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首页> 外文期刊>Molecular and Cellular Biology >Evi-1, a murine zinc finger proto-oncogene, encodes a sequence-specific DNA-binding protein.
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Evi-1, a murine zinc finger proto-oncogene, encodes a sequence-specific DNA-binding protein.

机译:鼠锌指原癌基因Evi-1编码序列特异性DNA结合蛋白。

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Evi-1 was originally identified as a common site of viral integration in murine myeloid tumors. Evi-1 encodes a 120-kDa polypeptide containing 10 zinc finger motifs located in two domains 380 amino acids apart and an acidic domain located carboxy terminal to the second set of zinc fingers. These features suggest that Evi-1 is a site-specific DNA-binding protein involved in the regulation of RNA transcription. We have purified Evi-1 protein from E. coli and have employed a gel shift-polymerase chain reaction method using random oligonucleotides to identify a high-affinity binding site for Evi-1. The consensus sequence for this binding site is TGACAAGATAA. Evi-1 protein specifically protects this motif from DNase I digestion. By searching the nucleotide sequence data bases, we have found this binding site both in sequences 5' to genes in putative or known regulatory regions and within intron sequences.
机译:Evi-1最初被确定为鼠髓样肿瘤中病毒整合的常见位点。 Evi-1编码一个120 kDa的多肽,该多肽包含10个锌指基序,位于两个相隔380个氨基酸的域中,而酸性域位于第二组锌指的羧基末端。这些特征表明,Evi-1是一种参与RNA转录调控的位点特异性DNA结合蛋白。我们从大肠杆菌中纯化了Evi-1蛋白,并采用了凝胶移位聚合酶链反应方法,使用随机寡核苷酸来鉴定Evi-1的高亲和力结合位点。该结合位点的共有序列是TGACAAGATAA。 Evi-1蛋白可特异性保护该基序免受DNase I消化。通过搜索核苷酸序列数据库,我们在推定的或已知的调控区域和内含子序列中的基因的5'序列中都发现了该结合位点。

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