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Barminomycin forms GC-specific adducts and virtual interstrand crosslinks with DNA.

机译:Barminomycin与DNA形成GC特异性加合物和虚拟链间交联。

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The sequence specificity of the binding of barminomycin (SN-07 chromophore) to DNA was investigated using an in vitro transcription assay. It was found that this compound formed blockages to transcription, and these blocks were highly selective for 5'-GC sequences. The half-lives of the first seven transcriptional blockages at 37 degrees C were 14-130 min, plus one site 200 min, with widely varying levels of essentially permanent blockages at each site (0-100%; average of 40%), indicative of considerable dependence on flanking sequences of adducts stability at individual GC sites. Barminomycin was also shown to form DNA virtual (i.e. functional) interstrand crosslinks. Such crosslinks were also relatively heat stable, with 40% of the DNA remaining crosslinked after heating at 90 degrees C for 5 min. The barminomycin-DNA adducts and crosslinks appear to be essentially identical to those formed between adriamycin and DNA. Whereas adriamycin requires prior activation with formaldehyde in order to form adducts and crosslinks, barminomycin behaves in all respects as if it is a pre-activated form of adriamycin.
机译:使用体外转录测定法研究了巴米霉素(SN-07生色团)与DNA结合的序列特异性。发现该化合物形成了转录的阻断,并且这些阻断对5'-GC序列具有高度选择性。在37摄氏度下,前七个转录阻断的半衰期为14-130分钟,外加一个 200分钟的位点,每个位点的基本永久阻断水平差异很大(0-100%;平均值为40%) ,表明在各个GC位置对加合物稳定性侧翼序列的依赖性很大。 Barminomycin还显示形成DNA虚拟(即功能性)链间交联。这样的交联也是相对热稳定的,在90℃下加热5分钟后,仍有40%的DNA保持交联。巴米霉素-DNA加合物和交联似乎与阿霉素和DNA之间形成的加合物和交联基本相同。阿霉素需要事先用甲醛活化才能形成加合物和交联,而巴米霉素在所有方面都表现得好像是阿霉素的预活化形式。

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