
RICHARDS, RI
HOLMAN, K
KOZMAN, H
KREMER, E
LYNCH, M
PRITCHARD, M
YU, S
MULLEY, J
SUTHERLAND, GR
[J]. JOURNAL OF MEDICAL GENETICS, 1991, 28 (12) : 818 - 823

← 1 2 3 →