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[DNA指纹与高变区:在医学和生物学中具有多种应用潜力的遗传标记]

[DNA fingerprints and hypervariable regions: genetic marker with many application potentials in medicine and biology].

作者信息

Fey M F

机构信息

Institut für Medizinische Onkologie der Universität, Inselspital Bern.

出版信息

Schweiz Med Wochenschr. 1989 Jun 10;119(23):815-25.

PMID:2672298
Abstract

DNA polymorphisms are based on variations in the nucleotide sequences of the DNA within a given population and are transmitted from parents to offspring by Mendelian inheritance. Most of these mutations are phenotypically silent. Two different types of DNA polymorphisms are restriction fragment length polymorphisms and highly variable regions (HVRs), the latter with many different alleles at a given locus. Molecular probes for HVRs (or DNA minisatellites) can detect a great number of cross-hybridising fragments dispersed throughout the genome. The polymorphic patterns of these fragments are completely individual-specific, hence termed DNA "fingerprints". DNA "fingerprinting" has been shown to be a powerful tool for establishing family relationships, for example in paternity disputes, and for the positive identification of individuals in forensic medicine. The technique may be used to document marrow engraftment in patients who have undergone allogeneic bone marrow transplantation. DNA "fingerprinting" is a new method of assessing clonality in human tumours by identifying clonal somatic mutations in the tumour DNA. Cloning of individual DNA "fingerprint" fragments yields locus-specific HVR probes which, due to their high rate of heterozygosity, are ideal for linkage analysis and prenatal diagnosis in single gene disorders. This is exemplified by adult polycystic kidney disease, which has been found by a 3'alpha-globin-HVR probe to be closely linked to the alpha-globin-gene cluster on chromosome 16p. Locus-specific HVR probes have been used for the molecular diagnosis of clonal chromosomal deletions or loss of heterozygosity at particular loci in a large variety of tumours. These findings are the basis for the identification of anti-oncogenes or putative tumour-suppressor genes in the human genome.

摘要

DNA多态性基于特定人群中DNA核苷酸序列的变异,并通过孟德尔遗传从父母传递给后代。这些突变大多在表型上是沉默的。两种不同类型的DNA多态性是限制性片段长度多态性和高变区(HVRs),后者在给定基因座上有许多不同的等位基因。HVRs(或DNA小卫星)的分子探针可以检测到大量分散在整个基因组中的交叉杂交片段。这些片段的多态性模式是完全个体特异性的,因此被称为DNA“指纹”。DNA“指纹识别”已被证明是建立家族关系的有力工具,例如在亲子鉴定纠纷中,以及在法医学中对个体进行阳性识别。该技术可用于记录接受同种异体骨髓移植患者的骨髓植入情况。DNA“指纹识别”是一种通过识别肿瘤DNA中的克隆体细胞突变来评估人类肿瘤克隆性的新方法。单个DNA“指纹”片段的克隆产生位点特异性HVR探针,由于其高杂合率,非常适合单基因疾病的连锁分析和产前诊断。成人多囊肾病就是一个例子,通过3'α-珠蛋白-HVR探针发现它与16号染色体p臂上的α-珠蛋白基因簇紧密连锁。位点特异性HVR探针已用于多种肿瘤中特定位点的克隆染色体缺失或杂合性缺失的分子诊断。这些发现是在人类基因组中鉴定抗癌基因或假定的肿瘤抑制基因的基础。

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