PRENATAL-DIAGNOSIS OF FRAGILE X-SYNDROME BY DIRECT-DETECTION OF THE DYNAMIC MUTATION DUE TO AN UNSTABLE DNA-SEQUENCE

被引：0

作者：

YAMAUCHI, M

NAGATA, S

SEKI, N

TOYAMA, Y

HARADA, N

NIIKAWA, N

MASUNO, I

KAJII, T

HORI, T

机构：

[1] NATL INST RADIOL SCI, DIV GENET, 4-9-1 ANAGAWA, CHIBA 263, JAPAN

[2] NATL FUKUOKA CENT HOSP, DEPT OBSTET & GYNECOL, FUKUOKA, JAPAN

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

[4] KYUSHU MED SCI, CYTOGENET RES LAB, FUKUOKA, JAPAN

[5] YAMAGUCHI UNIV, SCH MED, DEPT PEDIAT, YAMAGUCHI 753, JAPAN

[6] NAGASAKI UNIV, SCH MED, DEPT HUMAN GENET, NAGASAKI 852, JAPAN

[7] CHIBA UNIV, SCH MED, DEPT ANAT, CHIBA, JAPAN

来源：

CLINICAL GENETICS | 1993年 / 44卷 / 04期

关键词：

(CCG)N REPEAT; DIAGNOSTIC DNA PROBE; DYNAMIC MUTATION; FRAGILE X-SYNDROME; PRENATAL DIAGNOSIS;

D O I：

暂无

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

The fragile X syndrome is the most common familial form of mental retardation. The mutation causing the syndrome is dynamic mutation due to an unstable DNA (CCG)n repeat localized at Xq27.3. We have previously reported a PCR procedure to prepare a diagnostic probe, pPCRfx1, which can be used to determine the genotype of fragile X mutation individuals by Southern blot analysis. In the present study, pPCRfx1 was applied to the prenatal diagnosis, using chorionic villus cells, of a fetus which was at risk of having fragile X syndrome. In the PstI assay, the Southern blot showed the typical pattern of a female carrier with the full mutation. Analysis of the DNA methylation patterns by EcoRI + EagI assay showed that the EagI restriction site was not methylated on the mutated X chromosome of chorionic villi, but the sites were totally methylated in the brain and other tissues of the fetus. Thus the fetus was diagnosed to be a heterozygous female carrier of the dynamic mutation involved in the fragile X syndrome.

引用

页码：169 / 172

页数：4

共 20 条

[1] ANALYSIS OF FULL FRAGILE-X MUTATIONS IN FETAL TISSUES AND MONOZYGOTIC TWINS INDICATE THAT ABNORMAL METHYLATION AND SOMATIC HETEROGENEITY ARE ESTABLISHED EARLY IN DEVELOPMENT
DEVYS, D
BIANCALANA, V
ROUSSEAU, F
BOUE, J
MANDEL, JL
OBERLE, I
[J]. AMERICAN JOURNAL OF MEDICAL GENETICS, 1992, 43 (1-2): : 208 - 216
[2] DOBKIN CS, 1991, LANCET, V338, P957
[3] 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
[4] HIRST M, 1991, LANCET, V338, P956, DOI 10.1016/0140-6736(91)91831-E
[5] HERITABLE UNSTABLE DNA-SEQUENCES AND HYPERMETHYLATION ASSOCIATED WITH FRAGILE-X SYNDROME IN JAPANESE FAMILIES
HORI, T
YAMAUCHI, M
SEKI, N
TSUJI, S
IKUKO, K
[J]. CLINICAL GENETICS, 1993, 43 (01) : 34 - 38
[6] 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
[7] Molecular genetics of the fragile-X syndrome: a novel type of unstable mutation
Mandel, Jean-Louis
Heitz, Dominique
[J]. CURRENT OPINION IN GENETICS & DEVELOPMENT, 1992, 2 (03) : 422 - 430
[8] 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
[9] DETECTION OF FULL FRAGILE-X MUTATION
PERGOLIZZI, RG
ERSTER, SH
GOONEWARDENA, P
BROWN, WT
[J]. LANCET, 1992, 339 (8788) : 271 - 272
[10] FRAGILE X-SYNDROME - THE MOLECULAR PICTURE COMES INTO FOCUS
RICHARDS, RI
SUTHERLAND, GR
[J]. TRENDS IN GENETICS, 1992, 8 (07) : 249 - 255

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