RAPID PREPARATION OF DIAGNOSTIC PROBES FOR THE FRAGILE-X SYNDROME BY DIRECT PCR AMPLIFICATION OF HUMAN CHROMOSOMAL DNA

被引：7

作者：

YAMAUCHI, M

SEKI, N

HORI, TA

机构：

[1] Division of Genetics, National Institute of Radiological Sciences, Chiba, 263, Anagawa, Inage-ku

来源：

JAPANESE JOURNAL OF HUMAN GENETICS | 1992年 / 37卷 / 03期

关键词：

FRAGILE-X; POLYMERASE CHAIN REACTION (PCR); DNA DIAGNOSIS;

D O I：

10.1007/BF01900713

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

The fragile X syndrome is a common familial form of mental retardation and is associated with a rare fragile site at Xq27.3 (FRAXA). This disorder has recently been reported to correlate with length variations of restriction genomic DNA fragments which may due to the amplification of (CCG)n trinucleotide repeats located at the FRAXA locus. We described here a rapid preparation method of diagnostic DNA probes for the fragile X syndrome by direct enzymatic amplification of human chromosomal DNA. The PstI-assay, which is Southern blot analysis of DNA samples probed by PCR products, was shown to be sensitive method for diagnostic purposes to detect the size variations specific in the fragile X syndrome.

引用

页码：195 / 203

页数：9

共 10 条

[1]

ARINAMI T, 1987, HUM GENET, V77, P92

[2] DISTAMYCIN-A-INDUCIBLE FRAGILE SITES AND CANCER PRONENESS [J].

HORI, T ;

TAKAHASHI, E ;

ISHIHARA, T ;

MINAMIHISAMATSU, M ;

KANEKO, Y ;

MURATA, M .

CANCER GENETICS AND CYTOGENETICS, 1988, 34 (02) :177-187

[3] MAPPING OF DNA INSTABILITY AT THE FRAGILE-X TO A TRINUCLEOTIDE REPEAT SEQUENCE P(CCG)N [J].

KREMER, EJ ;

PRITCHARD, M ;

LYNCH, M ;

YU, S ;

HOLMAN, K ;

BAKER, E ;

WARREN, ST ;

SCHLESSINGER, D ;

SUTHERLAND, GR ;

RICHARDS, RI .

SCIENCE, 1991, 252 (5013) :1711-1714

[4] MOLECULAR HETEROGENEITY OF THE FRAGILE-X SYNDROME [J].

NAKAHORI, Y ;

KNIGHT, SJL ;

HOLLAND, J ;

SCHWARTZ, C ;

ROCHE, A ;

TARLETON, J ;

WONG, S ;

FLINT, TJ ;

FROSTERISKENIUS, U ;

BENTLEY, D ;

DAVIES, KE ;

HIRST, MC .

NUCLEIC ACIDS RESEARCH, 1991, 19 (16) :4355-4359

[5] ABSENCE OF EXPRESSION OF THE FMR-1 GENE IN FRAGILE-X SYNDROME [J].

PIERETTI, M ;

ZHANG, FP ;

FU, YH ;

WARREN, ST ;

OOSTRA, BA ;

CASKEY, CT ;

NELSON, DL .

CELL, 1991, 66 (04) :817-822

[6]

Sutherland G, 1985, FRAGILE SITES HUMAN

[7] IDENTIFICATION OF A GENE (FMR-1) CONTAINING A CGG REPEAT COINCIDENT WITH A BREAKPOINT CLUSTER REGION EXHIBITING LENGTH VARIATION IN FRAGILE-X SYNDROME [J].

VERKERK, AJMH ;

PIERETTI, M ;

SUTCLIFFE, JS ;

FU, YH ;

KUHL, DPA ;

PIZZUTI, A ;

REINER, O ;

RICHARDS, S ;

VICTORIA, MF ;

ZHANG, FP ;

EUSSEN, BE ;

VANOMMEN, GJB ;

BLONDEN, LAJ ;

RIGGINS, GJ ;

CHASTAIN, JL ;

KUNST, CB ;

GALJAARD, H ;

CASKEY, CT ;

NELSON, DL ;

OOSTRA, BA ;

WARREN, ST .

CELL, 1991, 65 (05) :905-914

[8] MOLECULAR-CLONING OF THE HUMAN CTP SYNTHETASE GENE BY FUNCTIONAL COMPLEMENTATION WITH PURIFIED HUMAN METAPHASE CHROMOSOMES [J].

YAMAUCHI, M ;

YAMAUCHI, N ;

MEUTH, M .

EMBO JOURNAL, 1990, 9 (07) :2095-2099

[9] GENOMIC ORGANIZATION AND CHROMOSOMAL LOCALIZATION OF THE HUMAN CTP SYNTHETASE GENE (CTPS) [J].

YAMAUCHI, M ;

YAMAUCHI, N ;

PHEAR, G ;

SPURR, NK ;

MARTINSSON, T ;

WEITH, A ;

MEUTH, M .

GENOMICS, 1991, 11 (04) :1088-1096

[10] FRAGILE-X GENOTYPE CHARACTERIZED BY AN UNSTABLE REGION OF DNA [J].

YU, S ;

PRITCHARD, M ;

KREMER, E ;

LYNCH, M ;

NANCARROW, J ;

BAKER, E ;

HOLMAN, K ;

MULLEY, JC ;

WARREN, ST ;

SCHLESSINGER, D ;

SUTHERLAND, GR ;

RICHARDS, RI .

SCIENCE, 1991, 252 (5009) :1179-1181

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