利用限制性内切酶带、脂蛋白DNA和结构改变对人类着丝粒区进行表征。

Molecular biology & medicine Pub Date : 1990-08-01
P H Arn, E W Jabs
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引用次数: 0

摘要

限制性内切酶诱导的显带研究有助于深入了解显带机制和染色体结构。我们研究了由各种限制性内切酶消化产生的染色体特异性阿尔法体DNA片段的大小是否与这些酶产生的c样带的存在与否有关。我们测定了来自五条不同染色体的阿尔法体DNA片段的大小,分别用六种不同的限制性内切酶进行消化。在特定的人类着丝点区域,蛋白限制性片段的长度与c样条带的产生没有明显的相关性。我们使用AluI酶和传统染色(CBG)技术来标记构象改变的着丝粒。这些包括双中心染色体,来自罗伯茨综合征患者的染色体和5-氮杂胞苷处理的中期染色体。在所有情况下,AluI产生的条带与CBG条带相似。我们发现5-氮杂胞苷诱导的着丝粒区明显去致密的部分没有带。我们的研究表明,限制性内切酶c样带化与脂蛋白DNA中限制性内切位点的存在没有严格的关系,着丝点区域的浓缩染色质构象可能在带化中起作用。
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Characterization of human centromeric regions using restriction enzyme banding, alphoid DNA and structural alterations.

Studies of banding induced by restriction enzymes may provide insight into banding mechanisms and chromosome structure. We examined whether or not the sizes of chromosome-specific alphoid DNA fragments created by digestion with various restriction enzymes relate to the presence or absence of C-like bands produced by these same enzymes. We sized alphoid DNA fragments from five different chromosomes, digested with each of six different restriction enzymes. There was no obvious correlation between the length of alphoid restriction fragments at specific human centromeric regions and the production of C-like bands. We used the enzyme AluI and traditional staining (CBG) techniques to band centromeres with conformational alterations. These included dicentric chromosomes, chromosomes from a patient with Roberts syndrome, and 5-azacytidine-treated prometaphase chromosomes. In all cases bands produced by AluI resembled CBG banding. We found that markedly decondensed portions of centromeric regions induced by 5-azacytidine did not band. Our studies demonstrate that restriction endonuclease C-like banding is not strictly related to the presence of restriction sites in alphoid DNA, and the condensed chromatin conformation at the centromeric region may play a role in banding.

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